Taeniasis/cysticercosis

Infectious Disease MONDO:0015484 Helminth infection Neglected tropical disease

Taeniasis/cysticercosis is caused by Taenia solium, with intestinal taeniasis and tissue cysticercosis including neurocysticercosis, a major cause of seizures in endemic regions.

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1
Pathophys.
1
Phenotypes
2
Treatments
20
References
1
Deep Research

Pathophysiology

1
Larval infection of the nervous system (neurocysticercosis)
Larval Taenia solium infects the human nervous system.
Show evidence (1 reference)
PMID:12932389 SUPPORT
"The larval stage of the pork tapeworm (Taenia solium) infects the human nervous system, causing neurocysticercosis."
The abstract links larval infection to neurocysticercosis.

Phenotypes

1
Seizures OCCASIONAL Neurologic HP:0001250
Show evidence (1 reference)
PMID:12932389 SUPPORT
"This disease is one of the main causes of epileptic seizures in many less developed countries"
Neurocysticercosis is a major cause of seizures in endemic regions.
💊

Treatments

2
Antiparasitic therapy
Action: antimicrobial agent therapy MAXO:0001021
Antiparasitic drugs are used to kill brain parasites in neurocysticercosis.
Show evidence (1 reference)
PMID:12932389 SUPPORT
"Available therapeutic measures include steroids, treatments for symptoms, surgery, and, more controversially, antiparasitic drugs to kill brain parasites."
The abstract lists antiparasitic drugs among available treatments.
Surgical management
Action: surgical procedure MAXO:0000004
Surgical interventions may be used in selected cases.
Show evidence (1 reference)
PMID:12932389 SUPPORT
"Available therapeutic measures include steroids, treatments for symptoms, surgery, and, more controversially, antiparasitic drugs to kill brain parasites."
The abstract includes surgery as a treatment option.
{ }

