Congenital sialidosis type 2 is the most severe, congenital-onset subtype of sialidosis type II (dysmorphic sialidosis), an autosomal recessive lysosomal storage disorder caused by biallelic NEU1 variants that abolish lysosomal neuraminidase-1 (alpha-N-acetyl neuraminidase/sialidase). Profound enzyme deficiency causes marked intracellular accumulation and urinary excretion of sialyloligosaccharides from before birth, producing nonimmune hydrops fetalis or neonatal ascites, coarse facies, hepatosplenomegaly, dysostosis multiplex, and severe neurological impairment, often with stillbirth or death in early infancy.
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Conditions with similar clinical presentations that must be differentiated from Congenital Sialidosis Type 2:
name: Congenital Sialidosis Type 2
creation_date: "2026-06-13T00:00:00Z"
description: >-
Congenital sialidosis type 2 is the most severe, congenital-onset subtype of sialidosis type II
(dysmorphic sialidosis), an autosomal recessive lysosomal storage disorder caused by biallelic
NEU1 variants that abolish lysosomal neuraminidase-1 (alpha-N-acetyl neuraminidase/sialidase).
Profound enzyme deficiency causes marked intracellular accumulation and urinary excretion of
sialyloligosaccharides from before birth, producing nonimmune hydrops fetalis or neonatal
ascites, coarse facies, hepatosplenomegaly, dysostosis multiplex, and severe neurological
impairment, often with stillbirth or death in early infancy.
category: Mendelian
disease_term:
preferred_term: congenital sialidosis type 2
term:
id: MONDO:0019682
label: congenital sialidosis type 2
mappings:
mondo_mappings:
- term:
id: MONDO:0019682
label: congenital sialidosis type 2
mapping_predicate: skos:exactMatch
mapping_source: MONDO
mapping_justification: Primary MONDO disease identifier for this congenital sialidosis type 2 entry.
synonyms:
- Congenital sialidosis
- Sialidosis type 2, congenital
- Hydropic sialidosis
parents:
- Lysosomal Storage Disorder
pathophysiology:
- name: Severe Neuraminidase-1 Deficiency
conforms_to: "lysosomal_substrate_accumulation#Lysosomal Hydrolase or Cofactor Deficiency"
description: >-
Biallelic NEU1 variants abolish lysosomal neuraminidase-1 (alpha-N-acetyl neuraminidase). The
profound deficiency of the congenital form prevents removal of terminal sialic acid from
sialoglycoconjugates from before birth.
gene:
preferred_term: NEU1
term:
id: hgnc:7758
label: NEU1
cell_types:
- preferred_term: fibroblast
term:
id: CL:0000057
label: fibroblast
evidence:
- reference: PMID:29693572
reference_title: "Sialidosis: A Review of Morphology and Molecular Biology of a Rare Pediatric Disorder."
supports: SUPPORT
evidence_source: HUMAN_CLINICAL
snippet: "caused by α-N-acetyl neuraminidase deficiency resulting from a mutation in\nthe neuraminidase gene (NEU1)"
explanation: "Sialidosis is caused by NEU1 (neuraminidase-1) deficiency."
- reference: PMID:26949572
reference_title: "Pathogenesis, Emerging therapeutic targets and Treatment in Sialidosis."
supports: SUPPORT
evidence_source: HUMAN_CLINICAL
snippet: "caused by mutations in the NEU1 gene, encoding the lysosomal sialidase NEU1"
explanation: "NEU1 encodes the lysosomal sialidase whose deficiency causes sialidosis."
downstream:
- target: Sialyloligosaccharide Lysosomal Accumulation
description: Loss of sialidase prevents desialylation, so sialylated substrates accumulate from before birth.
- name: Sialyloligosaccharide Lysosomal Accumulation
conforms_to: "lysosomal_substrate_accumulation#Lysosomal Substrate Accumulation"
description: >-
Without sialidase activity, sialylated oligosaccharides and glycopeptides accumulate markedly in
lysosomes (and are excreted in urine) from prenatal life, producing severe multisystem storage
disease with hydrops.
cell_types:
- preferred_term: fibroblast
term:
id: CL:0000057
label: fibroblast
cellular_components:
- preferred_term: lysosome
term:
id: GO:0005764
label: lysosome
biological_processes:
- preferred_term: oligosaccharide catabolic process
modifier: DECREASED
term:
id: GO:0009313
label: oligosaccharide catabolic process
evidence:
- reference: PMID:29693572
reference_title: "Sialidosis: A Review of Morphology and Molecular Biology of a Rare Pediatric Disorder."
supports: SUPPORT
evidence_source: HUMAN_CLINICAL
snippet: "This genetic alteration leads to abnormal intracellular accumulation as well as urinary excretion of"
explanation: "NEU1 deficiency causes intracellular accumulation and urinary excretion of sialyloligosaccharides."
downstream:
- target: Hydrops fetalis
description: Severe prenatal lysosomal storage can manifest as hydrops fetalis.
- target: Coarse facial features
description: Multisystem storage disease contributes to coarse facial features.
- target: Hepatosplenomegaly
description: Visceral lysosomal storage contributes to hepatosplenomegaly.
phenotypes:
- name: Hydrops fetalis
description: >-
Nonimmune hydrops fetalis or neonatal ascites is the defining presentation of the congenital
form, from severe prenatal storage.
phenotype_term:
preferred_term: Hydrops fetalis
term:
id: HP:0001789
label: Hydrops fetalis
evidence:
- reference: PMID:26949572
reference_title: "Pathogenesis, Emerging therapeutic targets and Treatment in Sialidosis."
supports: SUPPORT
evidence_source: HUMAN_CLINICAL
snippet: "Type II patients with the most acute, congenital form of the disease develop hydrops fetalis, neonatal ascites, or both"
explanation: Hydrops fetalis/neonatal ascites defines the most acute congenital form of sialidosis type II.
- name: Coarse facial features
description: Coarse/dysmorphic facies of the severe (type II) form.
phenotype_term:
preferred_term: Coarse facial features
term:
id: HP:0000280
label: Coarse facial features
evidence:
- reference: PMID:29693572
reference_title: "Sialidosis: A Review of Morphology and Molecular Biology of a Rare Pediatric Disorder."
supports: SUPPORT
evidence_source: HUMAN_CLINICAL
snippet: "sialidosis type II (dysmorphic or severe form)"
explanation: "Type II sialidosis is the dysmorphic form with coarse facial features."
