Metastatic Pancreatic Adenocarcinoma

MONDO:0006047 pancreatic adenocarcinoma

Metastatic pancreatic adenocarcinoma is pancreatic ductal adenocarcinoma that has disseminated to distant sites, most often liver, peritoneum, and lung. The disease is characterized by near-universal KRAS pathway activation, early cellular plasticity, dense desmoplastic stroma, neural invasion, profound immune suppression, and rapid systemic progression.

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1
Mappings
5
Pathophys.
5
Phenotypes
4
Genes
1
Treatments
11
References
1
Deep Research
🔗

Mappings

MONDO
MONDO:0006047 pancreatic adenocarcinoma
skos:closeMatch MONDO
Closest MONDO parent term available for metastatic pancreatic adenocarcinoma.

Pathophysiology

5
KRAS-Centered Oncogenic Signaling
KRAS signaling is the dominant oncogenic engine in pancreatic adenocarcinoma and drives proliferation, stress adaptation, invasion, and metastatic competence. Even KRAS-wildtype tumors often remain dependent on parallel kinase and fusion pathways.
MAPK cascade link ↑ INCREASED cell population proliferation link ↑ INCREASED
Show evidence (1 reference)
PMID:35302596 SUPPORT Other
"KRAS mutation (MT) is a major oncogenic driver in pancreatic ductal adenocarcinoma (PDAC)."
This directly supports KRAS as the central driver pathway in PDAC.
Early Dissemination and EMT
Metastatic spread can begin early, before the primary tumor becomes clinically dominant. Cellular plasticity, EMT-like transitions, and squamous or mesenchymal programs enable escape from precursor and invasive lesions.
epithelial to mesenchymal transition link ↑ INCREASED cell migration link ↑ INCREASED
Show evidence (1 reference)
PMID:41814069 SUPPORT Other
"We explore the biological and spatial-temporal evolution of precancerous lesions, such as PanINs and IPMNs, and examine how phenotypic plasticity and overlapping cellular programs-including squamous transdifferentiation, epithelial-to-mesenchymal transition (EMT), and acquisition of mesenchymal..."
This directly supports EMT-linked early dissemination in pancreatic adenocarcinoma.
Perineural Invasion
Pancreatic adenocarcinoma has marked neurotropism. Tumor cells track along nerves, exploit neurotrophic cues, and use neural routes as low-resistance corridors for local spread and distant metastatic behavior.
positive regulation of cell migration link ↑ INCREASED
Show evidence (1 reference)
PMID:35449152 SUPPORT Human Clinical
"Perineural invasion (PNI) is a pathologic feature of pancreatic cancer and is associated with poor outcomes, metastasis, and recurrence in pancreatic cancer patients."
This supports perineural invasion as a metastasis-associated feature of pancreatic cancer.
Desmoplastic Stromal Remodeling
A fibrotic, CAF-rich, immune-excluding stroma compresses vessels, impairs drug delivery, and creates a mechanically and metabolically favorable niche for metastatic progression.
extracellular matrix organization link ↑ INCREASED angiogenesis link ⚠ ABNORMAL
Immune Evasion and Metastatic Selection
Pancreatic adenocarcinoma develops profound immune suppression with myeloid dominance, T-cell exclusion, and checkpoint-indifferent metastatic outgrowth. These programs help disseminated clones survive in liver and peritoneal sites.
negative regulation of immune response link ↑ INCREASED

Phenotypes

5
Digestive 1
Jaundice FREQUENT Jaundice (HP:0000952)
Show evidence (1 reference)
PMID:25726049 SUPPORT Human Clinical
"Common signs and symptoms of PDA include abdominal or back pain, jaundice, weight loss, pruritus, and nausea/vomiting."
Directly lists jaundice as a common presenting symptom of pancreatic ductal adenocarcinoma.
Constitutional 3
Abdominal pain VERY_FREQUENT Abdominal pain (HP:0002027)
Show evidence (1 reference)
PMID:25726049 SUPPORT Human Clinical
"Common signs and symptoms of PDA include abdominal or back pain, jaundice, weight loss, pruritus, and nausea/vomiting."
Directly lists abdominal pain as a common presenting symptom of pancreatic ductal adenocarcinoma.
Fatigue Fatigue (HP:0012378)
Back pain FREQUENT Back pain (HP:0003418)
Show evidence (1 reference)
PMID:25726049 SUPPORT Human Clinical
"Common signs and symptoms of PDA include abdominal or back pain, jaundice, weight loss, pruritus, and nausea/vomiting."
Directly lists back pain as a common presenting symptom of pancreatic ductal adenocarcinoma.
Growth 1
Weight loss VERY_FREQUENT Weight loss (HP:0001824)
Show evidence (1 reference)
PMID:25726049 SUPPORT Human Clinical
"Common signs and symptoms of PDA include abdominal or back pain, jaundice, weight loss, pruritus, and nausea/vomiting."
Directly lists weight loss as a common presenting symptom of pancreatic ductal adenocarcinoma.
🧬