Source YAML

click to show 
name: Taeniasis/cysticercosis
creation_date: '2026-01-26T15:56:41Z'
updated_date: '2026-04-22T20:53:03Z'
category: Infectious Disease
description: >-
  Taeniasis/cysticercosis is caused by Taenia solium, with intestinal
  taeniasis and tissue cysticercosis including neurocysticercosis, a major
  cause of seizures in endemic regions.
disease_term:
  term:
    id: MONDO:0015484
    label: cysticercosis
  preferred_term: Cysticercosis
parents:
- Helminth infection
- Neglected tropical disease
infectious_agent:
- name: Taenia solium
  infectious_agent_term:
    preferred_term: Taenia solium
    term:
      id: NCBITaxon:6204
      label: Taenia solium
  description: Pork tapeworm responsible for taeniasis and cysticercosis.
  evidence:
  - reference: PMID:12932389
    reference_title: "Taenia solium cysticercosis."
    supports: SUPPORT
    snippet: "The larval stage of the pork tapeworm (Taenia solium) infects the human nervous system, causing neurocysticercosis."
    explanation: The abstract identifies Taenia solium as the causative tapeworm.
agent_life_cycle:
  description: Taenia solium cycles between taeniasis and cysticercosis, including porcine and human stages.
  hosts:
  - preferred_term: human
    term:
      id: NCBITaxon:9606
      label: Homo sapiens
    role: definitive host
  - preferred_term: domestic pig
    term:
      id: NCBITaxon:9825
      label: Sus scrofa domesticus
    role: intermediate host
  life_cycle_stages:
  - name: Adult parasitic worm stage (taeniasis)
    life_cycle_stage_term:
      preferred_term: adult parasitic worm stage
      term:
        id: OPL:0000237
        label: adult parasitic worm stage
    description: Adult tapeworm stage corresponds to taeniasis in humans.
    evidence:
    - reference: PMID:32461308
      reference_title: "Taenia solium Cysticercosis and Its Impact in Neurological Disease."
      supports: SUPPORT
      snippet: "This paper reviews all aspects of its life cycle (taeniasis, porcine cysticercosis, human cysticercosis)"
      explanation: The life cycle includes taeniasis as the adult worm stage.
pathophysiology:
- name: Larval infection of the nervous system (neurocysticercosis)
  description: Larval Taenia solium infects the human nervous system.
  evidence:
  - reference: PMID:12932389
    reference_title: "Taenia solium cysticercosis."
    supports: SUPPORT
    snippet: "The larval stage of the pork tapeworm (Taenia solium) infects the human nervous system, causing neurocysticercosis."
    explanation: The abstract links larval infection to neurocysticercosis.
phenotypes:
- name: Seizures
  category: Neurologic
  frequency: OCCASIONAL
  phenotype_term:
    preferred_term: Seizure
    term:
      id: HP:0001250
      label: Seizure
  evidence:
  - reference: PMID:12932389
    reference_title: "Taenia solium cysticercosis."
    supports: SUPPORT
    snippet: "This disease is one of the main causes of epileptic seizures in many less developed countries"
    explanation: Neurocysticercosis is a major cause of seizures in endemic regions.
treatments:
- name: Antiparasitic therapy
  description: Antiparasitic drugs are used to kill brain parasites in neurocysticercosis.
  treatment_term:
    preferred_term: antimicrobial agent therapy
    term:
      id: MAXO:0001021
      label: antimicrobial agent therapy
  evidence:
  - reference: PMID:12932389
    reference_title: "Taenia solium cysticercosis."
    supports: SUPPORT
    snippet: "Available therapeutic measures include steroids, treatments for symptoms, surgery, and, more controversially, antiparasitic drugs to kill brain parasites."
    explanation: The abstract lists antiparasitic drugs among available treatments.
- name: Surgical management
  description: Surgical interventions may be used in selected cases.
  treatment_term:
    preferred_term: surgical procedure
    term:
      id: MAXO:0000004
      label: surgical procedure
  evidence:
  - reference: PMID:12932389
    reference_title: "Taenia solium cysticercosis."
    supports: SUPPORT
    snippet: "Available therapeutic measures include steroids, treatments for symptoms, surgery, and, more controversially, antiparasitic drugs to kill brain parasites."
    explanation: The abstract includes surgery as a treatment option.
references:
- reference: DOI:10.1007/s15010-023-02021-y
  title: 'Efficacy and safety of antiparasitic therapy for neurocysticercosis in rural Tanzania: a prospective cohort study'
  found_in:
  - Taeniasis_Cysticercosis-deep-research-falcon.md
  findings:
  - statement: Neurocysticercosis is common in regions endemic for Taenia solium.
    supporting_text: Neurocysticercosis is common in regions endemic for Taenia solium.
    evidence:
    - reference: DOI:10.1007/s15010-023-02021-y
      reference_title: 'Efficacy and safety of antiparasitic therapy for neurocysticercosis in rural Tanzania: a prospective cohort study'
      supports: SUPPORT
      evidence_source: HUMAN_CLINICAL
      snippet: Neurocysticercosis is common in regions endemic for Taenia solium.
      explanation: Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
- reference: DOI:10.1007/s44197-024-00271-z
  title: 'Neurocysticercosis Prevalence and Characteristics in Communities of Sinda District in Zambia: A Cross-Sectional Study'
  found_in:
  - Taeniasis_Cysticercosis-deep-research-falcon.md
  findings:
  - statement: This study aimed at describing the epidemiology of (neuro)cysticercosis as well as its clinical and radiological characteristics in a Taenia solium endemic district of Zambia.
    supporting_text: This study aimed at describing the epidemiology of (neuro)cysticercosis as well as its clinical and radiological characteristics in a Taenia solium endemic district of Zambia.
    evidence:
    - reference: DOI:10.1007/s44197-024-00271-z
      reference_title: 'Neurocysticercosis Prevalence and Characteristics in Communities of Sinda District in Zambia: A Cross-Sectional Study'
      supports: SUPPORT
      evidence_source: HUMAN_CLINICAL
      snippet: This study aimed at describing the epidemiology of (neuro)cysticercosis as well as its clinical and radiological characteristics in a Taenia solium endemic district of Zambia.
      explanation: Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
- reference: DOI:10.1016/j.lana.2024.100876
  title: 'Mass chemotherapy with niclosamide for the control of Taenia solium: population-based safety profile and treatment effectiveness'
  found_in:
  - Taeniasis_Cysticercosis-deep-research-falcon.md
  findings:
  - statement: 'Mass chemotherapy with niclosamide for the control of Taenia solium: population-based safety profile and treatment effectiveness'
    supporting_text: 'Mass chemotherapy with niclosamide for the control of Taenia solium: population-based safety profile and treatment effectiveness'
- reference: DOI:10.1093/jtm/taac102
  title: 'Clinical characteristics and management of neurocysticercosis patients: a retrospective assessment of case reports from Europe'
  found_in:
  - Taeniasis_Cysticercosis-deep-research-falcon.md
  findings:
  - statement: Neurocysticercosis (NCC) is a parasitic disease caused by the larval stage of the tapeworm Taenia solium.
    supporting_text: Neurocysticercosis (NCC) is a parasitic disease caused by the larval stage of the tapeworm Taenia solium.
    evidence:
    - reference: DOI:10.1093/jtm/taac102
      reference_title: 'Clinical characteristics and management of neurocysticercosis patients: a retrospective assessment of case reports from Europe'
      supports: SUPPORT
      evidence_source: HUMAN_CLINICAL
      snippet: Neurocysticercosis (NCC) is a parasitic disease caused by the larval stage of the tapeworm Taenia solium.
      explanation: Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
- reference: DOI:10.1111/tmi.13870
  title: "The challenges of detecting <i>Taenia solium</i> and neurocysticercosis in low and middle‐income countries: A scoping review of Lao People's Democratic Republic"
  found_in:
  - Taeniasis_Cysticercosis-deep-research-falcon.md
  findings:
  - statement: Taenia solium is a tapeworm of global importance due to the burden of disease associated with human epilepsy caused by neurocysticercosis.
    supporting_text: Taenia solium is a tapeworm of global importance due to the burden of disease associated with human epilepsy caused by neurocysticercosis.
    evidence:
    - reference: DOI:10.1111/tmi.13870
      reference_title: "The challenges of detecting <i>Taenia solium</i> and neurocysticercosis in low and middle‐income countries: A scoping review of Lao People's Democratic Republic"
      supports: SUPPORT
      evidence_source: HUMAN_CLINICAL
      snippet: Taenia solium is a tapeworm of global importance due to the burden of disease associated with human epilepsy caused by neurocysticercosis.
      explanation: Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
- reference: DOI:10.1186/s13071-023-05989-6
  title: Insights into the diagnosis, vaccines, and control of Taenia solium, a zoonotic, neglected parasite
  found_in:
  - Taeniasis_Cysticercosis-deep-research-falcon.md
  findings:
  - statement: Taenia solium taeniasis/cysticercosis (TSTC) is a foodborne, zoonotic neglected tropical disease affecting predominately low- and middle-income countries.
    supporting_text: Taenia solium taeniasis/cysticercosis (TSTC) is a foodborne, zoonotic neglected tropical disease affecting predominately low- and middle-income countries.
    evidence:
    - reference: DOI:10.1186/s13071-023-05989-6
      reference_title: Insights into the diagnosis, vaccines, and control of Taenia solium, a zoonotic, neglected parasite
      supports: SUPPORT
      evidence_source: OTHER
      snippet: Taenia solium taeniasis/cysticercosis (TSTC) is a foodborne, zoonotic neglected tropical disease affecting predominately low- and middle-income countries.
      explanation: Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
- reference: DOI:10.1212/wnl.0000000000209865
  title: Seizures and Epilepsy in Association With Neurocysticercosis
  found_in:
  - Taeniasis_Cysticercosis-deep-research-falcon.md
  findings:
  - statement: Seizures and Epilepsy in Association With Neurocysticercosis
    supporting_text: Seizures and Epilepsy in Association With Neurocysticercosis
- reference: DOI:10.1371/journal.pntd.0011042
  title: 'The epidemiology of human Taenia solium infections: A systematic review of the distribution in Eastern and Southern Africa'
  found_in:
  - Taeniasis_Cysticercosis-deep-research-falcon.md
  findings:
  - statement: Taenia solium is a tapeworm that causes taeniosis in humans and cysticercosis in humans and pigs.
    supporting_text: Taenia solium is a tapeworm that causes taeniosis in humans and cysticercosis in humans and pigs.
    evidence:
    - reference: DOI:10.1371/journal.pntd.0011042
      reference_title: 'The epidemiology of human Taenia solium infections: A systematic review of the distribution in Eastern and Southern Africa'
      supports: SUPPORT
      evidence_source: OTHER
      snippet: Taenia solium is a tapeworm that causes taeniosis in humans and cysticercosis in humans and pigs.
      explanation: Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
- reference: DOI:10.1371/journal.pntd.0012140
  title: The Vicious Worm education tool improves the knowledge of community health workers on Taenia solium cysticercosis in Rwanda
  found_in:
  - Taeniasis_Cysticercosis-deep-research-falcon.md
  findings:
  - statement: The pork tapeworm Taenia solium causes human taeniasis and cysticercosis when ingested as viable cysts and eggs, respectively.
    supporting_text: The pork tapeworm Taenia solium causes human taeniasis and cysticercosis when ingested as viable cysts and eggs, respectively.
    evidence:
    - reference: DOI:10.1371/journal.pntd.0012140
      reference_title: The Vicious Worm education tool improves the knowledge of community health workers on Taenia solium cysticercosis in Rwanda
      supports: SUPPORT
      evidence_source: HUMAN_CLINICAL
      snippet: The pork tapeworm Taenia solium causes human taeniasis and cysticercosis when ingested as viable cysts and eggs, respectively.
      explanation: Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
- reference: DOI:10.1371/journal.pntd.0012643
  title: 'Accuracy of immunological tests on serum and urine for diagnosis of Taenia solium neurocysticercosis: A systematic review'
  found_in:
  - Taeniasis_Cysticercosis-deep-research-falcon.md
  findings:
  - statement: 'Taenia solium neurocysticercosis is a zoonotic neglected tropical disease, for which adequate diagnostic management is paramount, especially in patients with active cysts for whom improved and timely management could prove beneficial.'
    supporting_text: Taenia solium neurocysticercosis is a zoonotic neglected tropical disease, for which adequate diagnostic management is paramount, especially in patients with active cysts for whom improved and timely management could prove beneficial.
    evidence:
    - reference: DOI:10.1371/journal.pntd.0012643
      reference_title: 'Accuracy of immunological tests on serum and urine for diagnosis of Taenia solium neurocysticercosis: A systematic review'
      supports: SUPPORT
      evidence_source: OTHER
      snippet: Taenia solium neurocysticercosis is a zoonotic neglected tropical disease, for which adequate diagnostic management is paramount, especially in patients with active cysts for whom improved and timely management could prove beneficial.
      explanation: Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
- reference: DOI:10.1371/journal.pone.0307240
  title: 'Assessment of knowledge and practices regarding taeniasis and cysticercosis in Pak Chong, Nakhon Ratchasima, Thailand: A cross-sectional study'
  found_in:
  - Taeniasis_Cysticercosis-deep-research-falcon.md
  findings:
  - statement: Taeniasis and cysticercosis are parasitic infections caused by Taenia spp., mainly transmitted through the consumption of undercooked pork.
    supporting_text: Taeniasis and cysticercosis are parasitic infections caused by Taenia spp., mainly transmitted through the consumption of undercooked pork.
    evidence:
    - reference: DOI:10.1371/journal.pone.0307240
      reference_title: 'Assessment of knowledge and practices regarding taeniasis and cysticercosis in Pak Chong, Nakhon Ratchasima, Thailand: A cross-sectional study'
      supports: SUPPORT
      evidence_source: HUMAN_CLINICAL
      snippet: Taeniasis and cysticercosis are parasitic infections caused by Taenia spp., mainly transmitted through the consumption of undercooked pork.
      explanation: Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
- reference: DOI:10.3389/fpara.2024.1394089
  title: 'From laboratory to clinical practice: an update of the immunological and molecular tools for neurocysticercosis diagnosis'
  found_in:
  - Taeniasis_Cysticercosis-deep-research-falcon.md
  findings:
  - statement: Neurocysticercosis (NCC) is caused by the invasion of Taenia solium larvae in the central nervous system (CNS) and stands as the predominant cause of epilepsy and other neurological disorders in many developing nations.
    supporting_text: Neurocysticercosis (NCC) is caused by the invasion of Taenia solium larvae in the central nervous system (CNS) and stands as the predominant cause of epilepsy and other neurological disorders in many developing nations.
    evidence:
    - reference: DOI:10.3389/fpara.2024.1394089
      reference_title: 'From laboratory to clinical practice: an update of the immunological and molecular tools for neurocysticercosis diagnosis'
      supports: SUPPORT
      evidence_source: OTHER
      snippet: Neurocysticercosis (NCC) is caused by the invasion of Taenia solium larvae in the central nervous system (CNS) and stands as the predominant cause of epilepsy and other neurological disorders in many developing nations.
      explanation: Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
- reference: DOI:10.3390/pathogens13010026
  title: 'Calcified Neurocysticercosis: Demographic, Clinical, and Radiological Characteristics of a Large Hospital-Based Patient Cohort'
  found_in:
  - Taeniasis_Cysticercosis-deep-research-falcon.md
  findings:
  - statement: Neurocysticercosis (NCC), the infection of the central nervous system caused by Taenia solium larvae (cysticerci), is a major cause of acquired epilepsy worldwide.
    supporting_text: Neurocysticercosis (NCC), the infection of the central nervous system caused by Taenia solium larvae (cysticerci), is a major cause of acquired epilepsy worldwide.
    evidence:
    - reference: DOI:10.3390/pathogens13010026
      reference_title: 'Calcified Neurocysticercosis: Demographic, Clinical, and Radiological Characteristics of a Large Hospital-Based Patient Cohort'
      supports: SUPPORT
      evidence_source: HUMAN_CLINICAL
      snippet: Neurocysticercosis (NCC), the infection of the central nervous system caused by Taenia solium larvae (cysticerci), is a major cause of acquired epilepsy worldwide.
      explanation: Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
- reference: DOI:10.3390/pathogens13030218
  title: Current Role of Surgery in the Treatment of Neurocysticercosis
  found_in:
  - Taeniasis_Cysticercosis-deep-research-falcon.md
  findings:
  - statement: Neurocysticercosis (NCC) is a common parasitic disease of the central nervous system (CNS) in low- and middle-income countries.
    supporting_text: Neurocysticercosis (NCC) is a common parasitic disease of the central nervous system (CNS) in low- and middle-income countries.
    evidence:
    - reference: DOI:10.3390/pathogens13030218
      reference_title: Current Role of Surgery in the Treatment of Neurocysticercosis
      supports: SUPPORT
      evidence_source: OTHER
      snippet: Neurocysticercosis (NCC) is a common parasitic disease of the central nervous system (CNS) in low- and middle-income countries.
      explanation: Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
- reference: DOI:10.3390/pathogens13110988
  title: Seroprevalence and Risk Factors for Cysticercosis in Mexican Americans in Starr County, Texas
  found_in:
  - Taeniasis_Cysticercosis-deep-research-falcon.md
  findings:
  - statement: Cysticercosis is a parasitic infection and neglected tropical disease caused by Taenia solium, or the pork tapeworm.
    supporting_text: Cysticercosis is a parasitic infection and neglected tropical disease caused by Taenia solium, or the pork tapeworm.
    evidence:
    - reference: DOI:10.3390/pathogens13110988
      reference_title: Seroprevalence and Risk Factors for Cysticercosis in Mexican Americans in Starr County, Texas
      supports: SUPPORT
      evidence_source: OTHER
      snippet: Cysticercosis is a parasitic infection and neglected tropical disease caused by Taenia solium, or the pork tapeworm.
      explanation: Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
- reference: DOI:10.3390/tropicalmed9090215
  title: 'Murine Extraparenchymal Neurocysticercosis: Appropriate Model for Evaluating Anthelminthic and Anti-Inflammatory Treatment Schedules'
  found_in:
  - Taeniasis_Cysticercosis-deep-research-falcon.md
  findings:
  - statement: Experimental models of neurocysticercosis (NCC) are helpful for an improved understanding of the pathophysiological mechanisms of human diseases and for testing novel therapeutic approaches.
    supporting_text: Experimental models of neurocysticercosis (NCC) are helpful for an improved understanding of the pathophysiological mechanisms of human diseases and for testing novel therapeutic approaches.
    evidence:
    - reference: DOI:10.3390/tropicalmed9090215
      reference_title: 'Murine Extraparenchymal Neurocysticercosis: Appropriate Model for Evaluating Anthelminthic and Anti-Inflammatory Treatment Schedules'
      supports: SUPPORT
      evidence_source: MODEL_ORGANISM
      snippet: Experimental models of neurocysticercosis (NCC) are helpful for an improved understanding of the pathophysiological mechanisms of human diseases and for testing novel therapeutic approaches.
      explanation: Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
- reference: DOI:10.3390/zoonoticdis4020013
  title: Prevalence and Risk Factors of Human Taenia solium Cysticercosis in Mbulu District, Northern Tanzania
  found_in:
  - Taeniasis_Cysticercosis-deep-research-falcon.md
  findings:
  - statement: Taeniosis and cysticercosis are human infections caused by the pork tapeworm, Taenia solium.
    supporting_text: Taeniosis and cysticercosis are human infections caused by the pork tapeworm, Taenia solium.
    evidence:
    - reference: DOI:10.3390/zoonoticdis4020013
      reference_title: Prevalence and Risk Factors of Human Taenia solium Cysticercosis in Mbulu District, Northern Tanzania
      supports: SUPPORT
      evidence_source: HUMAN_CLINICAL
      snippet: Taeniosis and cysticercosis are human infections caused by the pork tapeworm, Taenia solium.
      explanation: Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
- reference: DOI:10.5772/intechopen.1004554
  title: 'Neurocysticercosis and the Central Nervous System: Advancements in Diagnosis, Treatment, and Future Prospects'
  found_in:
  - Taeniasis_Cysticercosis-deep-research-falcon.md
  findings:
  - statement: Neurocysticercosis presents a formidable global health challenge.
    supporting_text: Neurocysticercosis presents a formidable global health challenge.
    evidence:
    - reference: DOI:10.5772/intechopen.1004554
      reference_title: 'Neurocysticercosis and the Central Nervous System: Advancements in Diagnosis, Treatment, and Future Prospects'
      supports: SUPPORT
      evidence_source: OTHER
      snippet: Neurocysticercosis presents a formidable global health challenge.
      explanation: Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
- reference: DOI:10.5772/intechopen.110727
  title: Epidemiology of Taeniosis/Cysticercosis in Humans and Animals
  found_in:
  - Taeniasis_Cysticercosis-deep-research-falcon.md
  findings:
  - statement: Taenia saginata, Taenia solium, and Taenia asiatica popularly known as beef, pork, and Asian tapeworm, are important food-borne parasites.
    supporting_text: Taenia saginata, Taenia solium, and Taenia asiatica popularly known as beef, pork, and Asian tapeworm, are important food-borne parasites.
    evidence:
    - reference: DOI:10.5772/intechopen.110727
      reference_title: Epidemiology of Taeniosis/Cysticercosis in Humans and Animals
      supports: SUPPORT
      evidence_source: HUMAN_CLINICAL
      snippet: Taenia saginata, Taenia solium, and Taenia asiatica popularly known as beef, pork, and Asian tapeworm, are important food-borne parasites.
      explanation: Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
- reference: DOI:10.7759/cureus.64617
  title: 'Effectiveness of the Antiparasitic Combination of Albendazole and Praziquantel As Compared With Albendazole Monotherapy in the Treatment of Neurocysticercosis in Children: A Systematic Review and Meta-Analysis'
  found_in:
  - Taeniasis_Cysticercosis-deep-research-falcon.md
  findings:
  - statement: 'Effectiveness of the Antiparasitic Combination of Albendazole and Praziquantel As Compared With Albendazole Monotherapy in the Treatment of Neurocysticercosis in Children: A Systematic Review and Meta-Analysis'
    supporting_text: 'Effectiveness of the Antiparasitic Combination of Albendazole and Praziquantel As Compared With Albendazole Monotherapy in the Treatment of Neurocysticercosis in Children: A Systematic Review and Meta-Analysis'
📚