- name: Hepatosplenomegaly
description: Visceral organomegaly present from birth.
phenotype_term:
preferred_term: Hepatosplenomegaly
term:
id: HP:0001433
label: Hepatosplenomegaly
evidence:
- reference: PMID:26949572
reference_title: "Pathogenesis, Emerging therapeutic targets and Treatment in Sialidosis."
supports: SUPPORT
evidence_source: HUMAN_CLINICAL
snippet: "Their clinical presentation at birth includes facial edema, inguinal hernias and hepatosplenomegaly"
explanation: Hepatosplenomegaly is present at birth in congenital sialidosis type II.
biochemical:
- name: Urinary sialyloligosaccharides
presence: INCREASED
context: Increased urinary excretion of sialyloligosaccharides is a diagnostic biochemical marker.
evidence:
- reference: PMID:29693572
reference_title: "Sialidosis: A Review of Morphology and Molecular Biology of a Rare Pediatric Disorder."
supports: SUPPORT
evidence_source: HUMAN_CLINICAL
snippet: "This genetic alteration leads to abnormal intracellular accumulation as well as urinary excretion of"
explanation: "Urinary sialyloligosaccharide excretion is a biochemical hallmark."
inheritance:
- name: Autosomal recessive
inheritance_term:
preferred_term: Autosomal recessive inheritance
term:
id: HP:0000007
label: Autosomal recessive inheritance
evidence:
- reference: PMID:29693572
reference_title: "Sialidosis: A Review of Morphology and Molecular Biology of a Rare Pediatric Disorder."
supports: SUPPORT
evidence_source: HUMAN_CLINICAL
snippet: "Sialidosis (MIM 256550) is a rare, autosomal recessive inherited disorder"
explanation: "Sialidosis is autosomal recessive."
genetic:
- name: NEU1
association: Biallelic NEU1 variants abolishing lysosomal neuraminidase-1 (severe alleles)
relationship_type: CAUSATIVE
variant_origin: GERMLINE
gene_term:
preferred_term: NEU1
term:
id: hgnc:7758
label: NEU1
evidence:
- reference: PMID:29693572
reference_title: "Sialidosis: A Review of Morphology and Molecular Biology of a Rare Pediatric Disorder."
supports: SUPPORT
evidence_source: HUMAN_CLINICAL
snippet: "An association exists between the impact of the individual mutations and the\nseverity of clinical presentation of sialidosis."
explanation: "Severe NEU1 alleles produce the congenital form of sialidosis."
diagnosis:
- name: Urinary oligosaccharides and NEU1 sequencing
diagnosis_term:
preferred_term: clinical laboratory procedure
term:
id: MAXO:0000006
label: clinical laboratory procedure
description: >-
Increased urinary sialyloligosaccharides and deficient neuraminidase activity suggest the
diagnosis, confirmed by NEU1 sequencing; prenatal/neonatal hydrops with storage prompts testing.
markers: Elevated urinary sialyloligosaccharides; deficient neuraminidase activity.
evidence:
- reference: PMID:29693572
reference_title: "Sialidosis: A Review of Morphology and Molecular Biology of a Rare Pediatric Disorder."
supports: SUPPORT
evidence_source: HUMAN_CLINICAL
snippet: "A definitive diagnosis is made after the identification\nof a mutation in the NEU1 gene."
explanation: "Definitive diagnosis requires NEU1 sequencing."
differential_diagnoses:
- name: Galactosialidosis
description: >-
Combined neuraminidase and beta-galactosidase deficiency from cathepsin A (CTSA) deficiency,
which can also present with hydrops, but reflects secondary NEU1 loss.
disease_term:
preferred_term: galactosialidosis
term:
id: MONDO:0009737
label: galactosialidosis
distinguishing_features:
- Combined NEU1 and beta-galactosidase deficiency due to CTSA defect, versus primary NEU1 deficiency in sialidosis.
evidence:
- reference: PMID:26949572
reference_title: "Pathogenesis, Emerging therapeutic targets and Treatment in Sialidosis."
supports: SUPPORT
evidence_source: HUMAN_CLINICAL
snippet: "NEU1 requirement to complex with the\nprotective protein/cathepsin A for stability and activation"
explanation: "NEU1 depends on cathepsin A; CTSA deficiency causes galactosialidosis with secondary NEU1 loss."
treatments:
- name: Supportive Care
description: >-
No curative therapy exists; the congenital form is often fatal perinatally and management is
supportive and palliative.
treatment_term:
preferred_term: Supportive Care
term:
id: NCIT:C15747
label: Supportive Care
definitions:
- name: Clinical case definition of congenital sialidosis type 2
definition_type: CASE_DEFINITION
description: >-
Congenital sialidosis type 2 is the most severe, congenital-onset form of NEU1-related
sialidosis, defined by biallelic severe NEU1 variants with profound neuraminidase deficiency,
marked sialyloligosaccharide accumulation, and nonimmune hydrops fetalis.
scope: Disease-level case definition for the congenital severe form of sialidosis type 2.
evidence:
- reference: PMID:29693572
reference_title: "Sialidosis: A Review of Morphology and Molecular Biology of a Rare Pediatric Disorder."
supports: SUPPORT
evidence_source: HUMAN_CLINICAL
snippet: "sialidosis type II (dysmorphic or severe form)"
explanation: "Anchors the case definition in the severe (type II) form of sialidosis."