Genetic Associations

4
KRAS (Somatic activating mutation)
Show evidence (1 reference)
PMID:33347393 SUPPORT Human Clinical
"This systematic review and meta-analysis supports the use of driver mutations in the P53, SMAD4, and KRAS genes as prognostic markers for pancreatic cancer."
Directly supports KRAS as an established driver mutation and prognostic marker in pancreatic cancer.
TP53 (Somatic loss of function)
Show evidence (1 reference)
PMID:33347393 SUPPORT Human Clinical
"This systematic review and meta-analysis supports the use of driver mutations in the P53, SMAD4, and KRAS genes as prognostic markers for pancreatic cancer."
Directly supports TP53 mutation as an established driver and poor prognostic marker in pancreatic cancer.
SMAD4 (Somatic loss of function)
Show evidence (1 reference)
PMID:33347393 SUPPORT Human Clinical
"This systematic review and meta-analysis supports the use of driver mutations in the P53, SMAD4, and KRAS genes as prognostic markers for pancreatic cancer."
Directly supports SMAD4 mutation as an established driver and poor prognostic marker in pancreatic cancer.
CDKN2A (Somatic loss of function)
Show evidence (1 reference)
PMID:18772397 SUPPORT Human Clinical
"This list includes the classic tumor suppressor genes CDKN2A (p16), SMAD4, and TP53, as well as genes that had not previously been implicated in pancreatic cancer development."
Directly identifies CDKN2A/p16 as a classic tumor suppressor gene affected by homozygous deletion in pancreatic cancers.
💊

Treatments

1
Maintenance Olaparib for Germline BRCA-Mutated Disease
Action: targeted therapy Ontology label: Targeted Therapy NCIT:C93352
Agent: olaparib
Maintenance olaparib is used after platinum-based chemotherapy for metastatic pancreatic adenocarcinoma with a germline BRCA mutation, targeting homologous recombination repair deficiency.
Show evidence (1 reference)
DOI:10.1200/jco.21.01604 SUPPORT Human Clinical
"The phase III POLO study demonstrated significant progression-free survival (PFS) benefit for active olaparib maintenance therapy versus placebo for patients with metastatic pancreatic adenocarcinoma and a germline BRCA mutation."
The phase III POLO trial supports maintenance olaparib in germline BRCA-mutated metastatic pancreatic adenocarcinoma.
🌍

Environmental Factors

3
Smoking
Smoking is a major modifiable pancreatic cancer risk factor and is linked to aggressive disease biology.
Show evidence (1 reference)
PMID:34002083 SUPPORT Human Clinical
"there are key modifiable risk factors for pancreatic cancer such as cigarette smoking, obesity, diabetes and alcohol intake."
Directly identifies cigarette smoking as a leading modifiable risk factor for pancreatic cancer.
Chronic pancreatitis
Chronic pancreatic inflammation promotes stromal remodeling and tumor evolution.
Obesity and diabetes
Metabolic dysfunction can reinforce inflammatory and growth-factor programs relevant to dissemination.
Show evidence (1 reference)
PMID:34002083 SUPPORT Human Clinical
"there are key modifiable risk factors for pancreatic cancer such as cigarette smoking, obesity, diabetes and alcohol intake."
Directly identifies obesity and diabetes as key modifiable risk factors for pancreatic cancer.
{ }