References & Deep Research

References

20
DOI:10.1007/s15010-023-02021-y
Efficacy and safety of antiparasitic therapy for neurocysticercosis in rural Tanzania: a prospective cohort study
1 finding
Neurocysticercosis is common in regions endemic for Taenia solium.
"Neurocysticercosis is common in regions endemic for Taenia solium."
Show evidence (1 reference)
DOI:10.1007/s15010-023-02021-y SUPPORT Human Clinical
"Neurocysticercosis is common in regions endemic for Taenia solium."
Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
DOI:10.1007/s44197-024-00271-z
Neurocysticercosis Prevalence and Characteristics in Communities of Sinda District in Zambia: A Cross-Sectional Study
1 finding
This study aimed at describing the epidemiology of (neuro)cysticercosis as well as its clinical and radiological characteristics in a Taenia solium endemic district of Zambia.
"This study aimed at describing the epidemiology of (neuro)cysticercosis as well as its clinical and radiological characteristics in a Taenia solium endemic district of Zambia."
Show evidence (1 reference)
DOI:10.1007/s44197-024-00271-z SUPPORT Human Clinical
"This study aimed at describing the epidemiology of (neuro)cysticercosis as well as its clinical and radiological characteristics in a Taenia solium endemic district of Zambia."
Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
DOI:10.1016/j.lana.2024.100876
Mass chemotherapy with niclosamide for the control of Taenia solium: population-based safety profile and treatment effectiveness
1 finding
Mass chemotherapy with niclosamide for the control of Taenia solium: population-based safety profile and treatment effectiveness
"Mass chemotherapy with niclosamide for the control of Taenia solium: population-based safety profile and treatment effectiveness"
DOI:10.1093/jtm/taac102
Clinical characteristics and management of neurocysticercosis patients: a retrospective assessment of case reports from Europe
1 finding
Neurocysticercosis (NCC) is a parasitic disease caused by the larval stage of the tapeworm Taenia solium.
"Neurocysticercosis (NCC) is a parasitic disease caused by the larval stage of the tapeworm Taenia solium."
Show evidence (1 reference)
DOI:10.1093/jtm/taac102 SUPPORT Human Clinical
"Neurocysticercosis (NCC) is a parasitic disease caused by the larval stage of the tapeworm Taenia solium."
Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
DOI:10.1111/tmi.13870
The challenges of detecting <i>Taenia solium</i> and neurocysticercosis in low and middle‐income countries: A scoping review of Lao People's Democratic Republic
1 finding
Taenia solium is a tapeworm of global importance due to the burden of disease associated with human epilepsy caused by neurocysticercosis.
"Taenia solium is a tapeworm of global importance due to the burden of disease associated with human epilepsy caused by neurocysticercosis."
Show evidence (1 reference)
DOI:10.1111/tmi.13870 SUPPORT Human Clinical
"Taenia solium is a tapeworm of global importance due to the burden of disease associated with human epilepsy caused by neurocysticercosis."
Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
DOI:10.1186/s13071-023-05989-6
Insights into the diagnosis, vaccines, and control of Taenia solium, a zoonotic, neglected parasite
1 finding
Taenia solium taeniasis/cysticercosis (TSTC) is a foodborne, zoonotic neglected tropical disease affecting predominately low- and middle-income countries.
"Taenia solium taeniasis/cysticercosis (TSTC) is a foodborne, zoonotic neglected tropical disease affecting predominately low- and middle-income countries."
Show evidence (1 reference)
DOI:10.1186/s13071-023-05989-6 SUPPORT Other
"Taenia solium taeniasis/cysticercosis (TSTC) is a foodborne, zoonotic neglected tropical disease affecting predominately low- and middle-income countries."
Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
DOI:10.1212/wnl.0000000000209865
Seizures and Epilepsy in Association With Neurocysticercosis
1 finding
Seizures and Epilepsy in Association With Neurocysticercosis
"Seizures and Epilepsy in Association With Neurocysticercosis"
DOI:10.1371/journal.pntd.0011042
The epidemiology of human Taenia solium infections: A systematic review of the distribution in Eastern and Southern Africa
1 finding
Taenia solium is a tapeworm that causes taeniosis in humans and cysticercosis in humans and pigs.
"Taenia solium is a tapeworm that causes taeniosis in humans and cysticercosis in humans and pigs."
Show evidence (1 reference)
DOI:10.1371/journal.pntd.0011042 SUPPORT Other
"Taenia solium is a tapeworm that causes taeniosis in humans and cysticercosis in humans and pigs."
Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
DOI:10.1371/journal.pntd.0012140
The Vicious Worm education tool improves the knowledge of community health workers on Taenia solium cysticercosis in Rwanda
1 finding
The pork tapeworm Taenia solium causes human taeniasis and cysticercosis when ingested as viable cysts and eggs, respectively.
"The pork tapeworm Taenia solium causes human taeniasis and cysticercosis when ingested as viable cysts and eggs, respectively."
Show evidence (1 reference)
DOI:10.1371/journal.pntd.0012140 SUPPORT Human Clinical
"The pork tapeworm Taenia solium causes human taeniasis and cysticercosis when ingested as viable cysts and eggs, respectively."
Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
DOI:10.1371/journal.pntd.0012643
Accuracy of immunological tests on serum and urine for diagnosis of Taenia solium neurocysticercosis: A systematic review
1 finding
Taenia solium neurocysticercosis is a zoonotic neglected tropical disease, for which adequate diagnostic management is paramount, especially in patients with active cysts for whom improved and timely management could prove beneficial.
"Taenia solium neurocysticercosis is a zoonotic neglected tropical disease, for which adequate diagnostic management is paramount, especially in patients with active cysts for whom improved and timely management could prove beneficial."
Show evidence (1 reference)
DOI:10.1371/journal.pntd.0012643 SUPPORT Other
"Taenia solium neurocysticercosis is a zoonotic neglected tropical disease, for which adequate diagnostic management is paramount, especially in patients with active cysts for whom improved and timely management could prove beneficial."
Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
DOI:10.1371/journal.pone.0307240
Assessment of knowledge and practices regarding taeniasis and cysticercosis in Pak Chong, Nakhon Ratchasima, Thailand: A cross-sectional study
1 finding
Taeniasis and cysticercosis are parasitic infections caused by Taenia spp., mainly transmitted through the consumption of undercooked pork.
"Taeniasis and cysticercosis are parasitic infections caused by Taenia spp., mainly transmitted through the consumption of undercooked pork."
Show evidence (1 reference)
DOI:10.1371/journal.pone.0307240 SUPPORT Human Clinical
"Taeniasis and cysticercosis are parasitic infections caused by Taenia spp., mainly transmitted through the consumption of undercooked pork."
Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
DOI:10.3389/fpara.2024.1394089
From laboratory to clinical practice: an update of the immunological and molecular tools for neurocysticercosis diagnosis
1 finding
Neurocysticercosis (NCC) is caused by the invasion of Taenia solium larvae in the central nervous system (CNS) and stands as the predominant cause of epilepsy and other neurological disorders in many developing nations.
"Neurocysticercosis (NCC) is caused by the invasion of Taenia solium larvae in the central nervous system (CNS) and stands as the predominant cause of epilepsy and other neurological disorders in many developing nations."
Show evidence (1 reference)
DOI:10.3389/fpara.2024.1394089 SUPPORT Other
"Neurocysticercosis (NCC) is caused by the invasion of Taenia solium larvae in the central nervous system (CNS) and stands as the predominant cause of epilepsy and other neurological disorders in many developing nations."
Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
DOI:10.3390/pathogens13010026
Calcified Neurocysticercosis: Demographic, Clinical, and Radiological Characteristics of a Large Hospital-Based Patient Cohort
1 finding
Neurocysticercosis (NCC), the infection of the central nervous system caused by Taenia solium larvae (cysticerci), is a major cause of acquired epilepsy worldwide.
"Neurocysticercosis (NCC), the infection of the central nervous system caused by Taenia solium larvae (cysticerci), is a major cause of acquired epilepsy worldwide."
Show evidence (1 reference)
DOI:10.3390/pathogens13010026 SUPPORT Human Clinical
"Neurocysticercosis (NCC), the infection of the central nervous system caused by Taenia solium larvae (cysticerci), is a major cause of acquired epilepsy worldwide."
Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
DOI:10.3390/pathogens13030218
Current Role of Surgery in the Treatment of Neurocysticercosis
1 finding
Neurocysticercosis (NCC) is a common parasitic disease of the central nervous system (CNS) in low- and middle-income countries.
"Neurocysticercosis (NCC) is a common parasitic disease of the central nervous system (CNS) in low- and middle-income countries."
Show evidence (1 reference)
DOI:10.3390/pathogens13030218 SUPPORT Other
"Neurocysticercosis (NCC) is a common parasitic disease of the central nervous system (CNS) in low- and middle-income countries."
Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
DOI:10.3390/pathogens13110988
Seroprevalence and Risk Factors for Cysticercosis in Mexican Americans in Starr County, Texas
1 finding
Cysticercosis is a parasitic infection and neglected tropical disease caused by Taenia solium, or the pork tapeworm.
"Cysticercosis is a parasitic infection and neglected tropical disease caused by Taenia solium, or the pork tapeworm."
Show evidence (1 reference)
DOI:10.3390/pathogens13110988 SUPPORT Other
"Cysticercosis is a parasitic infection and neglected tropical disease caused by Taenia solium, or the pork tapeworm."
Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
DOI:10.3390/tropicalmed9090215
Murine Extraparenchymal Neurocysticercosis: Appropriate Model for Evaluating Anthelminthic and Anti-Inflammatory Treatment Schedules
1 finding
Experimental models of neurocysticercosis (NCC) are helpful for an improved understanding of the pathophysiological mechanisms of human diseases and for testing novel therapeutic approaches.
"Experimental models of neurocysticercosis (NCC) are helpful for an improved understanding of the pathophysiological mechanisms of human diseases and for testing novel therapeutic approaches."
Show evidence (1 reference)
DOI:10.3390/tropicalmed9090215 SUPPORT Model Organism
"Experimental models of neurocysticercosis (NCC) are helpful for an improved understanding of the pathophysiological mechanisms of human diseases and for testing novel therapeutic approaches."
Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
DOI:10.3390/zoonoticdis4020013
Prevalence and Risk Factors of Human Taenia solium Cysticercosis in Mbulu District, Northern Tanzania
1 finding
Taeniosis and cysticercosis are human infections caused by the pork tapeworm, Taenia solium.
"Taeniosis and cysticercosis are human infections caused by the pork tapeworm, Taenia solium."
Show evidence (1 reference)
DOI:10.3390/zoonoticdis4020013 SUPPORT Human Clinical
"Taeniosis and cysticercosis are human infections caused by the pork tapeworm, Taenia solium."
Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
DOI:10.5772/intechopen.1004554
Neurocysticercosis and the Central Nervous System: Advancements in Diagnosis, Treatment, and Future Prospects
1 finding
Neurocysticercosis presents a formidable global health challenge.
"Neurocysticercosis presents a formidable global health challenge."
Show evidence (1 reference)
DOI:10.5772/intechopen.1004554 SUPPORT Other
"Neurocysticercosis presents a formidable global health challenge."
Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
DOI:10.5772/intechopen.110727
Epidemiology of Taeniosis/Cysticercosis in Humans and Animals
1 finding
Taenia saginata, Taenia solium, and Taenia asiatica popularly known as beef, pork, and Asian tapeworm, are important food-borne parasites.
"Taenia saginata, Taenia solium, and Taenia asiatica popularly known as beef, pork, and Asian tapeworm, are important food-borne parasites."
Show evidence (1 reference)
DOI:10.5772/intechopen.110727 SUPPORT Human Clinical
"Taenia saginata, Taenia solium, and Taenia asiatica popularly known as beef, pork, and Asian tapeworm, are important food-borne parasites."
Deep research cited this publication as relevant literature for Taeniasis Cysticercosis.
DOI:10.7759/cureus.64617
Effectiveness of the Antiparasitic Combination of Albendazole and Praziquantel As Compared With Albendazole Monotherapy in the Treatment of Neurocysticercosis in Children: A Systematic Review and Meta-Analysis
1 finding
Effectiveness of the Antiparasitic Combination of Albendazole and Praziquantel As Compared With Albendazole Monotherapy in the Treatment of Neurocysticercosis in Children: A Systematic Review and Meta-Analysis
"Effectiveness of the Antiparasitic Combination of Albendazole and Praziquantel As Compared With Albendazole Monotherapy in the Treatment of Neurocysticercosis in Children: A Systematic Review and Meta-Analysis"

Deep Research

1
Falcon
Disease Characteristics Research Template
Edison Scientific Literature 68 citations 2026-04-04T17:09:12.996470

Question: You are an expert researcher providing comprehensive, well-cited information.

Provide detailed information focusing on: 1. Key concepts and definitions with current understanding 2. Recent developments and latest research (prioritize 2023-2024 sources) 3. Current applications and real-world implementations 4. Expert opinions and analysis from authoritative sources 5. Relevant statistics and data from recent studies

Format as a comprehensive research report with proper citations. Include URLs and publication dates where available. Always prioritize recent, authoritative sources and provide specific citations for all major claims.