Congenital sialidosis type II is the most severe prenatal-onset end of the NEU1-related lysosomal storage disorder spectrum (“sialidosis”), typically presenting in utero or at birth with nonimmune hydrops fetalis, ascites, and generalized edema and often resulting in stillbirth or death shortly after birth. It is caused by biallelic loss-of-function variants in NEU1 (autosomal recessive inheritance) leading to near-complete deficiency of lysosomal neuraminidase-1 (sialidase) activity and subsequent lysosomal accumulation and urinary excretion of sialylated oligosaccharides and glycopeptides (“sialyl-oligosacchariduria”). Recent 2023–2024 studies emphasize additional downstream mechanisms beyond “storage,” including dysregulated lysosomal exocytosis (via LAMP1 hypersialylation) and organ-specific consequences such as kidney disease (“nephrosialidosis”) linked to hypersialylation-dependent megalin trafficking defects. (khan2018sialidosisareview pages 3-5, vlekkert2024aavmediatedgenetherapy pages 1-5, kho2023severekidneydysfunction pages 1-2)
Sialidosis (mucolipidosis I) is an ultra-rare, autosomal recessive lysosomal storage disease caused by deficiency of lysosomal neuraminidase-1 (NEU1), leading to accumulation and excretion of sialylated metabolites. Clinical severity ranges from type I (attenuated) to type II (severe neuropathic). Type II is further subdivided into congenital/hydropic, infantile, and juvenile forms based on age at onset. (khan2018sialidosisareview pages 3-5, vlekkert2024aavmediatedgenetherapy pages 1-5, khan2018sialidosisareview pages 1-3)
The congenital/hydropic subtype is described as the severe prenatal form: “It manifests itself prenatally and is characterized by ascites and hydrops fetalis, hepatomegaly and stillbirths or death at a very early age.” (khan2018sialidosisareview pages 3-5)
| Identifier system | ID | Preferred name | Synonyms / notes | Source URL | Publication date |
|---|---|---|---|---|---|
| MONDO | MONDO_0009738 | sialidosis type 2 | Disease entity for severe early-onset NEU1-related sialidosis; congenital/hydropic, infantile, and juvenile forms are subtypes/clinical subdivisions of type II (OpenTargets Search: Sialidosis, khan2018sialidosisareview pages 3-5, vlekkert2024aavmediatedgenetherapy pages 1-5) | https://platform.opentargets.org/disease/MONDO_0009738 | — |
| Orphanet | Orphanet_87876 | sialidosis type II | Orphanet disease entry corresponding to type II sialidosis; congenital (hydropic) form is the prenatal/neonatal severe subtype (OpenTargets Search: Sialidosis, khan2018sialidosisareview pages 3-5) | https://www.orpha.net/consor/cgi-bin/OC_Exp.php?Lng=EN&Expert=87876 | — |
| OMIM / MIM | 256550 | Sialidosis | Core inherited disorder caused by NEU1 deficiency; type II includes congenital/hydropic subtype; review explicitly cites “Sialidosis (MIM #256550)” (khan2018sialidosisareview pages 3-5, khan2018sialidosisareview pages 1-3) | https://omim.org/entry/256550 | 2018 (review citing MIM) |
| MeSH | Not clearly established for congenital type II as a distinct MeSH term | Sialidosis / Mucolipidosis I (broader indexing may vary) | Literature commonly indexes the broader disorder rather than a separate congenital type II term; use disease-level MeSH with subtype noted in free text (khan2018sialidosisareview pages 1-3, peng2025geneticinsightsand pages 1-2) | https://meshb.nlm.nih.gov/ | — |
| ICD-10 | No specific code identified for congenital type II | Sialidosis type II, congenital (hydropic) subtype | Usually classified under broader lysosomal storage/metabolic disorder categories rather than a unique congenital-type-specific ICD-10 code; verify locally in coding system implementation (khan2018sialidosisareview pages 3-5) | https://icd.who.int/browse10/2019/en | — |
| ICD-11 | No specific code confirmed from retrieved evidence | Sialidosis type II, congenital (hydropic) subtype | Retrieved evidence supports nomenclature but not a distinct ICD-11 identifier for the congenital subtype; map to broader sialidosis entry if needed after terminology validation (khan2018sialidosisareview pages 3-5, vlekkert2024aavmediatedgenetherapy pages 1-5) | https://icd.who.int/ | — |
| Clinical subtype designation | — | congenital sialidosis type II | Also called congenital or hydropic subtype; manifests prenatally and is characterized by ascites, hydrops fetalis, hepatomegaly, and stillbirth or very early death (khan2018sialidosisareview pages 3-5) | https://doi.org/10.3390/diagnostics8020029 | 2018 |
| Clinical subtype designation | — | sialidosis type II, congenital/hydropic form | Severe neuropathic NEU1-deficiency phenotype within type II; recent preclinical gene-therapy paper uses the same classification framework (vlekkert2024aavmediatedgenetherapy pages 1-5) | https://doi.org/10.1101/2023.11.10.566667 | 2024 |
Table: This table summarizes the main identifiers and naming conventions for congenital sialidosis type II, linking the congenital/hydropic form to the broader type II disease entity. It is useful for harmonizing OMIM, MONDO, Orphanet, and coding terminology in a disease knowledge base.
Notes: In the retrieved evidence, identifiers are most consistently available at the disease-entity level (sialidosis; sialidosis type II) rather than as a separate MONDO/Orphanet entity specifically for the “congenital/hydropic” subtype. (OpenTargets Search: Sialidosis, khan2018sialidosisareview pages 3-5)
Commonly used: - Sialidosis type II, congenital/hydropic subtype (or “congenital sialidosis”) (khan2018sialidosisareview pages 3-5, vlekkert2024aavmediatedgenetherapy pages 1-5) - Mucolipidosis I / sialidosis (vlekkert2024aavmediatedgenetherapy pages 1-5)
The congenital/hydropic phenotype is primarily derived from aggregated disease-level resources (reviews) that compile individual case reports and fetal pathology series (e.g., tabulated congenital cases). (khan2018sialidosisareview pages 3-5, khan2018sialidosisareview media 784849f6, khan2018sialidosisareview media 429fda1b, khan2018sialidosisareview media 29bee092)
Genetic cause: biallelic pathogenic variants in NEU1 encoding lysosomal neuraminidase-1 (sialidase). (khan2018sialidosisareview pages 1-3, peng2025geneticinsightsand pages 1-2)
Primary mechanistic defect: deficient NEU1 activity prevents normal lysosomal catabolism of sialylated glycoconjugates, leading to lysosomal accumulation and abnormal excretion of sialylated oligosaccharides/glycopeptides. (vlekkert2024aavmediatedgenetherapy pages 1-5, mosca2020conventionalandunconventional pages 1-3, kho2023severekidneydysfunction pages 1-2)
No validated genetic or environmental protective factors specific to congenital sialidosis type II were identified in retrieved sources.