Source YAML

click to show 
name: Metastatic Pancreatic Adenocarcinoma
creation_date: '2026-03-28T21:15:00Z'
updated_date: '2026-05-10T09:08:36Z'
description: >-
  Metastatic pancreatic adenocarcinoma is pancreatic ductal adenocarcinoma that has
  disseminated to distant sites, most often liver, peritoneum, and lung. The disease
  is
  characterized by near-universal KRAS pathway activation, early cellular plasticity,
  dense desmoplastic stroma, neural invasion, profound immune suppression, and rapid
  systemic progression.
categories:
- Gastrointestinal Cancer
- Metastatic Cancer
- Solid Tumor
parents:
- pancreatic adenocarcinoma
disease_term:
  preferred_term: metastatic pancreatic adenocarcinoma
  term:
    id: MONDO:0006047
    label: pancreatic adenocarcinoma
mappings:
  mondo_mappings:
  - term:
      id: MONDO:0006047
      label: pancreatic adenocarcinoma
    mapping_predicate: skos:closeMatch
    mapping_source: MONDO
    mapping_justification: Closest MONDO parent term available for metastatic pancreatic adenocarcinoma.
prevalence:
- population: Metastatic pancreatic ductal adenocarcinoma
  notes: The 5-year survival rate remains persistently low in PDAC, especially once metastatic dissemination is established.
  evidence:
  - reference: PMID:41814069
    reference_title: Early cellular plasticity promotes progression and dissemination in pancreatic adenocarcinoma.
    supports: SUPPORT
    evidence_source: OTHER
    snippet: Pancreatic ductal adenocarcinoma (PDAC) remains one of the most lethal malignancies, with limited therapeutic success and a persistently low 5-year survival rate.
    explanation: This supports the extremely poor long-term prognosis of metastatic pancreatic adenocarcinoma.
pathophysiology:
- name: KRAS-Centered Oncogenic Signaling
  description: >-
    KRAS signaling is the dominant oncogenic engine in pancreatic adenocarcinoma and
    drives
    proliferation, stress adaptation, invasion, and metastatic competence. Even KRAS-wildtype
    tumors often remain dependent on parallel kinase and fusion pathways.
  evidence:
  - reference: PMID:35302596
    reference_title: Molecular Characterization of KRAS Wild-type Tumors in Patients with Pancreatic Adenocarcinoma.
    supports: SUPPORT
    evidence_source: OTHER
    snippet: KRAS mutation (MT) is a major oncogenic driver in pancreatic ductal adenocarcinoma (PDAC).
    explanation: This directly supports KRAS as the central driver pathway in PDAC.
  biological_processes:
  - preferred_term: MAPK cascade
    modifier: INCREASED
    term:
      id: GO:0000165
      label: MAPK cascade
  - preferred_term: cell population proliferation
    modifier: INCREASED
    term:
      id: GO:0008283
      label: cell population proliferation
- name: Early Dissemination and EMT
  description: >-
    Metastatic spread can begin early, before the primary tumor becomes clinically
    dominant.
    Cellular plasticity, EMT-like transitions, and squamous or mesenchymal programs
    enable
    escape from precursor and invasive lesions.
  evidence:
  - reference: PMID:41814069
    reference_title: Early cellular plasticity promotes progression and dissemination in pancreatic adenocarcinoma.
    supports: SUPPORT
    evidence_source: OTHER
    snippet: We explore the biological and spatial-temporal evolution of precancerous lesions, such as PanINs and IPMNs, and examine how phenotypic plasticity and overlapping cellular programs-including squamous transdifferentiation, epithelial-to-mesenchymal transition (EMT), and acquisition of mesenchymal features-contribute to early dissemination, treatment resistance, and surgical failure.
    explanation: This directly supports EMT-linked early dissemination in pancreatic adenocarcinoma.
  biological_processes:
  - preferred_term: epithelial to mesenchymal transition
    modifier: INCREASED
    term:
      id: GO:0001837
      label: epithelial to mesenchymal transition
  - preferred_term: cell migration
    modifier: INCREASED
    term:
      id: GO:0016477
      label: cell migration
- name: Perineural Invasion
  description: >-
    Pancreatic adenocarcinoma has marked neurotropism. Tumor cells track along nerves,
    exploit neurotrophic cues, and use neural routes as low-resistance corridors for
    local
    spread and distant metastatic behavior.
  evidence:
  - reference: PMID:35449152
    reference_title: HGF/c-Met pathway facilitates the perineural invasion of pancreatic cancer by activating the mTOR/NGF axis.
    supports: SUPPORT
    evidence_source: HUMAN_CLINICAL
    snippet: Perineural invasion (PNI) is a pathologic feature of pancreatic cancer and is associated with poor outcomes, metastasis, and recurrence in pancreatic cancer patients.
    explanation: This supports perineural invasion as a metastasis-associated feature of pancreatic cancer.
  biological_processes:
  - preferred_term: positive regulation of cell migration
    modifier: INCREASED
    term:
      id: GO:0030335
      label: positive regulation of cell migration
- name: Desmoplastic Stromal Remodeling
  description: >-
    A fibrotic, CAF-rich, immune-excluding stroma compresses vessels, impairs drug
    delivery,
    and creates a mechanically and metabolically favorable niche for metastatic progression.