Disease Characteristics Research Template

Target Disease

  • Disease Name: Taeniasis/cysticercosis
  • MONDO ID: (if available)
  • Category: Infectious Disease

Research Objectives

Please provide a comprehensive research report on Taeniasis/cysticercosis covering all of the disease characteristics listed below. This report will be used to populate a disease knowledge base entry. Be thorough and cite primary literature (PMID preferred) for all claims.

For each section, suggested databases/resources are listed. These are the first places you should search for information on each topic.

1. Disease Information

Search first: OMIM, Orphanet, ICD-10/ICD-11, MeSH, PubMed

  • What is the disease? Provide a concise overview.
  • What are the key identifiers? (OMIM, Orphanet, ICD-10/ICD-11, MeSH, Mondo)
  • What are the common synonyms and alternative names?
  • Is the information derived from individual patients (e.g., EHR) or aggregated disease-level resources?

2. Etiology

  • Disease Causal Factors: What are the primary causes? (genetic, environmental, infectious, mechanistic)
  • Risk Factors:

    Search first: PubMed, Cochrane Library, UpToDate, clinical guidelines, ClinVar, ClinGen, GWAS Catalog, PheGenI, CTD, CDC, WHO, epidemiological databases

  • Genetic risk factors (causal variants, susceptibility loci, modifier genes)
  • Environmental risk factors (toxins, lifestyle, occupational exposures, age, sex, family history)
  • Protective Factors:

    Search first: PubMed, Cochrane Library, clinical trial databases, GWAS Catalog, gnomAD, WHO, CDC, nutrition databases

  • Genetic protective factors (protective variants, modifier alleles)
  • Environmental protective factors (diet, lifestyle, exposures that reduce risk)
  • Gene-Environment Interactions: How do genetic and environmental factors interact to influence disease?

    Search first: CTD, PubMed, PheGenI, GxE databases

3. Phenotypes

Search first: HPO (Human Phenotype Ontology), OMIM, Orphanet, PubMed, clinicaltrials.gov, MedDRA, SNOMED CT, DECIPHER, LOINC

For each phenotype, provide: - Phenotype type: symptoms, clinical signs, physical manifestations, behavioral changes, or laboratory abnormalities

For symptoms/signs: HPO, OMIM, Orphanet, PubMed For behavioral changes: HPO, DSM, RDoC (Research Domain Criteria), PubMed For laboratory abnormalities: LOINC, SNOMED CT, LabTests Online, PubMed - Phenotype characteristics: Search first: OMIM, Orphanet, HPO, PubMed - Age of symptom onset (neonatal, childhood, adult-onset, late-onset) - Symptom severity (mild, moderate, severe, variable) - Symptom progression (stable, progressive, episodic, fluctuating) - Frequency among affected individuals (percentage or qualitative) - Quality of life impact: Effects on daily functioning and well-being (per-phenotype when possible) Search first: EQ-5D database, SF-36, WHO QOL databases, PubMed - Suggest HPO (Human Phenotype Ontology) terms for each phenotype

4. Genetic/Molecular Information

  • Causal Genes: Gene mutations or chromosomal abnormalities responsible for disease (gene symbols, OMIM IDs)

    Search first: OMIM, ClinVar, HGMD, Ensembl, NCBI Gene

  • Pathogenic Variants:
  • Affected genes (gene symbols, HGNC IDs) > Search first: OMIM, NCBI Gene, Ensembl, HGNC, UniProt, GeneCards
  • Variant classification (pathogenic, likely pathogenic, VUS per ACMG/AMP guidelines) > Search first: ClinVar, ClinGen, ACMG/AMP guidelines, VarSome
  • Variant type/class (missense, frameshift, nonsense, splice-site, structural)
  • Allele frequency in population databases > Search first: gnomAD, 1000 Genomes, ExAC, TOPMed, dbSNP
  • Somatic vs germline origin > Search first: COSMIC (somatic), ClinVar, ICGC, TCGA
  • Functional consequences (loss of function, gain of function, dominant negative)
  • Modifier Genes: Genes that modify disease severity or expression
  • Epigenetic Information: DNA methylation, histone modifications, chromatin changes affecting disease

    Search first: ENCODE, Roadmap Epigenomics, MethBase, DiseaseMeth

  • Chromosomal Abnormalities: Large-scale genetic changes (aneuploidy, translocations, inversions)

    Search first: DECIPHER, ClinVar, ECARUCA, UCSC Genome Browser

5. Environmental Information

  • Environmental Factors: Non-genetic contributing factors (toxins, radiation, pollution, occupational exposure)

    Search first: CTD (Comparative Toxicogenomics Database), TOXNET, PubMed, EPA databases

  • Lifestyle Factors: Behavioral factors (smoking, diet, exercise, alcohol consumption)

    Search first: CDC databases, WHO, PubMed, NHANES

  • Infectious Agents: If applicable, pathogens causing or triggering disease (bacteria, viruses, fungi, parasites)

    Search first: NCBI Taxonomy, ViPR, BV-BRC, MicrobeDB, GIDEON

6. Mechanism / Pathophysiology

  • Molecular Pathways: Specific signaling cascades or biochemical pathways involved (Wnt, MAPK, mTOR, PI3K-AKT, etc.)

    Search first: KEGG, Reactome, WikiPathways, PathBank, BioCyc

  • Cellular Processes: Cell-level mechanisms (apoptosis, autophagy, cell cycle dysregulation, inflammation, etc.)

    Search first: Gene Ontology (GO), Reactome, KEGG, PubMed

  • Protein Dysfunction: How protein structure or function is altered (misfolding, aggregation, loss of function, gain of function)

    Search first: UniProt, PDB (Protein Data Bank), InterPro, Pfam, AlphaFold

  • Metabolic Changes: Alterations in metabolic processes (energy metabolism, lipid metabolism, amino acid metabolism)

    Search first: KEGG, BioCyc, HMDB (Human Metabolome Database), BRENDA

  • Immune System Involvement: Role of immune response (autoimmunity, immunodeficiency, chronic inflammation)

    Search first: ImmPort, Immunome Database, IEDB, Gene Ontology

  • Tissue Damage Mechanisms: How tissues/ are injured (oxidative stress, ischemia, fibrosis, necrosis)

    Search first: PubMed, Gene Ontology, Reactome

  • Biochemical Abnormalities: Specific molecular defects (enzyme deficiencies, receptor dysfunction, ion channel defects)

    Search first: BRENDA, UniProt, KEGG, OMIM, PubMed

  • Epigenetic Changes: DNA methylation, histone modifications affecting gene expression in disease

    Search first: ENCODE, Roadmap Epigenomics, MethBase, DiseaseMeth

  • Molecular Profiling (if available):
  • Transcriptomics/gene expression changes > Search first: GEO (Gene Expression Omnibus), ArrayExpress, GTEx, Human Cell Atlas, SRA
  • Proteomics findings > Search first: PRIDE, ProteomeXchange, Human Protein Atlas, STRING, BioGRID
  • Metabolomics signatures > Search first: MetaboLights, Metabolomics Workbench, HMDB, METLIN
  • Lipidomics alterations > Search first: LIPID MAPS, SwissLipids, LipidHome, Metabolomics Workbench
  • Genomic structural features > Search first: UCSC Genome Browser, Ensembl, NCBI, dbVar, DGV
  • Advanced Technologies (if applicable):
  • Single-cell analysis findings (cell-type specific mechanisms, cellular heterogeneity) > Search first: Human Cell Atlas, Single Cell Portal, GEO, CELLxGENE
  • Spatial transcriptomics findings > Search first: GEO, Spatial Research, Vizgen, 10x Genomics data
  • Multi-omics integration results > Search first: TCGA, ICGC, cBioPortal, LinkedOmics, PubMed
  • Functional genomics screens (CRISPR, RNAi) > Search first: DepMap, GenomeRNAi, PubMed, BioGRID ORCS

For each mechanism, describe: - The causal chain from initial trigger to clinical manifestation - Which mechanisms are upstream vs downstream - What cell types and biological processes are involved - Suggest GO terms for biological processes and CL terms for cell types

7. Anatomical Structures Affected

  • Organ Level:
  • Primary organs directly affected
  • Secondary organ involvement (complications, secondary effects)
  • Body systems involved (cardiovascular, nervous, digestive, respiratory, endocrine, etc.)

    Search first: Uberon, FMA (Foundational Model of Anatomy), OMIM, HPO, ICD-11, MeSH, SNOMED CT

  • Tissue and Cell Level:
  • Specific tissue types affected (epithelial, connective, muscle, nervous)
  • Specific cell populations targeted (with Cell Ontology terms)

    Search first: Uberon, Human Protein Atlas, Cell Ontology, Human Cell Atlas, CellMarker, PanglaoDB

  • Subcellular Level:
  • Cellular compartments involved (mitochondria, nucleus, ER, lysosomes) (with GO Cellular Component terms)

    Search first: Gene Ontology (Cellular Component), UniProt, Human Protein Atlas

  • Localization:
  • Specific anatomical sites (with UBERON terms) > Search first: FMA, Uberon, NeuroNames (for brain), SNOMED CT
  • Lateralization (unilateral, bilateral, asymmetric) > Search first: HPO, clinical literature, imaging databases

8. Temporal Development

  • Onset:
  • Typical age of onset (congenital, pediatric, adult, geriatric)
  • Onset pattern (acute, subacute, chronic, insidious)

    Search first: OMIM, Orphanet, HPO, PubMed

  • Progression:
  • Disease stages (early, intermediate, advanced, end-stage) > Search first: Cancer Staging Manual (AJCC), WHO classifications, PubMed
  • Progression rate (rapid, slow, variable)
  • Disease course pattern (episodic, relapsing-remitting, progressive, stable)
  • Disease duration (self-limited, chronic lifelong)

    Search first: Disease registries, longitudinal cohort databases, natural history studies, PubMed, Orphanet, OMIM

  • Patterns:
  • Remission patterns (spontaneous, treatment-induced) > Search first: Clinical trial databases, disease registries, PubMed
  • Critical periods (time windows of vulnerability or opportunity for intervention) > Search first: PubMed, developmental biology databases, clinical guidelines

9. Inheritance and Population

  • Epidemiology:
  • Prevalence (cases per 100,000 at given time)
  • Incidence (new cases per 100,000 per year)

    Search first: Orphanet, CDC, WHO, GBD (Global Burden of Disease), national registries, SEER, disease registries

  • For Genetic Etiology:
  • Inheritance pattern (AD, AR, X-linked, mitochondrial, multifactorial, polygenic) > Search first: OMIM, Orphanet, ClinVar, GTR (Genetic Testing Registry)
  • Penetrance (complete, incomplete, age-dependent) > Search first: ClinVar, OMIM, PubMed, ClinGen
  • Expressivity (variable, consistent) > Search first: OMIM, ClinVar, PubMed
  • Genetic anticipation (increasing severity in successive generations) > Search first: OMIM, PubMed (especially for repeat expansion disorders)
  • Germline mosaicism > Search first: ClinVar, OMIM, genetic counseling literature, PubMed
  • Founder effects (population-specific mutations) > Search first: gnomAD, population genetics databases, PubMed
  • Consanguinity role > Search first: OMIM, population studies, genetic counseling resources
  • Carrier frequency > Search first: gnomAD, carrier screening databases, GeneReviews, GTR
  • Population Demographics:
  • Affected populations (ethnic or demographic groups with higher prevalence) > Search first: gnomAD, 1000 Genomes, PAGE Study, PubMed, population registries
  • Geographic distribution (endemic areas, regional variation) > Search first: WHO, CDC, GBD, Orphanet, geographic epidemiology databases
  • Geographic distribution of specific variants
  • Sex ratio (male:female) > Search first: Disease registries, OMIM, PubMed, epidemiological databases
  • Age distribution of affected individuals > Search first: CDC, disease registries, SEER, Orphanet

10. Diagnostics

  • Clinical Tests:
  • Laboratory tests (blood, urine, tissue chemistry, specific enzyme assays) > Search first: LOINC, LabTests Online, PubMed
  • Biomarkers (proteins, metabolites, genetic markers, circulating biomarkers) > Search first: FDA Biomarker List, BEST (Biomarkers, EndpointS, and other Tools), PubMed
  • Imaging studies (X-ray, CT, MRI, PET, ultrasound) > Search first: RadLex, DICOM, Radiopaedia, imaging databases
  • Functional tests (pulmonary function, cardiac stress tests) > Search first: LOINC, clinical guidelines, PubMed
  • Electrophysiology (EEG, EMG, ECG, nerve conduction studies) > Search first: LOINC, clinical neurophysiology databases, PubMed
  • Biopsy findings (histopathology, immunohistochemistry) > Search first: SNOMED CT, College of American Pathologists resources, PubMed
  • Pathology findings (microscopic examination) > Search first: SNOMED CT, Digital Pathology databases, PubMed
  • Genetic Testing:

    Search first: GTR (Genetic Testing Registry), GeneReviews, ClinGen

  • Overview of recommended genetic testing approach
  • Whole genome sequencing (WGS) utility > Search first: GTR, ClinVar, GEL (Genomics England), gnomAD
  • Whole exome sequencing (WES) utility > Search first: GTR, ClinVar, OMIM, GeneMatcher
  • Gene panels (which panels, which genes) > Search first: GTR, ClinVar, laboratory-specific databases
  • Single gene testing > Search first: GTR, ClinVar, OMIM, GeneReviews
  • Chromosomal microarray (CMA) > Search first: DECIPHER, ClinVar, dbVar, ECARUCA
  • Karyotyping > Search first: Chromosome Abnormality Database, ClinVar, cytogenetics resources
  • FISH > Search first: ClinVar, cytogenetics databases, PubMed
  • Mitochondrial DNA testing > Search first: MITOMAP, MSeqDR, ClinVar, GTR
  • Repeat expansion testing > Search first: GTR, ClinVar, repeat expansion databases, PubMed
  • Omics-Based Diagnostics (if applicable):
  • RNA sequencing / transcriptomics > Search first: GEO, ArrayExpress, GTEx, RNA-seq databases
  • Proteomics > Search first: PRIDE, ProteomeXchange, FDA Biomarker database
  • Metabolomics > Search first: MetaboLights, Metabolomics Workbench, HMDB
  • Epigenomics > Search first: GEO, ENCODE, Roadmap Epigenomics, MethBase
  • Liquid biopsy > Search first: COSMIC, ClinVar, liquid biopsy databases, PubMed
  • Clinical Criteria:
  • Standardized diagnostic criteria (DSM, ICD, society guidelines) > Search first: DSM-5, ICD-11, clinical society guidelines, UpToDate
  • Differential diagnosis (other conditions to rule out, with distinguishing features) > Search first: DynaMed, UpToDate, clinical decision support systems
  • Screening:
  • Screening methods for asymptomatic individuals (newborn screening, carrier screening, cascade screening) > Search first: ACMG recommendations, CDC newborn screening, GTR

11. Outcome/Prognosis

  • Survival and Mortality:
  • Survival rate (5-year, 10-year, overall) > Search first: SEER, cancer registries, disease-specific registries, PubMed
  • Life expectancy (with and without treatment if applicable) > Search first: Orphanet, disease registries, actuarial databases, PubMed
  • Mortality rate > Search first: CDC, WHO, GBD, national mortality databases
  • Disease-specific mortality (deaths directly attributable to disease) > Search first: Disease registries, CDC Wonder, GBD, PubMed
  • Morbidity and Function:
  • Morbidity (disease-related disability and health impacts) > Search first: GBD, WHO, disability databases, PubMed
  • Disability outcomes (long-term functional impairments) > Search first: ICF (International Classification of Functioning), disability registries
  • Quality of life measures (EQ-5D, SF-36, PROMIS, disease-specific tools) > Search first: EQ-5D database, SF-36, PROMIS, PubMed
  • Disease Course:
  • Complications (secondary problems: infections, organ failure, etc.) > Search first: ICD codes, disease registries, clinical databases, PubMed
  • Recovery potential (likelihood and extent of recovery, with vs without treatment) > Search first: Natural history studies, rehabilitation databases, PubMed
  • Prediction:
  • Prognostic factors (age, disease severity, biomarkers, treatment response) > Search first: Prognostic models databases, clinical calculators, PubMed
  • Prognostic biomarkers (molecular markers predicting disease course) > Search first: FDA Biomarker database, PubMed, cancer prognostic databases

12. Treatment

  • Pharmacotherapy:
  • Pharmacological treatments (drug names, drug classes, mechanisms of action) > Search first: DrugBank, RxNorm, ATC classification, DailyMed, FDA databases
  • Pharmacogenomics (how genetic variants affect drug metabolism, efficacy, toxicity) > Search first: PharmGKB, CPIC (Clinical Pharmacogenetics), FDA Table of PGx Biomarkers
  • Advanced Therapeutics:
  • Gene therapy (viral vectors, CRISPR, gene replacement, gene editing) > Search first: ClinicalTrials.gov, FDA gene therapy database, ASGCT resources
  • Cell therapy (stem cell transplant, CAR-T, cellular therapeutics) > Search first: ClinicalTrials.gov, FDA cell therapy database, FACT standards
  • RNA-based therapies (ASOs, siRNA, mRNA therapies) > Search first: ClinicalTrials.gov, FDA approvals, PubMed
  • Targeted therapies (treatments directed at specific molecular targets) > Search first: My Cancer Genome, OncoKB, ClinicalTrials.gov, FDA approvals
  • Immunotherapies (checkpoint inhibitors, monoclonal antibodies) > Search first: Cancer Immunotherapy Database, FDA approvals, ClinicalTrials.gov
  • Surgical and Interventional:
  • Surgical interventions (types of surgery, timing, outcomes) > Search first: CPT codes, surgical registries, clinical guidelines, PubMed
  • Supportive and Rehabilitative:
  • Supportive care (symptom management, pain control, nutrition) > Search first: Clinical guidelines, Cochrane Library, PubMed
  • Rehabilitation (physical therapy, occupational therapy, speech therapy) > Search first: Rehabilitation medicine databases, clinical guidelines, PubMed
  • Experimental:
  • Experimental treatments in clinical trials (with NCT identifiers if available) > Search first: ClinicalTrials.gov, EU Clinical Trials Register, WHO ICTRP
  • Treatment Outcomes:
  • Treatment response rates > Search first: Clinical trial databases, FDA reviews, systematic reviews, PubMed
  • Side effects and adverse events > Search first: FDA Adverse Event Reporting System (FAERS), MedWatch, PubMed
  • Treatment Strategy:
  • Treatment algorithms (clinical pathways, decision trees) > Search first: Clinical practice guidelines, NCCN Guidelines, UpToDate
  • Combination therapies > Search first: ClinicalTrials.gov, treatment guidelines, PubMed
  • Personalized medicine approaches (genotype-guided treatment) > Search first: My Cancer Genome, CIViC, PharmGKB, precision medicine databases

For each treatment, suggest MAXO (Medical Action Ontology) terms where applicable.

13. Prevention

  • Prevention Levels:
  • Primary prevention (preventing disease occurrence: vaccination, risk factor modification) > Search first: CDC, WHO, USPSTF recommendations, Cochrane Library
  • Secondary prevention (early detection and treatment: screening programs, early intervention) > Search first: USPSTF, CDC screening guidelines, WHO
  • Tertiary prevention (preventing complications in those with disease) > Search first: Clinical guidelines, disease management protocols, PubMed
  • Immunization: Vaccine strategies (if applicable)

    Search first: CDC vaccine schedules, WHO immunization, FDA vaccine database

  • Screening and Early Detection:
  • Screening programs (population-based: newborn screening, cancer screening) > Search first: CDC screening programs, USPSTF, cancer screening databases
  • Genetic screening (carrier screening, preimplantation genetic diagnosis, prenatal testing) > Search first: ACMG recommendations, ACOG guidelines, GTR
  • Risk stratification (identifying high-risk individuals for targeted prevention) > Search first: Risk prediction models, clinical calculators, PubMed
  • Behavioral Interventions: Lifestyle modifications to reduce risk

    Search first: CDC, WHO, behavioral intervention databases, Cochrane Library

  • Counseling: Genetic counseling (risk assessment, family planning guidance)

    Search first: NSGC resources, ACMG guidelines, GeneReviews

  • Public Health:
  • Public health interventions (sanitation, vector control, health education) > Search first: CDC, WHO, public health databases, PubMed
  • Environmental interventions (reducing environmental risk factors) > Search first: EPA databases, WHO environmental health, PubMed
  • Prophylaxis: Preventive medications or procedures

    Search first: Clinical guidelines, FDA approvals, PubMed

14. Other Species / Natural Disease

  • Taxonomy: Species affected (with NCBI Taxon identifiers)

    Search first: NCBI Taxonomy

  • Breed: Specific breeds affected (with VBO identifiers if applicable)

    Search first: VBO (Vertebrate Breed Ontology)

  • Gene: Orthologous genes in other species (with NCBI Gene IDs)

    Search first: NCBI Gene

  • Natural Disease:
  • Naturally occurring disease in other species (companion animals, wildlife) > Search first: OMIA (Online Mendelian Inheritance in Animals), VetCompass, PubMed
  • Veterinary relevance and importance in animal health > Search first: OMIA, veterinary databases, PubMed
  • Comparative Biology:
  • Comparative pathology (similarities and differences across species) > Search first: OMIA, comparative pathology databases, PubMed
  • Evolutionary conservation of disease mechanisms > Search first: HomoloGene, OrthoMCL, Alliance of Genome Resources
  • Transmission (if applicable):
  • Zoonotic potential > Search first: CDC zoonotic diseases, WHO zoonoses, GIDEON
  • Cross-species susceptibility > Search first: NCBI Taxonomy, veterinary databases, PubMed

15. Model Organisms

  • Model Types:
  • Model organism type (mammalian, invertebrate, cellular, in vitro) > Search first: Alliance of Genome Resources, model organism databases
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  • Genetic Models:
  • Types available (knockout, knock-in, transgenic, conditional, humanized) > Search first: MGI, IMPC, KOMP, EuMMCR, IMSR
  • Model Characteristics:
  • Phenotype recapitulation (how well model reproduces human disease features) > Search first: Model organism databases, comparative studies, PubMed
  • Model limitations (aspects of human disease not captured) > Search first: Model organism databases, PubMed, review articles
  • Applications:
  • Research applications (what aspects of disease can be studied) > Search first: Model organism databases, PubMed
  • Resources:
  • Model databases > Search first: MGI, RGD, ZFIN, FlyBase, WormBase, IMSR, EMMA, MMRRC

Citation Requirements

  • Cite primary literature (PMID preferred) for all mechanistic and clinical claims
  • Prioritize recent reviews and landmark papers
  • Include direct quotes from abstracts where possible to support key statements
  • Distinguish evidence source types: human clinical, model organism, in vitro, computational

Output Format

Structure your response as a comprehensive narrative organized by the sections above. For each section, provide: - Factual content with specific details (numbers, percentages, gene names, variant nomenclature) - Ontology term suggestions (HPO, GO, CL, UBERON, CHEBI, MAXO, MONDO) where applicable - Evidence citations with PMIDs - Direct quotes from abstracts to support key claims - Clear indication when information is not available or not applicable for this disease

This report will be used to populate a disease knowledge base entry with: - Pathophysiology descriptions with causal chains - Gene/protein annotations (HGNC, GO terms) - Phenotype associations (HP terms) with frequencies - Cell type involvement (CL terms) - Anatomical locations (UBERON terms) - Chemical entities (CHEBI terms) - Treatment annotations (MAXO terms) - Evidence items with PMIDs and exact abstract quotes - Epidemiology, prognosis, diagnostic, and prevention information - Animal model descriptions with phenotype recapitulation details

Comprehensive Disease Characteristics Research Report: Taeniasis/Cysticercosis (Taenia solium disease complex)

Executive summary (2023–2024 emphasis)

Taeniasis/cysticercosis is a zoonotic, food- and fecal–oral–transmitted disease complex caused primarily by Taenia solium (pork tapeworm) in which humans act as definitive hosts (intestinal tapeworm; taeniasis) and can also become accidental intermediate hosts (tissue cysticercosis), including infection of the central nervous system (neurocysticercosis; NCC). The most important clinical burden arises from NCC-associated seizures/epilepsy and complications of extraparenchymal disease such as hydrocephalus. Recent (2023–2024) work highlights (i) persistent high community prevalence in parts of sub-Saharan Africa with many asymptomatic infections, (ii) improving but still limited diagnostic accessibility, with multiple high-performing immunodiagnostic platforms under validation, (iii) strong effectiveness signals for albendazole + praziquantel combination regimens in active disease, and (iv) increasing real‑world implementation evidence for mass treatment of taeniasis with niclosamide as a transmission-interruption tool. (zulu2023theepidemiologyof pages 1-2, larkins2023thechallengesof pages 1-2, acker2024accuracyofimmunological pages 7-10, stelzle2023efficacyandsafety pages 1-2, wardle2024masschemotherapywith pages 1-2, zulu2024neurocysticercosisprevalenceand pages 1-2)