No established gene–environment interactions specific to congenital sialidosis type II were found in the retrieved evidence.
The congenital/hydropic subtype is characterized by prenatal fluid overload and early lethality; additional findings vary across cases. In a comprehensive review, the distinguishing congenital group features were “hydrops, ascites, and edema … followed by coarse features, dysostosis multiplex, and hepatosplenomegaly.” (khan2018sialidosisareview pages 3-5)
| Clinical feature | Suggested HPO term(s) | Typical onset | Notes / frequency info if available | Key supporting citations |
|---|---|---|---|---|
| Hydrops fetalis | Hydrops fetalis HP:0001789 | Prenatal | Hallmark of the congenital/hydropic subtype; described as a distinguishing feature of the severe congenital group and associated with stillbirth or death shortly after birth | (khan2018sialidosisareview pages 3-5, vlekkert2024aavmediatedgenetherapy pages 1-5, mosca2020conventionalandunconventional pages 1-3, khan2018sialidosisareview media 784849f6, khan2018sialidosisareview media 429fda1b, khan2018sialidosisareview media 29bee092) |
| Ascites / neonatal ascites | Ascites HP:0001541; Fetal ascites HP:0001791 | Prenatal / neonatal | Prominent in congenital type II; often reported together with hydrops fetalis; may be isolated or refractory congenital ascites in case literature summarized in the review | (khan2018sialidosisareview pages 3-5, vlekkert2024aavmediatedgenetherapy pages 1-5, mosca2020conventionalandunconventional pages 1-3, khan2018sialidosisareview media 784849f6, khan2018sialidosisareview media 429fda1b, khan2018sialidosisareview media 29bee092) |
| Generalized edema / facial edema | Edema HP:0000969; Generalized edema HP:0007430; Facial edema HP:0010669 | Prenatal / neonatal | Review states hydrops, ascites, and edema are distinguishing congenital features; gene-therapy review specifically notes facial edema in acute congenital cases | (khan2018sialidosisareview pages 3-5, vlekkert2024aavmediatedgenetherapy pages 1-5, khan2018sialidosisareview pages 11-13) |
| Hepatomegaly | Hepatomegaly HP:0002240 | Prenatal / neonatal / infantile | Included in congenital presentation and severe infantile type II; may be part of broader visceromegaly | (khan2018sialidosisareview pages 3-5, vlekkert2024aavmediatedgenetherapy pages 1-5, mosca2020conventionalandunconventional pages 1-3) |
| Hepatosplenomegaly | Hepatosplenomegaly HP:0001433; Splenomegaly HP:0001744 | Neonatal / infantile | Common severe type II somatic feature; congenital review notes hepatosplenomegaly among frequent findings after hydrops/ascites/edema | (khan2018sialidosisareview pages 3-5, vlekkert2024aavmediatedgenetherapy pages 1-5, mosca2020conventionalandunconventional pages 1-3, peng2025geneticinsightsand pages 1-2) |
| Coarse facial features | Coarse facial features HP:0000280 | Neonatal / infantile | Frequent in infantile/juvenile type II; also noted among congenital cases | (khan2018sialidosisareview pages 3-5, vlekkert2024aavmediatedgenetherapy pages 1-5, mosca2020conventionalandunconventional pages 1-3, peng2025geneticinsightsand pages 1-2) |
| Dysostosis multiplex / skeletal dysplasia | Dysostosis multiplex HP:0000943; Skeletal dysplasia HP:0002652; Abnormal vertebral morphology HP:0000925 | Prenatal / infantile | Congenital review highlights dysostosis multiplex; severe type II also described with skeletal dysplasia and vertebral deformities | (khan2018sialidosisareview pages 3-5, vlekkert2024aavmediatedgenetherapy pages 1-5, mosca2020conventionalandunconventional pages 1-3) |
| Inguinal hernia | Inguinal hernia HP:0000023 | Neonatal | Specifically mentioned in acute congenital form; review notes it as an infrequent congenital manifestation | (khan2018sialidosisareview pages 3-5, vlekkert2024aavmediatedgenetherapy pages 1-5) |
| Cherry-red macula / cherry-red spot | Cherry red spot of the macula HP:0010729 | Infantile | More typical of infantile/juvenile severe type II than hydropic congenital cases; part of the classic ophthalmic phenotype | (vlekkert2024aavmediatedgenetherapy pages 1-5, peng2025geneticinsightsand pages 1-2, khan2018sialidosisareview pages 11-13) |
| Myoclonus | Myoclonus HP:0001336 | Infantile / juvenile | Common neurologic sign in severe type II beyond the congenital lethal presentation; used clinically with seizures for symptomatic management | (vlekkert2024aavmediatedgenetherapy pages 1-5, peng2025geneticinsightsand pages 1-2, khan2018sialidosisareview pages 11-13) |
| Seizures | Seizure HP:0001250 | Infantile / juvenile | Mentioned in severe type II spectrum and in supportive-care discussions; often grouped with myoclonus | (vlekkert2024aavmediatedgenetherapy pages 1-5) |
| Hearing loss | Hearing impairment HP:0000365 | Infantile / juvenile | Included in severe type II phenotype in the 2024 preclinical gene-therapy introduction; less emphasized for hydropic congenital cases | (vlekkert2024aavmediatedgenetherapy pages 1-5, khan2018sialidosisareview pages 5-7) |
| Cardiomyopathy | Cardiomyopathy HP:0001638 | Infantile | Listed among severe type II manifestations in recent review/preclinical summary; uncommon but clinically important | (vlekkert2024aavmediatedgenetherapy pages 1-5) |
| Nephrotic syndrome / nephrosialidosis | Nephrotic syndrome HP:0000100; Proteinuria HP:0000093 | Infantile / childhood | Subset of type II patients develop nephrosialidosis with abrupt fulminant glomerular nephropathy; renal involvement is infrequent in congenital review but important in severe type II | (kho2023severekidneydysfunction pages 1-2) |
| Developmental delay / severe intellectual disability | Global developmental delay HP:0001263; Intellectual disability, severe HP:0010864 | Infantile | Severe type II is associated with marked neurodevelopmental impairment/“mental retardation”; often not assessable in lethal prenatal congenital cases | (mosca2020conventionalandunconventional pages 1-3, peng2025geneticinsightsand pages 1-2, khan2018sialidosisareview pages 11-13) |
| Stillbirth / very early death | Stillbirth HP:0003826; Neonatal death HP:0003811 | Prenatal / neonatal | Congenital hydropic form is often lethal during fetal development or shortly after birth | (khan2018sialidosisareview pages 3-5, vlekkert2024aavmediatedgenetherapy pages 1-5, mosca2020conventionalandunconventional pages 1-3) |
Table: This table maps the major prenatal, neonatal, and infantile manifestations of congenital/severe sialidosis type II to suggested Human Phenotype Ontology terms. It is designed for knowledge-base curation and highlights which findings are characteristic of the hydropic congenital form versus the broader severe type II spectrum.