  biological_processes:
  - preferred_term: extracellular matrix organization
    modifier: INCREASED
    term:
      id: GO:0030198
      label: extracellular matrix organization
  - preferred_term: angiogenesis
    modifier: ABNORMAL
    term:
      id: GO:0001525
      label: angiogenesis
- name: Immune Evasion and Metastatic Selection
  description: >-
    Pancreatic adenocarcinoma develops profound immune suppression with myeloid dominance,
    T-cell exclusion, and checkpoint-indifferent metastatic outgrowth. These programs
    help
    disseminated clones survive in liver and peritoneal sites.
  biological_processes:
  - preferred_term: negative regulation of immune response
    modifier: INCREASED
    term:
      id: GO:0050777
      label: negative regulation of immune response
phenotypes:
- category: Gastrointestinal
  name: Abdominal pain
  frequency: VERY_FREQUENT
  description: Abdominal pain reflects primary pancreatic invasion and metastatic extension.
  phenotype_term:
    preferred_term: Abdominal pain
    term:
      id: HP:0002027
      label: Abdominal pain
  evidence:
  - reference: PMID:25726049
    reference_title: Diagnostic evaluation and staging of pancreatic ductal adenocarcinoma.
    supports: SUPPORT
    evidence_source: HUMAN_CLINICAL
    snippet: >-
      Common signs and symptoms of PDA include abdominal or back pain,
      jaundice, weight loss, pruritus, and nausea/vomiting.
    explanation: >-
      Directly lists abdominal pain as a common presenting symptom of
      pancreatic ductal adenocarcinoma.
- category: Constitutional
  name: Weight loss
  frequency: VERY_FREQUENT
  description: Profound cancer cachexia is common in metastatic pancreatic adenocarcinoma.
  phenotype_term:
    preferred_term: Weight loss
    term:
      id: HP:0001824
      label: Weight loss
  evidence:
  - reference: PMID:25726049
    reference_title: Diagnostic evaluation and staging of pancreatic ductal adenocarcinoma.
    supports: SUPPORT
    evidence_source: HUMAN_CLINICAL
    snippet: >-
      Common signs and symptoms of PDA include abdominal or back pain,
      jaundice, weight loss, pruritus, and nausea/vomiting.
    explanation: >-
      Directly lists weight loss as a common presenting symptom of
      pancreatic ductal adenocarcinoma.
- category: Constitutional
  name: Fatigue
  description: Fatigue reflects systemic inflammation, malnutrition, and treatment intensity.
  phenotype_term:
    preferred_term: Fatigue
    term:
      id: HP:0012378
      label: Fatigue
- category: Hepatic
  name: Jaundice
  frequency: FREQUENT
  description: Jaundice may result from biliary obstruction or extensive liver involvement.
  phenotype_term:
    preferred_term: Jaundice
    term:
      id: HP:0000952
      label: Jaundice
  evidence:
  - reference: PMID:25726049
    reference_title: Diagnostic evaluation and staging of pancreatic ductal adenocarcinoma.
    supports: SUPPORT
    evidence_source: HUMAN_CLINICAL
    snippet: >-
      Common signs and symptoms of PDA include abdominal or back pain,
      jaundice, weight loss, pruritus, and nausea/vomiting.
    explanation: >-
      Directly lists jaundice as a common presenting symptom of pancreatic
      ductal adenocarcinoma.
- category: Musculoskeletal
  name: Back pain
  frequency: FREQUENT
  description: Back pain reflects retroperitoneal spread and neural invasion.
  phenotype_term:
    preferred_term: Back pain
    term:
      id: HP:0003418
      label: Back pain
  evidence:
  - reference: PMID:25726049
    reference_title: Diagnostic evaluation and staging of pancreatic ductal adenocarcinoma.
    supports: SUPPORT
    evidence_source: HUMAN_CLINICAL
    snippet: >-
      Common signs and symptoms of PDA include abdominal or back pain,
      jaundice, weight loss, pruritus, and nausea/vomiting.
    explanation: >-
      Directly lists back pain as a common presenting symptom of pancreatic
      ductal adenocarcinoma.
genetic:
- name: KRAS
  association: Somatic activating mutation
  notes: KRAS mutation is the canonical driver of PDAC and supports metastatic fitness.
  evidence:
  - reference: PMID:33347393
    reference_title: "Clinical Effect of Driver Mutations of KRAS, CDKN2A/P16, TP53, and SMAD4 in Pancreatic Cancer: A Meta-Analysis."
    supports: SUPPORT
    evidence_source: HUMAN_CLINICAL
    snippet: >-
      This systematic review and meta-analysis supports the use of driver
      mutations in the P53, SMAD4, and KRAS genes as prognostic markers for
      pancreatic cancer.
    explanation: >-
      Directly supports KRAS as an established driver mutation and
      prognostic marker in pancreatic cancer.
- name: TP53
  association: Somatic loss of function
  notes: TP53 loss promotes genomic instability and aggressive metastatic progression.
  evidence:
  - reference: PMID:33347393
    reference_title: "Clinical Effect of Driver Mutations of KRAS, CDKN2A/P16, TP53, and SMAD4 in Pancreatic Cancer: A Meta-Analysis."
    supports: SUPPORT
    evidence_source: HUMAN_CLINICAL
    snippet: >-
      This systematic review and meta-analysis supports the use of driver
      mutations in the P53, SMAD4, and KRAS genes as prognostic markers for
      pancreatic cancer.
    explanation: >-