Domain Key finding/statistic Setting/population Notes on methods Source (author year journal) URL/DOI
Definition Taenia solium causes taeniosis in humans (adult intestinal tapeworm) and cysticercosis in humans and pigs; neurocysticercosis (NCC) is CNS infection by larval cysticerci and is a major cause of epilepsy in endemic regions (zulu2023theepidemiologyof pages 1-2, larkins2023thechallengesof pages 1-2, aderinto2024neurocysticercosisandthe pages 1-2) Human and pig host cycle; endemic LMIC settings Review/systematic-review definitions synthesizing host roles and transmission biology Zulu 2023 PLoS Negl Trop Dis; Larkins 2023 Trop Med Int Health https://doi.org/10.1371/journal.pntd.0011042 ; https://doi.org/10.1111/tmi.13870
Epidemiology In Sinda District, Zambia, cysticercosis seroprevalence was estimated at 20.1% and NCC prevalence at 13.5%; among people reporting epileptic seizures, NCC prevalence was 38.0% (omeragic2024epidemiologyoftaeniosiscysticercosis pages 6-8) 1,249 community participants with POC testing; 233 received CT Cross-sectional study with TS POC screening followed by clinical evaluation and cerebral CT Zulu 2024 J Epidemiol Glob Health https://doi.org/10.1007/s44197-024-00271-z
Epidemiology In Starr County, Texas, cysticercosis seroprevalence was 7.4% (45/605); calcified NCC-compatible lesions were found in 2/45 seropositive individuals (omeragic2024epidemiologyoftaeniosiscysticercosis pages 6-8) Mexican-American adults on the Texas–Mexico border Cross-sectional serosurvey with follow-up brain imaging among seropositive participants Duffey 2024 Pathogens https://doi.org/10.3390/pathogens13110988
Epidemiology In Mbulu District, Tanzania, human cysticercosis prevalence was 7.67% (23/300); infection tended to be lower among prior anthelmintic users, though not statistically significant (omeragic2024epidemiologyoftaeniosiscysticercosis pages 6-8) Community participants aged 5–89 years Baseline community study using Ag-ELISA plus household risk-factor assessment Bandi 2024 Zoonotic Diseases https://doi.org/10.3390/zoonoticdis4020013
Epidemiology Eastern and Southern Africa review found wide ranges: cysticercosis seroprevalence 0.7–40.8% by Ag-ELISA, 13.1–45.3% by Ab-ELISA; taeniosis prevalence by microscopy 0.1–14.7%; NCC-suggestive CT lesions 1.0–76% (zulu2023theepidemiologyof pages 1-2, zulu2023theepidemiologyof pages 9-10) 16 of 27 countries in Eastern/Southern Africa Systematic review of 113 reports (2000–2022 literature) highlighting large geographic heterogeneity and surveillance gaps Zulu 2023 PLoS Negl Trop Dis https://doi.org/10.1371/journal.pntd.0011042
Phenotype Seizures were the most frequent presentation in European NCC cases: 59% overall in abstracted cases; headache occurred in 52%; other neurological signs/symptoms in 54%; outcome favorable in 90% (stelzle2023clinicalcharacteristicsand pages 6-10) 293 NCC cases diagnosed/treated in Europe (2000–2019) Retrospective assessment of published and unpublished cases; all had neuroimaging Stelzle 2023 J Travel Med https://doi.org/10.1093/jtm/taac102
Phenotype Across updated 2008–2023 NCC literature, epileptic seizures and headache remained the most frequent manifestations; pooled headache frequency increased to 45.1% versus 36.2% in earlier review (figuet2024distributiondesmanifestations pages 85-90, figuet2024distributiondesmanifestationsa pages 85-90) People diagnosed with NCC across 63 included studies Systematic review/meta-analysis; mortality too heterogeneous to pool; limited longitudinal natural-history data Figuet 2024 systematic review/meta-analysis Not available in gathered evidence
Phenotype/Pathophysiology In a large Peru calcified NCC cohort, 79.2% had previous seizures; median number of calcifications was 3 and frontal lobe location was most common (79%) (bustos2023calcifiedneurocysticercosisdemographic pages 2-4) 524 hospital-based patients with calcified NCC in Peru Cohort of CT-defined calcified NCC; combined clinical, imaging, EEG, and serology/antigen testing Bustos 2023 Pathogens https://doi.org/10.3390/pathogens13010026
Diagnostics Neuroimaging (CT/MRI) remains the definitive modality for NCC diagnosis; immunological tests are supportive, especially where imaging access is limited (toribio2024fromlaboratoryto pages 1-2, toribio2024fromlaboratoryto pages 11-12) Endemic/resource-limited settings and specialty centers 2024 diagnostic review summarizing clinical translation of immunologic and molecular tools Toribio 2024 Front Parasitol https://doi.org/10.3389/fpara.2024.1394089
Diagnostics LLGP Western blot showed high sensitivity for parenchymal active multiple cysts (81.1–100%) but much lower sensitivity for single cysts (<62.6%); specificity was 92.3–100% (acker2024accuracyofimmunological pages 7-10) Studies mainly from South America and South/Southeast Asia 2024 systematic review of 53 studies / 123 tests; major heterogeneity and risk-of-bias issues Van Acker 2024 PLoS Negl Trop Dis https://doi.org/10.1371/journal.pntd.0012643
Diagnostics A multi-antigen print immunoassay (MAPIA) reported 100% sensitivity for active single and multiple parenchymal cysts and 98.5% specificity, though based on small samples (acker2024accuracyofimmunological pages 10-11) NCC diagnostic studies Promising assay under evaluation; not yet established as routine standard Van Acker 2024 PLoS Negl Trop Dis https://doi.org/10.1371/journal.pntd.0012643
Diagnostics DOT-ELISA and urine-based tests showed promising performance: e.g., urine dipstick sensitivity 96.7% and specificity 100.0% in subarachnoid NCC controls, but further validation is needed (acker2024accuracyofimmunological pages 22-23) Subarachnoid/extraparenchymal-focused diagnostic subsets Review of rapid/POC and alternative-antigen assays; implementation evidence still limited Van Acker 2024 PLoS Negl Trop Dis https://doi.org/10.1371/journal.pntd.0012643
Treatment In rural Tanzania, albendazole monotherapy resolved or calcified 42% of 138 cysts by end of follow-up; among patients later receiving albendazole + praziquantel, 63 of 66 cysts (95%) resolved; seizure frequency declined significantly (p<0.001), with infrequent mild–moderate adverse events (stelzle2023clinicalcharacteristicsand pages 6-10) 63 NCC patients in Tanzania; 17 completed albendazole-only follow-up, 8 received combination therapy Prospective cohort, 2018–2022; antiparasitic therapy accompanied by corticosteroids and anti-seizure medication as indicated Stelzle 2023 Infection https://doi.org/10.1007/s15010-023-02021-y
Treatment Pediatric systematic review found higher complete lesion resolution with albendazole + praziquantel than albendazole alone: 62% vs 26.3% at 6 months in one trial (dewi2024effectivenessofthe pages 4-5) Children with NCC in randomized comparative studies 2024 systematic review/meta-analysis of pediatric evidence; lesion resolution and calcification outcomes extracted Dewi 2024 Cureus https://doi.org/10.7759/cureus.64617
Treatment/Surgery For hydrocephalus in extraparenchymal NCC, endoscopic third ventriculostomy reported symptom resolution in 70–95%; shunt/endoscopy choice depends on anatomy and local expertise (filho2024currentroleof pages 4-6, filho2024currentroleof media 744e0baf) Patients with hydrocephalus/intraventricular or extraparenchymal NCC Narrative surgical review; figures illustrate VP shunt failure versus successful endoscopic cyst removal/ETV Hamamoto Filho 2024 Pathogens https://doi.org/10.3390/pathogens13030218
Prevention/Control Mass niclosamide chemotherapy was evaluated as a safe and effective population-based control strategy for T. solium transmission (omeragic2024epidemiologyoftaeniosiscysticercosis pages 6-8) Population-based control program in the Americas 2024 field implementation study emphasizing taeniasis control to interrupt the life cycle Wardle 2024 Lancet Reg Health Am https://doi.org/10.1016/j.lana.2024.100876
Prevention/Control Community knowledge is often poor: in Thailand, 98.3% of respondents had less accurate knowledge despite many reporting generally correct preventive practices; older age and some municipal settings predicted poorer practice scores (omeragic2024epidemiologyoftaeniosiscysticercosis pages 6-8) 360 respondents in Pak Chong District, Thailand Cross-sectional KAP survey supporting education as a prevention pillar Phumrattanaprapin 2024 PLoS One https://doi.org/10.1371/journal.pone.0307240
Prevention/Control The Vicious Worm educational tool significantly improved community health worker knowledge on T. solium cysticercosis in Rwanda (omeragic2024epidemiologyoftaeniosiscysticercosis pages 6-8) 207 community health workers in Nyamagabe District, Rwanda Mixed-methods evaluation before, immediately after, and 4 weeks after training Uwibambe 2024 PLoS Negl Trop Dis https://doi.org/10.1371/journal.pntd.0012140
Trials NCT02612896 compared elimination vs control strategies in Zambia; elimination arm combined repeated human praziquantel MDA, health education, and pig treatment/vaccination; status completed; study completion Feb 2022 (NCT02612896 chunk 1, NCT02612896 chunk 2) ~2,900 participants in Katete district, Zambia Non-randomized parallel One Health community intervention with pig and human outcomes tracked over years Institute of Tropical Medicine Belgium, ClinicalTrials.gov 2016 https://clinicaltrials.gov/study/NCT02612896
Trials NCT02947581 (SANTO) tested albendazole + praziquantel vs albendazole + placebo for basal subarachnoid NCC; 107 enrolled; primary completion Aug 2020; terminated because placebo supply became unavailable (NCT02947581 chunk 2, NCT02947581 chunk 1) Adults 18–65 with subarachnoid NCC in Peru/Brazil/Ecuador sites Phase 3 double-blind randomized placebo-controlled trial; MRI parasite-volume reduction was the primary endpoint Universidad Peruana Cayetano Heredia, ClinicalTrials.gov 2016 https://clinicaltrials.gov/study/NCT02947581
Trials NCT01296958 evaluated targeted screening for intestinal T. solium tapeworm carriers plus niclosamide treatment versus community education; 1,811 enrolled; completed Jan 2013 (NCT01296958 chunk 1) Community members in Peru Non-randomized parallel screening/control strategy trial with porcine seroprevalence and tapeworm prevalence outcomes Oregon Health & Science University, ClinicalTrials.gov 2011 https://clinicaltrials.gov/study/NCT01296958

Table: This table compiles the most decision-relevant 2023-2024 evidence on Taenia solium taeniasis/cysticercosis/neurocysticercosis across definitions, epidemiology, phenotype, diagnostics, treatment, prevention, and interventional trials. It is useful as a concise evidence map for building a disease knowledge base entry or research summary.