Formal phenotype frequencies specifically for congenital/hydropic type II were not quantified in the retrieved evidence set. The congenital-case table compiled in the 2018 review provides case-by-case features rather than aggregate percentages. (khan2018sialidosisareview media 784849f6, khan2018sialidosisareview media 429fda1b, khan2018sialidosisareview media 29bee092)
For congenital/hydropic cases, quality-of-life measures are generally not applicable due to fetal/neonatal lethality. For infantile/juvenile type II survivors, major impacts include severe neurologic disability and multisystem complications; standardized HRQoL instruments (e.g., EQ-5D/SF-36) were not identified in retrieved sources.
NEU1 catalyzes lysosomal removal of terminal sialic acids; a recent genetics review states NEU1 “catalyzes the breakdown of sialic acid-containing substances within lysosomes by hydrolyzing terminal sialic acid residues.” (peng2025geneticinsightsand pages 1-2)
Example genotype–phenotype detail (recent review): A reported patient with compound heterozygosity (exon3:c.544A>G and exon5:c.1021+1G>A) had neuraminidase activity “reduced to 6.4% of normal,” illustrating residual activity as a severity correlate. (peng2025geneticinsightsand pages 4-6)
NEU1 depends on a lysosomal multienzyme complex including PPCA/CTSA (protective protein/cathepsin A) and β-galactosidase (GLB1). In a 2024 preclinical gene-therapy study: “In mammalian tissues NEU1 is found in a high molecular weight complex with … PPCA … and … β-galactosidase” and “Interaction with PPCA is a prerequisite for the proper localization, stability and activation of NEU1. In absence of a functional PPCA, NEU1 is enzymatically silent.” (vlekkert2024aavmediatedgenetherapy pages 1-5)
This is central to the differential diagnosis with galactosialidosis (CTSA/PPCA deficiency) causing secondary NEU1 deficiency. (khan2018sialidosisareview pages 1-3, mosca2020conventionalandunconventional pages 1-3)
No disease-specific epigenetic alterations or recurrent chromosomal abnormalities were identified in the retrieved evidence.
Congenital sialidosis type II is a monogenic lysosomal disorder; no consistent environmental/lifestyle/infectious contributors were identified in retrieved sources.
NEU1 loss-of-function → lysosomal failure to desialylate glycoconjugates → storage of sialylated glycoproteins/oligosaccharides and systemic dysfunction. (vlekkert2024aavmediatedgenetherapy pages 1-5, mosca2020conventionalandunconventional pages 1-3)
A 2024 preprint abstract describes the foundational mechanism: “Sialidosis is a glycoprotein storage disease caused by deficiency of the lysosomal sialidase NEU1, which leads to pathogenic accumulation of sialylated glycoproteins and oligosaccharides in tissues and body fluids.” (vlekkert2024aavmediatedgenetherapy pages 1-5)
Beyond storage, NEU1 has been characterized as a negative regulator of lysosomal exocytosis. In Neu1−/− mice, NEU1 deficiency increases LAMP1+ lysosomes docked at the plasma membrane, promoting extracellular release of lysosomal contents, with downstream tissue remodeling and fibrosis. (vlekkert2024aavmediatedgenetherapy pages 1-5, khan2018sialidosisareview pages 1-3)
A 2023 JCI Insight study focused on the severe renal presentation in a subset of type II patients (“nephrosialidosis”) and modeled it in Neu1-deficient mice. Its abstract states that mice exhibited “elevated urinary albumin levels, loss of nephrons, renal fibrosis, presence of storage vacuoles,” and that glycoprotein sialylation was increased, including megalin; “Megalin levels were severely reduced, and the protein was directed to lysosomes instead of the apical membrane,” supporting impaired proximal tubular protein reabsorption as a mechanism for proteinuria. (kho2023severekidneydysfunction pages 1-2)
GO Biological Process (suggested): - Lysosomal catabolic process; glycoprotein catabolic process; lysosomal exocytosis; protein glycosylation/desialylation; endocytosis and receptor-mediated endocytosis; extracellular matrix organization/fibrosis; autophagy (renal findings include autophagy markers in mechanistic work). (vlekkert2024aavmediatedgenetherapy pages 1-5, kho2023severekidneydysfunction pages 9-11, kho2023severekidneydysfunction pages 1-2)
GO Cellular Component (suggested): - Lysosome; plasma membrane; endosome; extracellular space (lysosomal content release); glomerulus-related compartments (renal). (vlekkert2024aavmediatedgenetherapy pages 1-5, kho2023severekidneydysfunction pages 1-2)
Cell Ontology terms (suggested key cell types): - Kidney proximal tubule epithelial cell; podocyte; glomerular endothelial cell; macrophage/microglia (neuroinflammation/microgliosis in models); connective tissue fibroblast/myocyte (fibrosis/atrophy models). (khan2018sialidosisareview pages 5-7, kho2023severekidneydysfunction pages 9-11, vlekkert2024aavmediatedgenetherapy pages 1-5)
Organ-level involvement (severe type II spectrum): - Fetal/placental and systemic prenatal involvement with multiorgan vacuolation in congenital cases (liver, bone marrow, kidney, brain) and placental vacuolation indicating early fetal storage. (khan2018sialidosisareview pages 3-5, khan2018sialidosisareview pages 5-7) - Liver/spleen: hepatomegaly/hepatosplenomegaly. (khan2018sialidosisareview pages 3-5, vlekkert2024aavmediatedgenetherapy pages 1-5) - Skeletal system: dysostosis multiplex/skeletal dysplasia and vertebral deformities. (vlekkert2024aavmediatedgenetherapy pages 1-5, mosca2020conventionalandunconventional pages 1-3) - Central nervous system: severe neuropathology in type II; neurodegeneration mechanisms described in mouse models. (kho2023severekidneydysfunction pages 1-2, vlekkert2024aavmediatedgenetherapy pages 1-5) - Kidney: nephrosialidosis with glomerular nephropathy/nephrotic syndrome subset; megalin-mediated reabsorption defects in models. (kho2023severekidneydysfunction pages 1-2)
Subcellular localization: Lysosome (primary); plasma membrane docking/fusion events are emphasized in lysosomal exocytosis model; cell-surface hypersialylation affects trafficking receptors such as megalin. (vlekkert2024aavmediatedgenetherapy pages 1-5, kho2023severekidneydysfunction pages 1-2)
UBERON suggestions (high-level): fetal placenta, liver, spleen, kidney glomerulus, bone, brain.