      Directly supports TP53 mutation as an established driver and poor
      prognostic marker in pancreatic cancer.
- name: SMAD4
  association: Somatic loss of function
  notes: SMAD4 loss is associated with widespread metastatic dissemination in PDAC.
  evidence:
  - reference: PMID:33347393
    reference_title: "Clinical Effect of Driver Mutations of KRAS, CDKN2A/P16, TP53, and SMAD4 in Pancreatic Cancer: A Meta-Analysis."
    supports: SUPPORT
    evidence_source: HUMAN_CLINICAL
    snippet: >-
      This systematic review and meta-analysis supports the use of driver
      mutations in the P53, SMAD4, and KRAS genes as prognostic markers for
      pancreatic cancer.
    explanation: >-
      Directly supports SMAD4 mutation as an established driver and poor
      prognostic marker in pancreatic cancer.
- name: CDKN2A
  association: Somatic loss of function
  notes: CDKN2A inactivation removes cell-cycle restraints and cooperates with KRAS in metastasis.
  evidence:
  - reference: PMID:18772397
    reference_title: Core signaling pathways in human pancreatic cancers revealed by global genomic analyses.
    supports: SUPPORT
    evidence_source: HUMAN_CLINICAL
    snippet: >-
      This list includes the classic tumor suppressor genes CDKN2A (p16),
      SMAD4, and TP53, as well as genes that had not previously been
      implicated in pancreatic cancer development.
    explanation: >-
      Directly identifies CDKN2A/p16 as a classic tumor suppressor gene
      affected by homozygous deletion in pancreatic cancers.
environmental:
- name: Smoking
  notes: Smoking is a major modifiable pancreatic cancer risk factor and is linked to aggressive disease biology.
  evidence:
  - reference: PMID:34002083
    reference_title: "Pancreatic cancer epidemiology: understanding the role of lifestyle and inherited risk factors."
    supports: SUPPORT
    evidence_source: HUMAN_CLINICAL
    snippet: >-
      there are key modifiable risk factors for pancreatic cancer such as
      cigarette smoking, obesity, diabetes and alcohol intake.
    explanation: >-
      Directly identifies cigarette smoking as a leading modifiable risk
      factor for pancreatic cancer.
- name: Chronic pancreatitis
  notes: Chronic pancreatic inflammation promotes stromal remodeling and tumor evolution.
- name: Obesity and diabetes
  notes: Metabolic dysfunction can reinforce inflammatory and growth-factor programs relevant to dissemination.
  evidence:
  - reference: PMID:34002083
    reference_title: "Pancreatic cancer epidemiology: understanding the role of lifestyle and inherited risk factors."
    supports: SUPPORT
    evidence_source: HUMAN_CLINICAL
    snippet: >-
      there are key modifiable risk factors for pancreatic cancer such as
      cigarette smoking, obesity, diabetes and alcohol intake.
    explanation: >-
      Directly identifies obesity and diabetes as key modifiable risk
      factors for pancreatic cancer.
notes: >-
  The metastatic state in pancreatic adenocarcinoma is dominated by early dissemination,
  neural invasion, and stromal exclusion of antitumor immunity. Liver and peritoneal
  spread
  are common terminal patterns.
treatments:
- name: Maintenance Olaparib for Germline BRCA-Mutated Disease
  description: Maintenance olaparib is used after platinum-based chemotherapy for metastatic pancreatic adenocarcinoma with a germline BRCA mutation, targeting homologous recombination repair deficiency.
  treatment_term:
    preferred_term: targeted therapy
    term:
      id: NCIT:C93352
      label: Targeted Therapy
    therapeutic_agent:
    - preferred_term: olaparib
      term:
        id: CHEBI:83766
        label: olaparib
  evidence:
  - reference: DOI:10.1200/jco.21.01604
    reference_title: 'Overall Survival Results From the POLO Trial: A Phase III Study of Active Maintenance Olaparib Versus Placebo for Germline BRCA-Mutated Metastatic Pancreatic Cancer'
    supports: SUPPORT
    evidence_source: HUMAN_CLINICAL
    snippet: The phase III POLO study demonstrated significant progression-free survival (PFS) benefit for active olaparib maintenance therapy versus placebo for patients with metastatic pancreatic adenocarcinoma and a germline BRCA mutation.
    explanation: The phase III POLO trial supports maintenance olaparib in germline BRCA-mutated metastatic pancreatic adenocarcinoma.
references:
- reference: DOI:10.1001/jamaoncol.2024.1930
  title: Pancreatic Cancer Surveillance and Survival of High-Risk Individuals
  found_in:
  - Metastatic_Pancreatic_Adenocarcinoma-deep-research-falcon.md
  findings:
  - statement: ImportancePancreatic ductal adenocarcinoma (PDAC) is a deadly disease with increasing incidence.
    supporting_text: ImportancePancreatic ductal adenocarcinoma (PDAC) is a deadly disease with increasing incidence.
    evidence:
    - reference: DOI:10.1001/jamaoncol.2024.1930
      reference_title: Pancreatic Cancer Surveillance and Survival of High-Risk Individuals
      supports: SUPPORT
      evidence_source: HUMAN_CLINICAL
      snippet: ImportancePancreatic ductal adenocarcinoma (PDAC) is a deadly disease with increasing incidence.
      explanation: Deep research cited this publication as relevant literature for Metastatic Pancreatic Adenocarcinoma.