1. Disease information

1.1 What is the disease? (definitions and scope)

Taeniasis is intestinal infection with the adult Taenia tapeworm in humans, acquired by eating raw/undercooked meat containing viable larval cysts (cysticerci). (larkins2023thechallengesof pages 1-2, aderinto2024neurocysticercosisandthe pages 8-9)

Cysticercosis is tissue infection with larval cysticerci acquired by ingestion of Taenia eggs; for T. solium, humans can become accidental intermediate hosts after ingesting eggs shed by a human tapeworm carrier. (aderinto2024neurocysticercosisandthe pages 1-2, aderinto2024neurocysticercosisandthe pages 8-9)

Neurocysticercosis (NCC) is cysticercosis involving the central nervous system (brain/spinal cord and associated spaces). NCC is emphasized as a leading (often preventable) cause of epilepsy in endemic regions. (zulu2023theepidemiologyof pages 1-2, larkins2023thechallengesof pages 1-2, aderinto2024neurocysticercosisandthe pages 7-8)

Direct abstract-supported statement (2024): “Neurocysticercosis (NCC) is caused by the invasion of Taenia solium larvae in the central nervous system (CNS) and stands as the predominant cause of epilepsy and other neurological disorders in many developing nations.” (toribio2024fromlaboratoryto pages 1-2)

1.2 Synonyms and alternative names

  • Taenia solium taeniasis/cysticercosis” (often abbreviated TSTC) (hossain2023insightsintothe pages 4-6)
  • “Human cysticercosis (HC/HCC)” for non-CNS tissue cysticercosis (zulu2023theepidemiologyof pages 1-2)
  • “Porcine cysticercosis (PCC)” for pig infection (hossain2023insightsintothe pages 4-6)

1.3 Key identifiers (ICD/MeSH/MONDO/Orphanet)

The retrieved full-text corpus used here did not include explicit ICD‑10/ICD‑11 codes, MeSH IDs, MONDO IDs, or Orphanet IDs in the accessible text excerpts. This is therefore a current evidence gap in this tool-backed retrieval run and should be supplemented from authoritative terminologies (WHO ICD-11 browser; NLM MeSH; MONDO/OBO Foundry; Orphanet) in a subsequent curation step. (zulu2023theepidemiologyof pages 1-2, toribio2024fromlaboratoryto pages 1-2)

1.4 Evidence source type

Information synthesized here is derived from aggregated disease-level resources (systematic reviews, narrative reviews, cohort/cross-sectional studies, and ClinicalTrials.gov registry records) rather than individual EHR-derived phenotyping. (zulu2023theepidemiologyof pages 1-2, acker2024accuracyofimmunological pages 7-10, NCT02947581 chunk 1)

2. Etiology

2.1 Causal factors

  • Infectious cause: Taenia solium (pork tapeworm) is the principal cause of the taeniasis/cysticercosis complex with major neurologic disease burden from NCC. (aderinto2024neurocysticercosisandthe pages 1-2, larkins2023thechallengesof pages 1-2)

2.2 Transmission and risk factors (gene–environment framing)

Core transmission biology: - Taeniasis follows ingestion of cysticerci in undercooked meat; cysticercosis follows ingestion of eggs, including via contaminated water/vegetables/hands/fomites. Eggs are infectious immediately and can persist for months under favorable conditions. (aderinto2024neurocysticercosisandthe pages 3-4, aderinto2024neurocysticercosisandthe pages 8-9) - Humans are definitive hosts for T. solium and can also act as intermediate hosts; pigs are key intermediate hosts for the zoonotic cycle. (aderinto2024neurocysticercosisandthe pages 1-2, zulu2023theepidemiologyof pages 1-2)

Environmental/behavioral risk factors emphasized in recent literature include inadequate sanitation, poor hygiene/handwashing infrastructure, unsafe water sources, and pig husbandry practices that permit pigs to access human feces/sewage—factors repeatedly invoked as drivers of household clustering and endemic persistence. (aderinto2024neurocysticercosisandthe pages 8-9, larkins2023thechallengesof pages 2-3, zulu2024neurocysticercosisprevalenceand pages 4-6)

Epidemiologic risk-factor estimate (2024, Zambia): small-scale farming was associated with higher odds of NCC (OR 5.28, 95% CI 1.56–17.86). (zulu2024neurocysticercosisprevalenceand pages 4-6)

2.3 Protective factors

Evidence in the retrieved texts supports protective effects of breaking transmission through: - Safe cooking/freezing of meat to kill cysticerci (e.g., cooking to ~60–65°C, freezing schedules) (aderinto2024neurocysticercosisandthe pages 3-4, aderinto2024neurocysticercosisandthe pages 8-9) - Treating human tapeworm carriers (taeniasis) and implementing One Health interventions targeting pigs and sanitation. (aderinto2024neurocysticercosisandthe pages 8-9, hossain2023insightsintothe pages 4-6)

A community study in Tanzania reported lower likelihood of cysticercosis among people who had taken anthelmintics, though this reduction was not statistically significant in that dataset. (omeragic2024epidemiologyoftaeniosiscysticercosis pages 6-8)

2.4 Genetic risk/protective factors and GxE

No robust human susceptibility loci, protective variants, or gene–environment interaction evidence was present in the retrieved excerpts; for this disease complex, the dominant drivers are infectious exposure and socio-environmental determinants. This is an evidence gap for the requested template. (zulu2023theepidemiologyof pages 1-2)

3. Phenotypes

3.1 Major clinical phenotypes and frequencies (humans)

Neurocysticercosis (NCC): - Seizures/epilepsy are the most frequent presentation. A large European retrospective assessment reported seizures as the initial presentation in 59% overall (and higher in children), with headache in 52% and other neurologic signs/symptoms in 54%; outcome was favorable in 90%. (stelzle2023clinicalcharacteristicsand pages 6-10) - A 2024 systematic review/meta-analysis (2008–2023) reported that seizures and headaches remain the most frequent manifestations; headache frequency in pooled summaries increased to 45.1% compared with 36.2% in an earlier period. (figuet2024distributiondesmanifestations pages 85-90)

Calcified NCC phenotype (Peru cohort): In a large hospital-based cohort of calcified NCC (n=524), 79.2% had previous seizures; calcifications were often frontal (79%); the cohort illustrates heterogeneity in burden and manifestations. (bustos2023calcifiedneurocysticercosisdemographic pages 2-4)

Population-level symptomatic fraction (2024, Zambia): In a community-based study, NCC prevalence was 13.5%, but only 16% of people with NCC had ever experienced epileptic seizures, emphasizing frequent asymptomatic infection. (zulu2024neurocysticercosisprevalenceand pages 1-2)

3.2 Phenotype characteristics (age of onset, severity, progression)

Progression is dominated by parasite stage and location: - Parenchymal cysts can be vesicular (often minimal inflammation) and later become degenerating lesions with inflammation/edema; eventual granuloma and calcification may persist lifelong and remain epileptogenic in some individuals. (singh2024seizuresandepilepsy pages 1-3, bustos2023calcifiedneurocysticercosisdemographic pages 1-2) - Extraparenchymal disease (subarachnoid/ventricular) is associated with raised intracranial pressure and hydrocephalus, often requiring neurosurgical intervention. (filho2024currentroleof pages 4-6, stelzle2023clinicalcharacteristicsand pages 6-10)

3.3 Suggested HPO terms (examples; ontology IDs to be confirmed during curation)

Based on the reported phenotypes, suggested HPO concepts include: - Seizures / Epileptic seizures; focal to bilateral tonic-clonic seizures (bustos2023calcifiedneurocysticercosisdemographic pages 2-4, stelzle2023clinicalcharacteristicsand pages 6-10) - Headache (stelzle2023clinicalcharacteristicsand pages 6-10) - Hydrocephalus / intracranial hypertension / papilledema (hydrocephalus is explicitly frequent in extraparenchymal disease; papilledema present in case descriptions) (stelzle2023clinicalcharacteristicsand pages 6-10, filho2024currentroleof pages 4-6) - Perilesional edema (imaging phenotype) (stelzle2023clinicalcharacteristicsand pages 6-10, singh2024seizuresandepilepsy pages 1-3) - Cognitive decline / higher brain function impairment (figuet2024distributiondesmanifestations pages 85-90, bustos2023calcifiedneurocysticercosisdemographic pages 1-2)

Because HPO IDs are not included in the retrieved texts, these are conceptual mappings requiring validation against the HPO database.

3.4 Quality-of-life impact

In a prospective Tanzania cohort, epilepsy-related quality of life (QOLIE-31) improved after treatment (median 87 to 95; p=0.02). (stelzle2023efficacyandsafety pages 7-10)

4. Genetic/Molecular information

4.1 Human causal genes and pathogenic variants

Not applicable in the classic Mendelian sense: taeniasis/cysticercosis is an infectious disease complex. No human causal genes/variants were provided in the retrieved evidence. (zulu2023theepidemiologyof pages 1-2)

4.2 Parasite molecular targets (contextual)

Recent diagnostics and control tools emphasize recombinant/synthetic antigens and monoclonal antibody targets for immunodiagnostics and vaccine development (e.g., pig vaccine TSOL18 is discussed in reviews), but specific gene symbols/IDs were not present in the retrieved excerpts. (hossain2023insightsintothe pages 4-6, toribio2024fromlaboratoryto pages 1-2)

5. Environmental information

Key environmental factors driving transmission are sanitation and water quality, and pig husbandry practices enabling fecal contamination of the environment and pig exposure. These factors are repeatedly cited as central to endemic persistence and a focus of One Health control. (aderinto2024neurocysticercosisandthe pages 8-9, zulu2024neurocysticercosisprevalenceand pages 4-6)

6. Mechanism / pathophysiology

6.1 Causal chain (upstream → downstream)

  1. Exposure: ingestion of eggs (→ cysticercosis) or cysticerci (→ taeniasis). (aderinto2024neurocysticercosisandthe pages 8-9)
  2. CNS invasion (NCC): larvae lodge in parenchyma, subarachnoid space, ventricles, or spinal cord. (singh2024seizuresandepilepsy pages 1-3)
  3. Stage-dependent host response: vesicular stage may have minimal inflammation; immune attack drives degeneration with enhancement and perilesional edema. (singh2024seizuresandepilepsy pages 1-3)
  4. Clinical manifestations: inflammatory edema and lesion location contribute to seizures; extraparenchymal disease contributes to arachnoiditis and CSF obstruction → hydrocephalus/intracranial hypertension. (singh2024seizuresandepilepsy pages 1-3, filho2024currentroleof pages 4-6)
  5. Long-term sequelae: calcified nodules can persist lifelong and remain seizure foci; mechanisms proposed include gliosis, blood–brain barrier disruption, and axonal damage. (bustos2023calcifiedneurocysticercosisdemographic pages 1-2, bustos2023calcifiedneurocysticercosisdemographic pages 2-4)

6.2 Mechanistic themes emphasized by authoritative 2023–2024 sources

  • A 2024 Neurology review links seizure occurrence to evolutionary stage, highlighting inflammation/edema in degenerating lesions and ongoing seizure risk even with calcified lesions. (singh2024seizuresandepilepsy pages 1-3)
  • Extraparenchymal NCC is increasingly recognized as proportionally more frequent and often more severe; medical therapy responses are variable and neurosurgical management is often required. (filho2024currentroleof pages 4-6)

6.3 Suggested GO biological process / CL cell types (conceptual)

The retrieved evidence points to inflammation and edema but does not enumerate specific immune pathways/cell subsets. Conceptual GO/CL mappings (requiring database validation) include: - GO: inflammatory response; leukocyte migration; regulation of cytokine production; blood–brain barrier organization/disruption (bustos2023calcifiedneurocysticercosisdemographic pages 2-4) - CL: microglia, astrocytes, endothelial cells, lymphocytes (inferred from “lymphocyte infiltration” and CNS inflammation discussions) (oliveira2024murineextraparenchymalneurocysticercosis pages 6-7)

No transcriptomics/proteomics/metabolomics signatures were available in the retrieved excerpts.

7. Anatomical structures affected

7.1 Organ-level and localization

  • CNS sites: brain parenchyma, subarachnoid space, ventricles, spinal cord. (singh2024seizuresandepilepsy pages 1-3)
  • Human cysticercosis can also involve muscle, subcutaneous tissue, eye, and other organs (reported as possible sites in reviews). (aderinto2024neurocysticercosisandthe pages 7-8)

UBERON suggestions (conceptual): brain, spinal cord, ventricular system, subarachnoid space/meninges, skeletal muscle, eye. (aderinto2024neurocysticercosisandthe pages 7-8, singh2024seizuresandepilepsy pages 1-3)

7.2 Subcellular localization

Not specified in retrieved excerpts.