These values are for sialidosis overall; congenital/hydropic type II is expected to be rarer, but subtype-specific rates were not found in retrieved sources.
A 2025 genetics review summarized population differences across sialidosis cohorts (not limited to congenital type II): - “Asian patients exhibit a lower incidence of impaired cognition (21.7%) … [vs] Caucasian patients (50.0%)” and “the occurrence of cherry-red patches is also lower in Asians (40.7% compared to 61.1% in Caucasians, P = 0.02).” (peng2025geneticinsightsand pages 2-4, peng2025geneticinsightsand pages 4-6)
A Taiwan-associated variant (c.544A>G; p.Ser182Gly) was highlighted as common in Asians and absent in Caucasians in the same review. (peng2025geneticinsightsand pages 4-6)
Congenital type II is associated with profound loss of enzyme function and high severity; explicit penetrance estimates were not identified.
| Diagnostic modality | Sample type | Expected finding in sialidosis type II | Distinguishes from | Notes / pitfalls | Key citations | URL / publication date |
|---|---|---|---|---|---|---|
| Urine oligosaccharide screening by thin-layer chromatography (TLC) | Urine | Abnormal urinary oligosaccharide pattern; increased urinary excretion of sialylated oligosaccharides / glycopeptides is a diagnostic hallmark of NEU1 deficiency | Supports separation from non-oligosaccharidosis causes of hydrops/ascites; helps prioritize sialidosis or galactosialidosis among lysosomal storage diseases | Screening test rather than standalone confirmation; congenital cases may also show oligosaccharides in ascitic fluid in historical reports summarized by review literature | (khan2018sialidosisareview pages 3-5, khan2018sialidosisareview pages 1-3, khan2018sialidosisareview pages 13-14, kho2023severekidneydysfunction pages 1-2) | https://doi.org/10.3390/diagnostics8020029 (2018-04-20); https://doi.org/10.1172/jci.insight.166470 (2023-10-23) |
| Neuraminidase (alpha-N-acetyl neuraminidase / NEU1) enzyme assay | Cultured skin fibroblasts from biopsy (gold standard), also leukocytes in some reports | Deficient lysosomal sialidase activity / neuraminidase deficiency | Confirms primary neuraminidase deficiency and narrows differential within lysosomal storage diseases | Fibroblasts are emphasized as the preferred material for sialidosis/galactosialidosis enzymology; specialized metabolic laboratories are often required | (khan2018sialidosisareview pages 3-5, serrano2024hepatomegalyandsplenomegaly pages 7-8, khan2018sialidosisareview pages 1-3, khan2018sialidosisareview pages 11-13) | https://doi.org/10.3390/diagnostics8020029 (2018-04-20); https://doi.org/10.3390/jcm13051465 (2024-03-01) |
| Paired beta-galactosidase assay with neuraminidase testing | Cultured fibroblasts or other enzymology sample used for lysosomal enzyme workup | Beta-galactosidase activity should be normal in primary sialidosis type II | Galactosialidosis (secondary combined NEU1 and beta-galactosidase deficiency due to CTSA/PPCA defects) | Essential differential step because galactosialidosis can phenocopy sialidosis; PPCA deficiency causes secondary NEU1 deficiency | (khan2018sialidosisareview pages 3-5, khan2018sialidosisareview pages 1-3, mosca2020conventionalandunconventional pages 1-3) | https://doi.org/10.3390/diagnostics8020029 (2018-04-20); https://doi.org/10.3390/jcm9030695 (2020-03-04) |
| Molecular genetic confirmation: targeted NEU1 sequencing | Blood, saliva, buccal swab, or DNA extracted from clinical specimen | Biallelic pathogenic/likely pathogenic NEU1 variants confirming autosomal recessive sialidosis | Distinguishes primary NEU1-related sialidosis from CTSA-related galactosialidosis and from other lysosomal storage disorders with overlapping hydrops/hepatosplenomegaly phenotypes | Definitive diagnosis requires variant interpretation in clinical context; useful for prenatal testing, carrier testing, and family counseling | (khan2018sialidosisareview pages 3-5, khan2018sialidosisareview pages 1-3, khan2018sialidosisareview pages 11-13, peng2025geneticinsightsand pages 1-2) | https://doi.org/10.3390/diagnostics8020029 (2018-04-20); https://doi.org/10.3390/genes16020151 (2025-01) |
| Exome / genome sequencing (WES/WGS) | Blood-derived DNA or family trio DNA | Identification of biallelic NEU1 variants, including novel missense, splice-site, frameshift, or compound-heterozygous variants | Useful when biochemical phenotype overlaps with other lysosomal disorders or when prenatal/neonatal presentations are nonspecific | Particularly valuable in atypical presentations or when single-gene testing is unrevealing; sequencing results may still require biochemical validation | (khan2018sialidosisareview pages 3-5, serrano2024hepatomegalyandsplenomegaly pages 7-8, peng2025geneticinsightsand pages 6-8) | https://doi.org/10.3390/diagnostics8020029 (2018-04-20); https://doi.org/10.3390/jcm13051465 (2024-03-01); https://doi.org/10.3390/genes16020151 (2025-01) |
| Prenatal / family-based molecular diagnosis | Fetal DNA, parental DNA, or prenatal specimen in at-risk pregnancies | Detection of familial NEU1 pathogenic variants before birth | Helps distinguish congenital hydropic sialidosis from other genetic causes of nonimmune hydrops fetalis | Particularly relevant because congenital type II may be lethal in utero or shortly after birth; enables recurrence-risk counseling | (khan2018sialidosisareview pages 11-13, khan2018sialidosisareview pages 13-14) | https://doi.org/10.3390/diagnostics8020029 (2018-04-20) |
| Peripheral blood smear / bone marrow smear | Peripheral blood or bone marrow | Storage granules in lymphocytes may be present | Supports lysosomal storage disease rather than isolated renal/hepatic disease | Ancillary, not disease-specific; should not replace enzyme or molecular confirmation | (khan2018sialidosisareview pages 3-5) | https://doi.org/10.3390/diagnostics8020029 (2018-04-20) |