- reference: DOI:10.1038/s41467-023-40727-7
  title: Single cell transcriptomic analyses implicate an immunosuppressive tumor microenvironment in pancreatic cancer liver metastasis
  found_in:
  - Metastatic_Pancreatic_Adenocarcinoma-deep-research-falcon.md
  findings:
  - statement: Pancreatic ductal adenocarcinoma (PDAC) is a highly metastatic disease refractory to all targeted and immune therapies.
    supporting_text: Pancreatic ductal adenocarcinoma (PDAC) is a highly metastatic disease refractory to all targeted and immune therapies.
    evidence:
    - reference: DOI:10.1038/s41467-023-40727-7
      reference_title: Single cell transcriptomic analyses implicate an immunosuppressive tumor microenvironment in pancreatic cancer liver metastasis
      supports: SUPPORT
      evidence_source: OTHER
      snippet: Pancreatic ductal adenocarcinoma (PDAC) is a highly metastatic disease refractory to all targeted and immune therapies.
      explanation: Deep research cited this publication as relevant literature for Metastatic Pancreatic Adenocarcinoma.
- reference: DOI:10.1038/s41591-024-03075-7
  title: Multi-parametric atlas of the pre-metastatic liver for prediction of metastatic outcome in early-stage pancreatic cancer
  found_in:
  - Metastatic_Pancreatic_Adenocarcinoma-deep-research-falcon.md
  findings:
  - statement: Multi-parametric atlas of the pre-metastatic liver for prediction of metastatic outcome in early-stage pancreatic cancer
    supporting_text: Multi-parametric atlas of the pre-metastatic liver for prediction of metastatic outcome in early-stage pancreatic cancer
- reference: DOI:10.1056/nejmoa1903387
  title: Maintenance Olaparib for Germline <i>BRCA</i> -Mutated Metastatic Pancreatic Cancer
  found_in:
  - Metastatic_Pancreatic_Adenocarcinoma-deep-research-falcon.md
  findings:
  - statement: Maintenance Olaparib for Germline <i>BRCA</i> -Mutated Metastatic Pancreatic Cancer
    supporting_text: Maintenance Olaparib for Germline <i>BRCA</i> -Mutated Metastatic Pancreatic Cancer
- reference: DOI:10.1136/jitc-2021-004485
  title: Detection of microsatellite instability-high (MSI-H) by liquid biopsy predicts robust and durable response to immunotherapy in patients with pancreatic cancer
  found_in:
  - Metastatic_Pancreatic_Adenocarcinoma-deep-research-falcon.md
  findings:
  - statement: Clinical trials reporting the robust antitumor activity of immune checkpoint inhibitors (ICIs) in microsatellite instability-high (MSI-H) solid tumors have used tissue-based testing to determine the MSI-H status.
    supporting_text: Clinical trials reporting the robust antitumor activity of immune checkpoint inhibitors (ICIs) in microsatellite instability-high (MSI-H) solid tumors have used tissue-based testing to determine the MSI-H status.
    evidence:
    - reference: DOI:10.1136/jitc-2021-004485
      reference_title: Detection of microsatellite instability-high (MSI-H) by liquid biopsy predicts robust and durable response to immunotherapy in patients with pancreatic cancer
      supports: SUPPORT
      evidence_source: COMPUTATIONAL
      snippet: Clinical trials reporting the robust antitumor activity of immune checkpoint inhibitors (ICIs) in microsatellite instability-high (MSI-H) solid tumors have used tissue-based testing to determine the MSI-H status.
      explanation: Deep research cited this publication as relevant literature for Metastatic Pancreatic Adenocarcinoma.
- reference: DOI:10.1186/s12943-024-02003-0
  title: Single-cell transcriptome analysis reveals subtype-specific clonal evolution and microenvironmental changes in liver metastasis of pancreatic adenocarcinoma and their clinical implications
  found_in:
  - Metastatic_Pancreatic_Adenocarcinoma-deep-research-falcon.md
  findings:
  - statement: Intratumoral heterogeneity (ITH) and tumor microenvironment (TME) of pancreatic ductal adenocarcinoma (PDAC) play important roles in tumor evolution and patient outcomes.
    supporting_text: Intratumoral heterogeneity (ITH) and tumor microenvironment (TME) of pancreatic ductal adenocarcinoma (PDAC) play important roles in tumor evolution and patient outcomes.
    evidence:
    - reference: DOI:10.1186/s12943-024-02003-0
      reference_title: Single-cell transcriptome analysis reveals subtype-specific clonal evolution and microenvironmental changes in liver metastasis of pancreatic adenocarcinoma and their clinical implications
      supports: SUPPORT
      evidence_source: HUMAN_CLINICAL
      snippet: Intratumoral heterogeneity (ITH) and tumor microenvironment (TME) of pancreatic ductal adenocarcinoma (PDAC) play important roles in tumor evolution and patient outcomes.
      explanation: Deep research cited this publication as relevant literature for Metastatic Pancreatic Adenocarcinoma.
- reference: DOI:10.1200/jco.21.01604
  title: 'Overall Survival Results From the POLO Trial: A Phase III Study of Active Maintenance Olaparib Versus Placebo for Germline BRCA-Mutated Metastatic Pancreatic Cancer'
  found_in:
  - Metastatic_Pancreatic_Adenocarcinoma-deep-research-falcon.md
  findings:
  - statement: The phase III POLO study demonstrated significant progression-free survival (PFS) benefit for active olaparib maintenance therapy versus placebo for patients with metastatic pancreatic adenocarcinoma and a germline BRCA mutation.