8. Temporal development

  • Prepatent period for taeniid cestodes is noted as ~1–3 months; adult worms may live years. (aderinto2024neurocysticercosisandthe pages 3-4)
  • NCC lesion evolution over time follows vesicular → degenerating/colloidal with inflammation → granuloma → calcification; seizures may occur at any stage. (singh2024seizuresandepilepsy pages 1-3)

Detailed stage durations and longitudinal natural history remain poorly synthesized due to limited community-based longitudinal studies, as emphasized by a 2024 meta-analysis. (figuet2024distributiondesmanifestations pages 85-90)

9. Inheritance and population

9.1 Epidemiology (recent statistics)

Zambia (2024, community-based): - TS POC cysticercosis-positive: 14% (177/1249) - Estimated cysticercosis seroprevalence: 20.1% (95% CI 14.6–27.0) - NCC prevalence: 13.5% (95% CI 8.4–21.1) - Active NCC prevalence: 1.1% (95% CI 0.6–2.0) - NCC associated with higher odds of epileptic seizures: OR 3.98 (95% CI 1.34–11.78) (zulu2024neurocysticercosisprevalenceand pages 1-2, zulu2024neurocysticercosisprevalenceand pages 4-6)

Eastern & Southern Africa evidence base (systematic review, 2023): Cysticercosis seroprevalence and CT-based NCC lesion prevalence vary widely (Ag-ELISA up to 40.8%; NCC-suggestive CT lesions up to 76% in selected populations), indicating extreme heterogeneity and surveillance gaps. (zulu2023theepidemiologyof pages 1-2, zulu2023theepidemiologyof pages 9-10)

United States border community (2024): Cysticercosis seroprevalence 7.4% (45/605) in Starr County, Texas; calcified NCC-compatible lesions in 2/45 seropositive individuals. (omeragic2024epidemiologyoftaeniosiscysticercosis pages 6-8)

9.2 Demographics

In a large calcified NCC cohort in Peru, mean age at enrollment was ~40 years and symptom onset ~29 years; women comprised 56.3%. (bustos2023calcifiedneurocysticercosisdemographic pages 2-4)

10. Diagnostics

10.1 Clinical criteria and imaging

  • Neuroimaging (CT/MRI) is fundamental/definitive for NCC diagnosis; immunologic tests are supportive and may be limited by stage and access. (toribio2024fromlaboratoryto pages 1-2)
  • A 2024 Zambia community study applied revised Del Brutto criteria and staged lesions as active (vesicular/degenerating) vs inactive (calcified). (zulu2024neurocysticercosisprevalenceand pages 2-4)

10.2 Immunodiagnostics (2024 systematic review)

A 2024 systematic review synthesized 53 studies with 123 tests; major points include: - LLGP Western blot sensitivity 81.1–100% for parenchymal active multiple cysts, but <62.6% for single cysts; specificity 92.3–100%. (acker2024accuracyofimmunological pages 7-10) - A multi-antigen print immunoassay (MAPIA) reported 100% sensitivity for active single/multiple parenchymal cysts and 98.5% specificity (small-sample evidence). (acker2024accuracyofimmunological pages 10-11) - Antigen detection tests (including urine-based assays) showed high sensitivity for extraparenchymal disease in some studies (e.g., urine dipstick sensitivity 96.7%, specificity 100% in a small evaluation). (acker2024accuracyofimmunological pages 22-23)

10.3 Molecular diagnostics

Recent reviews describe exploration of molecular diagnostics, but quantitative performance data were not provided in the retrieved excerpts. (toribio2024fromlaboratoryto pages 11-12, toribio2024fromlaboratoryto pages 13-13)

10.4 Screening

Population screening strategies include point-of-care serology followed by targeted CT, as implemented in the Zambia study. (zulu2024neurocysticercosisprevalenceand pages 1-2)

11. Outcome / prognosis

  • In a European retrospective compilation, outcomes were favorable in 90% of cases. (stelzle2023clinicalcharacteristicsand pages 6-10)
  • Prognosis varies strongly by lesion location (parenchymal vs extraparenchymal), stage (active vs calcified), and complication burden (e.g., hydrocephalus). (filho2024currentroleof pages 4-6, singh2024seizuresandepilepsy pages 1-3)

Mortality estimates were too heterogeneous for pooling in a 2024 meta-analysis, underscoring gaps in standardized outcome reporting. (figuet2024distributiondesmanifestations pages 85-90)

12. Treatment

12.1 Pharmacotherapy (active NCC)

Albendazole ± praziquantel: - Tanzania prospective cohort (2023): albendazole monotherapy (15 mg/kg/day for 10 days) led to 58/138 cysts (42%) disappearing or calcifying by follow-up; median seizure frequency decreased from 4/year to 0/year (p<0.001). In those requiring escalation, albendazole + praziquantel (50 mg/kg/day) resolved 63/66 cysts (95%) and was generally well tolerated; combination therapy headaches occurred in 3/8 patients, with otherwise stable vitals/labs. (stelzle2023efficacyandsafety pages 1-2, stelzle2023efficacyandsafety pages 6-7) - Pediatric evidence synthesis (2024): in one trial summarized in a meta-analysis, complete lesion resolution at 6 months was 62% with albendazole + praziquantel versus 26.3% with albendazole monotherapy. (dewi2024effectivenessofthe pages 4-5)

Taeniasis treatment and preventive chemotherapy: Niclosamide is commonly used to treat intestinal tapeworm carriage and can be deployed at scale (see prevention/control). (NCT01296958 chunk 1, wardle2024masschemotherapywith pages 1-2)

12.2 Anti-inflammatory and supportive care

Corticosteroids are commonly paired with cysticidal therapy to mitigate inflammatory reactions; the Tanzania cohort used dexamethasone with albendazole and maintained/optimized anti-seizure medications. (stelzle2023efficacyandsafety pages 2-4)

12.3 Surgery and interventional management

Extraparenchymal NCC with hydrocephalus may require VP shunting or neuro-endoscopic procedures. - A 2024 surgical review reports endoscopic third ventriculostomy (ETV) symptom resolution in 70–95% and highlights the role of endoscopy for cyst removal when feasible; VP shunting remains important where endoscopy is unavailable. (filho2024currentroleof pages 4-6)

Visual evidence of shunt failure and endoscopic approaches is available from the same review. (filho2024currentroleof media 744e0baf, filho2024currentroleof media 298e5ac1)

12.4 Clinical trials (registry evidence)

Representative interventional trials include: - NCT02947581 (SANTO): Phase 3 randomized trial of albendazole + praziquantel vs albendazole + placebo for subarachnoid NCC; terminated due to drug unavailability; primary endpoint was MRI parasite-volume reduction. (NCT02947581 chunk 1) - NCT02612896: Completed community One Health intervention in Zambia comparing “elimination” vs “control” strategies with repeated praziquantel MDA plus pig interventions and education; completion Feb 2022. (NCT02612896 chunk 1) - NCT01296958: Completed targeted screening for tapeworm carriers with niclosamide treatment vs education in Peru. (NCT01296958 chunk 1)

12.5 MAXO (Medical Action Ontology) suggestions (conceptual)

  • Anthelmintic therapy (albendazole, praziquantel, niclosamide)
  • Corticosteroid therapy
  • Antiseizure medication therapy
  • Ventriculoperitoneal shunt placement
  • Neuroendoscopic cyst removal / endoscopic third ventriculostomy These mappings require MAXO term ID validation outside the retrieved corpus.

13. Prevention

13.1 Primary prevention (One Health)

  • Safe meat preparation and sanitation/hand hygiene reduce both taeniasis and cysticercosis risk. (aderinto2024neurocysticercosisandthe pages 8-9)
  • Treating tapeworm carriers is central to interrupting egg shedding into the environment. (aderinto2024neurocysticercosisandthe pages 8-9, wardle2024masschemotherapywith pages 1-2)

13.2 Real-world implementation: mass niclosamide chemotherapy (2024)

A 2024 implementation study in Tumbes, Peru delivered three niclosamide rounds at 4‑month intervals to 77,397 eligible residents (68,751 treated at least once). Active follow-up captured adverse events in 65,551 people: AE prevalence 1.5% (988/65,551), 99.2% mild, 0 severe; most common symptoms were abdominal discomfort (56.4%), headache (24.6%), tongue numbness (14.3%), and diarrhea (13.8%). Programmatic treatment effectiveness against confirmed taeniasis was 75.0% cure at ~30 days (141/188). (wardle2024masschemotherapywith pages 1-2, wardle2024masschemotherapywith pages 4-5)

13.3 Health education and behavior change tools

  • A Rwanda evaluation found “The Vicious Worm” education tool significantly improved community health worker knowledge about T. solium cysticercosis and maintained gains at 4 weeks, though implementation barriers included digital illiteracy and lack of smartphones. (omeragic2024epidemiologyoftaeniosiscysticercosis pages 6-8)
  • A Thailand KAP study identified widespread knowledge gaps (98.3% categorized as less accurate knowledge), supporting need for targeted education to complement structural interventions. (omeragic2024epidemiologyoftaeniosiscysticercosis pages 6-8)

14. Other species / natural disease

14.1 Zoonosis and cross-species susceptibility

Humans are the definitive host for T. solium and pigs are key intermediate hosts; humans can also become accidental intermediate hosts (cysticercosis/NCC) after egg ingestion, making this a zoonotic One Health disease complex. (aderinto2024neurocysticercosisandthe pages 1-2, zulu2023theepidemiologyof pages 1-2)

14.2 Veterinary and control relevance

Pig-directed interventions (vaccination + deworming) are discussed as efficient methods to reduce exposure and transmission, though detailed country-specific deployment and commercial availability vary. (hossain2023insightsintothe pages 4-6)

NCBI Taxon IDs for relevant species were not provided in the retrieved excerpts and require supplementation from NCBI Taxonomy.

15. Model organisms

A 2024 experimental model paper describes murine/rat extraparenchymal NCC modeling using Taenia crassiceps inoculated into the subarachnoid space to reproduce features relevant to human extraparenchymal NCC and to evaluate albendazole ± dexamethasone schedules, including changes in ventricular size and inflammatory markers (e.g., IL-6 immunopositivity). (oliveira2024murineextraparenchymalneurocysticercosis pages 6-7)

This model is positioned as useful for studying the inflammation–treatment tradeoff in extraparenchymal disease. (oliveira2024murineextraparenchymalneurocysticercosis pages 6-7)

Recent developments and expert analysis (2023–2024)

  1. Diagnostics are moving from parasite-derived antigens toward recombinant/synthetic platforms and point-of-care formats, motivated by limited neuroimaging access in endemic areas; 2024 systematic review evidence highlights high accuracy for LLGP western blot in multi-cyst disease but limited sensitivity in single-cyst presentations, reinforcing the need for multi-antigen or antigen-detection strategies. (acker2024accuracyofimmunological pages 7-10, toribio2024fromlaboratoryto pages 1-2, acker2024accuracyofimmunological pages 10-11)

  2. Combination antiparasitic therapy is increasingly supported by real-world cohort and pediatric meta-analysis evidence, with high lesion-resolution rates after albendazole + praziquantel and acceptable short-term tolerability when paired with anti-inflammatory regimens and close supervision. (stelzle2023efficacyandsafety pages 1-2, stelzle2023efficacyandsafety pages 6-7, dewi2024effectivenessofthe pages 4-5)

  3. Implementation science is emerging for taeniasis MDA: large-scale niclosamide MDA in Peru demonstrated strong safety and moderate single-dose effectiveness, with identified predictors of failure (age, high coproantigen), providing concrete parameters for program optimization. (wardle2024masschemotherapywith pages 4-5)

  4. Population studies underscore that many infections are asymptomatic, even in high-prevalence settings, and that epilepsy linkage is strong at the population level but not universal at the individual level—important for screening and cost-effectiveness modeling. (zulu2024neurocysticercosisprevalenceand pages 1-2)

Key limitations of this report (evidence gaps in retrieved corpus)

  • Formal ontology identifiers (ICD‑10/11, MeSH IDs, MONDO, Orphanet) were not present in the retrieved excerpts and therefore could not be tool-cited here.
  • Human genetic susceptibility, epigenetic mechanisms, and multi-omics profiling evidence were not captured in the accessible texts.
  • Some guideline algorithms and certain diagnostic accuracy studies were referenced (e.g., a 2024 Lancet Infectious Diseases POC test paper) but were unobtainable within this run; the report therefore emphasizes sources available in full-text excerpts. (toribio2024fromlaboratoryto pages 13-13)

Primary URLs (publication dates as captured in metadata)

  • Zulu et al. 2024-07, Journal of Epidemiology and Global Health (Zambia community NCC prevalence): https://doi.org/10.1007/s44197-024-00271-z (zulu2024neurocysticercosisprevalenceand pages 1-2)
  • Stelzle et al. 2023-03, Infection (Tanzania cohort therapy): https://doi.org/10.1007/s15010-023-02021-y (stelzle2023efficacyandsafety pages 1-2)
  • Van Acker et al. 2024-11, PLOS Neglected Tropical Diseases (diagnostic accuracy systematic review): https://doi.org/10.1371/journal.pntd.0012643 (acker2024accuracyofimmunological pages 7-10)
  • Wardle et al. 2024-10, The Lancet Regional Health – Americas (niclosamide MDA): https://doi.org/10.1016/j.lana.2024.100876 (wardle2024masschemotherapywith pages 1-2)
  • Hamamoto Filho et al. 2024-02, Pathogens (surgery review): https://doi.org/10.3390/pathogens13030218 (filho2024currentroleof pages 4-6)
  • ClinicalTrials.gov NCT02612896: https://clinicaltrials.gov/study/NCT02612896 (NCT02612896 chunk 1)
  • ClinicalTrials.gov NCT02947581: https://clinicaltrials.gov/study/NCT02947581 (NCT02947581 chunk 1)

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