| Integrated LSD second-line workup | Plasma, leukocytes, fibroblasts, urine, DNA | Combination of low neuraminidase activity, abnormal urine oligosaccharides, and biallelic NEU1 variants | Helps distinguish from mucolipidoses, multiple sulfatase deficiency, and other hepatosplenomegaly-associated LSDs | Serrano 2024 recommends molecular testing accompanied by enzymatic testing when feasible; biopsy should generally be last resort | (serrano2024hepatomegalyandsplenomegaly pages 7-8, serrano2024hepatomegalyandsplenomegaly pages 2-3) | https://doi.org/10.3390/jcm13051465 (2024-03-01) |
| Interpretation safeguard for VUS / pseudodeficiency | DNA plus matched biochemical testing | Variants of uncertain significance should be corroborated by enzymology and/or biomarkers; pseudodeficiency may show low in vitro activity without true disease | Prevents overcalling sialidosis when lab abnormalities are non-pathogenic or inconclusive | Important pitfall from LSD diagnostics: VUS often need targeted biochemical confirmation; specialized labs improve interpretation | (lange2024systematicdiagnosisof pages 4-6, serrano2024hepatomegalyandsplenomegaly pages 7-8) | https://doi.org/10.51847/isa3beaurx (2024-01); https://doi.org/10.3390/jcm13051465 (2024-03-01) |
Table: This table summarizes the core diagnostic workflow and major differential-diagnostic issues for congenital sialidosis type II. It highlights the complementary roles of urine oligosaccharide screening, fibroblast neuraminidase assays, beta-galactosidase testing, and molecular confirmation, including key pitfalls such as VUS interpretation and pseudodeficiency.
Robust survival curves, median survival, or subtype-stratified mortality statistics were not identified in the retrieved evidence.
No approved disease-modifying therapy is established; current care is primarily supportive. In the 2024 gene-therapy preprint: “Currently, there is no target treatment or cure available for type I or II sialidosis. Patients receive supportive care and symptomatic relief, primarily for the management of myoclonus and seizures.” (vlekkert2024aavmediatedgenetherapy pages 1-5)
| Intervention type | Specific intervention | Mechanism / rationale | Evidence type | Key findings / outcomes | Limitations / notes | Key citations | URL and publication date |
|---|---|---|---|---|---|---|---|
| Supportive | Symptomatic management of myoclonus and seizures | No disease-modifying therapy is established; care focuses on controlling neurologic symptoms in surviving type II patients | Human clinical practice / review | Recent preclinical review states patients with sialidosis currently receive “supportive care and symptomatic relief, primarily for the management of myoclonus and seizures” | Evidence is descriptive rather than protocolized; especially relevant to infantile/juvenile type II rather than lethal hydropic congenital presentations | (vlekkert2024aavmediatedgenetherapy pages 1-5) | https://doi.org/10.1101/2023.11.10.566667 ; posted 2023-11-13 / cited as 2024 preprint |
| Supportive | Multidisciplinary monitoring in natural history protocols | Longitudinal neurologic, ophthalmologic, imaging, electrophysiologic, biochemical, and functional assessments help define progression and future trial endpoints | Observational trial / real-world implementation | NIH natural history protocol enrolls enzyme- or DNA-confirmed sialidosis/galactosialidosis patients and uses MRI/MRS, hearing testing, EEG, EMG/NCV, echocardiogram, abdominal ultrasound, ophthalmology, rehabilitation, speech, neurology, psychology, and biomarker sampling | Observational only; not a treatment; includes all sialidosis forms rather than congenital type II specifically | (NCT00029965 chunk 1) | https://clinicaltrials.gov/study/NCT00029965 ; first posted 2002-01-28, recruiting update 2026-05-29 |
| Experimental | Recombinant NEU1 enzyme replacement therapy (ERT) | Replaces deficient lysosomal neuraminidase-1 to reduce storage of sialylated glycoproteins / oligosaccharides | Mouse preclinical | Review summarizes “short-term ERT” in Neu1−/− mice using recombinant Neu1 from insect cells; corrected systemic pathology in mice | Strong immunogenicity limited durability/translation; no approved human ERT for sialidosis | (mosca2020conventionalandunconventional pages 1-3, khan2018sialidosisareview pages 11-13, khan2018sialidosisareview pages 14-16, peng2025geneticinsightsand pages 1-2) | https://doi.org/10.3390/jcm9030695 ; 2020-03-04 |
| Experimental | PPCA-based pharmacologic chaperone approach | NEU1 requires protective protein/cathepsin A (PPCA) for folding, lysosomal localization, stability, and activation; augmenting PPCA can rescue residual mutant NEU1 | In vitro and mouse preclinical | Recombinant PPCA and related chaperone strategies produced small but consistent increases in residual NEU1 activity in patient fibroblasts; prior AAV-PPCA work improved residual activity and prevented kidney pathology / oligosacchariduria in a type I model | Likely most applicable where residual NEU1 is present; evidence strongest for type I or attenuated variants, not fully null congenital cases | (mosca2020conventionalandunconventional pages 1-3, vlekkert2024aavmediatedgenetherapy pages 1-5, khan2022neu1—auniquetherapeutic pages 2-3) | https://doi.org/10.3390/jcm9030695 ; 2020-03-04 |
| Experimental | AAV-PPCA chaperone-mediated gene therapy | Liver-directed PPCA expression acts as a systemic chaperone to enhance residual NEU1 function | Mouse preclinical | Prior work cited in the 2024 preprint showed a single liver-specific AAV-PPCA dose “enhanced residual Neu1 activity and prevented kidney pathology and oligosacchariduria” | Mutation-dependent; mainly relevant to residual-activity alleles rather than severe congenital null alleles | (vlekkert2024aavmediatedgenetherapy pages 1-5, khan2018sialidosisareview pages 11-13) | https://doi.org/10.1101/2023.11.10.566667 ; posted 2023-11-13 / cited as 2024 preprint |