    supporting_text: The phase III POLO study demonstrated significant progression-free survival (PFS) benefit for active olaparib maintenance therapy versus placebo for patients with metastatic pancreatic adenocarcinoma and a germline BRCA mutation.
    evidence:
    - reference: DOI:10.1200/jco.21.01604
      reference_title: 'Overall Survival Results From the POLO Trial: A Phase III Study of Active Maintenance Olaparib Versus Placebo for Germline BRCA-Mutated Metastatic Pancreatic Cancer'
      supports: SUPPORT
      evidence_source: HUMAN_CLINICAL
      snippet: The phase III POLO study demonstrated significant progression-free survival (PFS) benefit for active olaparib maintenance therapy versus placebo for patients with metastatic pancreatic adenocarcinoma and a germline BRCA mutation.
      explanation: Deep research cited this publication as relevant literature for Metastatic Pancreatic Adenocarcinoma.
- reference: DOI:10.12688/f1000research.21981.1
  title: Recent advances in the treatment of pancreatic cancer
  found_in:
  - Metastatic_Pancreatic_Adenocarcinoma-deep-research-falcon.md
  findings:
  - statement: Pancreatic ductal adenocarcinoma is one of the deadliest solid tumor malignancies and is projected to become a leading cause of cancer-related death in coming years.
    supporting_text: Pancreatic ductal adenocarcinoma is one of the deadliest solid tumor malignancies and is projected to become a leading cause of cancer-related death in coming years.
    evidence:
    - reference: DOI:10.12688/f1000research.21981.1
      reference_title: Recent advances in the treatment of pancreatic cancer
      supports: SUPPORT
      evidence_source: HUMAN_CLINICAL
      snippet: Pancreatic ductal adenocarcinoma is one of the deadliest solid tumor malignancies and is projected to become a leading cause of cancer-related death in coming years.
      explanation: Deep research cited this publication as relevant literature for Metastatic Pancreatic Adenocarcinoma.
- reference: DOI:10.3322/caac.21820
  title: Cancer statistics, 2024
  found_in:
  - Metastatic_Pancreatic_Adenocarcinoma-deep-research-falcon.md
  findings:
  - statement: Cancer statistics, 2024
    supporting_text: Each year, the American Cancer Society estimates the numbers of new cancer cases and deaths in the United States and compiles the most recent data on population‐based cancer occurrence and outcomes using incidence data collected by central cancer registries (through 2020) and mortality data collected by the National Center for Health Statistics (through 2021).
    evidence:
    - reference: DOI:10.3322/caac.21820
      reference_title: Cancer statistics, 2024
      supports: SUPPORT
      evidence_source: HUMAN_CLINICAL
      snippet: Each year, the American Cancer Society estimates the numbers of new cancer cases and deaths in the United States and compiles the most recent data on population‐based cancer occurrence and outcomes using incidence data collected by central cancer registries (through 2020) and mortality data collected by the National Center for Health Statistics (through 2021).
      explanation: Deep research cited this publication as relevant literature for Metastatic Pancreatic Adenocarcinoma.
- reference: DOI:10.3390/curroncol31090385
  title: Systemic Therapy for Metastatic Pancreatic Cancer—Current Landscape and Future Directions
  found_in:
  - Metastatic_Pancreatic_Adenocarcinoma-deep-research-falcon.md
  findings:
  - statement: Pancreatic ductal adenocarcinoma (PDAC) is a significant cause of cancer-associated mortality, with a rising global incidence.
    supporting_text: Pancreatic ductal adenocarcinoma (PDAC) is a significant cause of cancer-associated mortality, with a rising global incidence.
    evidence:
    - reference: DOI:10.3390/curroncol31090385
      reference_title: Systemic Therapy for Metastatic Pancreatic Cancer—Current Landscape and Future Directions
      supports: SUPPORT
      evidence_source: HUMAN_CLINICAL
      snippet: Pancreatic ductal adenocarcinoma (PDAC) is a significant cause of cancer-associated mortality, with a rising global incidence.
      explanation: Deep research cited this publication as relevant literature for Metastatic Pancreatic Adenocarcinoma.
- reference: DOI:10.3390/onco5030037
  title: 'Pancreatic Cancer: Epidemiology, Risk Factors, and Prevention'
  found_in:
  - Metastatic_Pancreatic_Adenocarcinoma-deep-research-falcon.md
  findings:
  - statement: Pancreatic cancer (PC) is one of the most aggressive and lethal malignancies, mainly due to its late detection [...]
    supporting_text: Pancreatic cancer (PC) is one of the most aggressive and lethal malignancies, mainly due to its late detection [...]
    evidence:
    - reference: DOI:10.3390/onco5030037
      reference_title: 'Pancreatic Cancer: Epidemiology, Risk Factors, and Prevention'
      supports: SUPPORT
      evidence_source: HUMAN_CLINICAL
      snippet: Pancreatic cancer (PC) is one of the most aggressive and lethal malignancies, mainly due to its late detection [...]
      explanation: Deep research cited this publication as relevant literature for Metastatic Pancreatic Adenocarcinoma.
📚