| Experimental | Dual AAV gene therapy (NEU1 + PPCA; scAAV2/8 co-injection) | Directly restores NEU1 plus its required chaperone PPCA, aiming to correct enzyme deficiency, storage, lysosomal exocytosis, fibrosis, and neurovisceral pathology | Mouse preclinical | In Neu1−/− mice, treated animals were “phenotypically indistinguishable from their WT controls,” with restored NEU1 activity in most tissues, reversal of sialyl-oligosacchariduria, diminished/absent vacuolization in visceral organs and brain, normalization of lysosomal exocytosis, and prevention of generalized fibrosis | Preclinical bioRxiv study; not yet a human trial; long-term durability, dosing, immunity, and CNS translation remain to be established | (vlekkert2024aavmediatedgenetherapy pages 1-5) | https://doi.org/10.1101/2023.11.10.566667 ; posted 2023-11-13 / cited as 2024 preprint |
| Experimental | Pharmacologic proteostasis / proteasome inhibition (e.g., MG132; celastrol discussed in review) | May improve folding, trafficking, and lysosomal localization of defective NEU1 proteins | In vitro / preclinical | Review notes MG132 “enhances enzyme activity and its localization in cells expressing defective sialidase”; celastrol and other compounds were explored as adjunctive approaches | Early-stage only; toxicity and translational feasibility uncertain; not specific to congenital type II | (khan2018sialidosisareview pages 11-13, khan2018sialidosisareview pages 14-16) | https://doi.org/10.3390/diagnostics8020029 ; 2018-04-20 |
| Experimental / adjunctive | Dietary betaine supplementation | Proposed to stabilize residual mutant NEU1 and improve oligosaccharide handling | Mouse preclinical and patient fibroblasts | In residual-activity mouse models, betaine increased mutant NEU1 levels and resolved oligosacchariduria; patient fibroblasts showed small activity gains with several compounds | Data are primarily for type I / residual-activity disease, not severe congenital type II | (mosca2020conventionalandunconventional pages 1-3) | https://doi.org/10.3390/jcm9030695 ; 2020-03-04 |
| Supportive / preventive | Carrier detection, prenatal molecular diagnosis, genetic counseling | Because congenital hydropic type II can be lethal prenatally or neonatally, family-based molecular diagnosis supports reproductive planning and early diagnosis | Human clinical genetics | Review recommends “carrier detection in affected families, prenatal molecular diagnosis, and improved genetic counseling”; congenital cases have been diagnosed prenatally in reported literature | Prevents recurrence risk rather than treating affected fetus/newborn; requires known familial variants or robust molecular testing | (khan2018sialidosisareview pages 11-13, khan2018sialidosisareview pages 13-14) | https://doi.org/10.3390/diagnostics8020029 ; 2018-04-20 |
| Real-world research infrastructure | Biomarker and cell-model development within natural history studies | Builds outcome measures and translational platforms for future therapy testing | Observational trial / translational implementation | NIH protocol collects CSF, blood, urine biomarkers; establishes fibroblast cultures for “testing potential therapeutic agents” and creates iPSC-derived neural tissues for mechanistic and preclinical work | Indirect therapeutic value; no interventional efficacy results yet | (NCT00029965 chunk 1) | https://clinicaltrials.gov/study/NCT00029965 ; first posted 2002-01-28, recruiting update 2026-05-29 |
Table: This table summarizes the current management landscape for sialidosis type II, from symptomatic care to preclinical gene therapy and enzyme/chaperone approaches. It also includes natural-history study infrastructure that is already being used in practice to support biomarker discovery and future interventional trials.
Key 2023–2024 development: dual AAV gene therapy (NEU1 + PPCA) in Neu1−/− mice. The abstract reports treated animals “phenotypically indistinguishable from their WT controls,” with “restoration of NEU1 activity in most tissues, reversal of sialyl-oligosacchariduria, and normalization of lysosomal exocytosis,” and prevention of generalized fibrosis. (vlekkert2024aavmediatedgenetherapy pages 1-5)
MAXO suggestions (high-level): antiseizure medication therapy; supportive care; genetic counseling; enzyme replacement therapy (experimental); gene therapy (AAV-based) (preclinical).
No interventional NEU1 gene therapy or ERT trials for sialidosis type II were identified in the retrieved trial list. However, natural history and biomarker studies relevant to future trials exist, including: - NCT00029965 (NIH): Natural History of Glycosphingolipid Storage Disorders and Glycoprotein Disorders (includes enzyme/DNA-confirmed sialidosis). (NCT00029965 chunk 1)
Because this is a Mendelian autosomal recessive disorder, prevention focuses on recurrence-risk management: - Carrier detection and prenatal molecular diagnosis with genetic counseling are explicitly recommended in the congenital/type II context. (khan2018sialidosisareview pages 11-13)
Primary prevention via lifestyle or vaccination is not applicable.
No naturally occurring (non-model) animal cases were identified in the retrieved evidence.
Neu1−/− mice are widely used and closely resemble severe type II disease. The 2024 preprint states: “Neu1 knockout mice (Neu1−/−) closely resemble type II sialidosis … [with] severe growth retardation … premature death (4–6 months).” (vlekkert2024aavmediatedgenetherapy pages 1-5)
Kidney-specific mechanistic modeling of nephrosialidosis: Neu1-deficient mice show albuminuria, nephron loss, and renal fibrosis, and hypersialylation-driven megalin mistrafficking to lysosomes rather than the apical membrane. (kho2023severekidneydysfunction pages 1-2)
The NIH natural history protocol notes: “Some fibroblast lines will be used to create induced pluripotent stem cells (iPSC) for differentiation into neural tissues,” enabling CNS-relevant modeling and biomarker studies. (NCT00029965 chunk 1)
References
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