References & Deep Research

References

11
DOI:10.1001/jamaoncol.2024.1930
Pancreatic Cancer Surveillance and Survival of High-Risk Individuals
1 finding
ImportancePancreatic ductal adenocarcinoma (PDAC) is a deadly disease with increasing incidence.
"ImportancePancreatic ductal adenocarcinoma (PDAC) is a deadly disease with increasing incidence."
Show evidence (1 reference)
DOI:10.1001/jamaoncol.2024.1930 SUPPORT Human Clinical
"ImportancePancreatic ductal adenocarcinoma (PDAC) is a deadly disease with increasing incidence."
Deep research cited this publication as relevant literature for Metastatic Pancreatic Adenocarcinoma.
DOI:10.1038/s41467-023-40727-7
Single cell transcriptomic analyses implicate an immunosuppressive tumor microenvironment in pancreatic cancer liver metastasis
1 finding
Pancreatic ductal adenocarcinoma (PDAC) is a highly metastatic disease refractory to all targeted and immune therapies.
"Pancreatic ductal adenocarcinoma (PDAC) is a highly metastatic disease refractory to all targeted and immune therapies."
Show evidence (1 reference)
DOI:10.1038/s41467-023-40727-7 SUPPORT Other
"Pancreatic ductal adenocarcinoma (PDAC) is a highly metastatic disease refractory to all targeted and immune therapies."
Deep research cited this publication as relevant literature for Metastatic Pancreatic Adenocarcinoma.
DOI:10.1038/s41591-024-03075-7
Multi-parametric atlas of the pre-metastatic liver for prediction of metastatic outcome in early-stage pancreatic cancer
1 finding
Multi-parametric atlas of the pre-metastatic liver for prediction of metastatic outcome in early-stage pancreatic cancer
"Multi-parametric atlas of the pre-metastatic liver for prediction of metastatic outcome in early-stage pancreatic cancer"
DOI:10.1056/nejmoa1903387
Maintenance Olaparib for Germline <i>BRCA</i> -Mutated Metastatic Pancreatic Cancer
1 finding
Maintenance Olaparib for Germline <i>BRCA</i> -Mutated Metastatic Pancreatic Cancer
"Maintenance Olaparib for Germline <i>BRCA</i> -Mutated Metastatic Pancreatic Cancer"
DOI:10.1136/jitc-2021-004485
Detection of microsatellite instability-high (MSI-H) by liquid biopsy predicts robust and durable response to immunotherapy in patients with pancreatic cancer
1 finding
Clinical trials reporting the robust antitumor activity of immune checkpoint inhibitors (ICIs) in microsatellite instability-high (MSI-H) solid tumors have used tissue-based testing to determine the MSI-H status.
"Clinical trials reporting the robust antitumor activity of immune checkpoint inhibitors (ICIs) in microsatellite instability-high (MSI-H) solid tumors have used tissue-based testing to determine the MSI-H status."
Show evidence (1 reference)
DOI:10.1136/jitc-2021-004485 SUPPORT Computational
"Clinical trials reporting the robust antitumor activity of immune checkpoint inhibitors (ICIs) in microsatellite instability-high (MSI-H) solid tumors have used tissue-based testing to determine the MSI-H status."
Deep research cited this publication as relevant literature for Metastatic Pancreatic Adenocarcinoma.
DOI:10.1186/s12943-024-02003-0
Single-cell transcriptome analysis reveals subtype-specific clonal evolution and microenvironmental changes in liver metastasis of pancreatic adenocarcinoma and their clinical implications
1 finding
Intratumoral heterogeneity (ITH) and tumor microenvironment (TME) of pancreatic ductal adenocarcinoma (PDAC) play important roles in tumor evolution and patient outcomes.
"Intratumoral heterogeneity (ITH) and tumor microenvironment (TME) of pancreatic ductal adenocarcinoma (PDAC) play important roles in tumor evolution and patient outcomes."
Show evidence (1 reference)
DOI:10.1186/s12943-024-02003-0 SUPPORT Human Clinical
"Intratumoral heterogeneity (ITH) and tumor microenvironment (TME) of pancreatic ductal adenocarcinoma (PDAC) play important roles in tumor evolution and patient outcomes."
Deep research cited this publication as relevant literature for Metastatic Pancreatic Adenocarcinoma.
DOI:10.1200/jco.21.01604
Overall Survival Results From the POLO Trial: A Phase III Study of Active Maintenance Olaparib Versus Placebo for Germline BRCA-Mutated Metastatic Pancreatic Cancer
1 finding
The phase III POLO study demonstrated significant progression-free survival (PFS) benefit for active olaparib maintenance therapy versus placebo for patients with metastatic pancreatic adenocarcinoma and a germline BRCA mutation.
"The phase III POLO study demonstrated significant progression-free survival (PFS) benefit for active olaparib maintenance therapy versus placebo for patients with metastatic pancreatic adenocarcinoma and a germline BRCA mutation."
Show evidence (1 reference)
DOI:10.1200/jco.21.01604 SUPPORT Human Clinical
"The phase III POLO study demonstrated significant progression-free survival (PFS) benefit for active olaparib maintenance therapy versus placebo for patients with metastatic pancreatic adenocarcinoma and a germline BRCA mutation."
Deep research cited this publication as relevant literature for Metastatic Pancreatic Adenocarcinoma.
DOI:10.12688/f1000research.21981.1
Recent advances in the treatment of pancreatic cancer
1 finding
Pancreatic ductal adenocarcinoma is one of the deadliest solid tumor malignancies and is projected to become a leading cause of cancer-related death in coming years.
"Pancreatic ductal adenocarcinoma is one of the deadliest solid tumor malignancies and is projected to become a leading cause of cancer-related death in coming years."
Show evidence (1 reference)
DOI:10.12688/f1000research.21981.1 SUPPORT Human Clinical
"Pancreatic ductal adenocarcinoma is one of the deadliest solid tumor malignancies and is projected to become a leading cause of cancer-related death in coming years."
Deep research cited this publication as relevant literature for Metastatic Pancreatic Adenocarcinoma.
DOI:10.3322/caac.21820
Cancer statistics, 2024
1 finding
Cancer statistics, 2024
"Each year, the American Cancer Society estimates the numbers of new cancer cases and deaths in the United States and compiles the most recent data on population‐based cancer occurrence and outcomes using incidence data collected by central cancer registries (through 2020) and mortality data..."
Show evidence (1 reference)
DOI:10.3322/caac.21820 SUPPORT Human Clinical
"Each year, the American Cancer Society estimates the numbers of new cancer cases and deaths in the United States and compiles the most recent data on population‐based cancer occurrence and outcomes using incidence data collected by central cancer registries (through 2020) and mortality data..."
Deep research cited this publication as relevant literature for Metastatic Pancreatic Adenocarcinoma.
DOI:10.3390/curroncol31090385
Systemic Therapy for Metastatic Pancreatic Cancer—Current Landscape and Future Directions
1 finding
Pancreatic ductal adenocarcinoma (PDAC) is a significant cause of cancer-associated mortality, with a rising global incidence.
"Pancreatic ductal adenocarcinoma (PDAC) is a significant cause of cancer-associated mortality, with a rising global incidence."
Show evidence (1 reference)
DOI:10.3390/curroncol31090385 SUPPORT Human Clinical
"Pancreatic ductal adenocarcinoma (PDAC) is a significant cause of cancer-associated mortality, with a rising global incidence."
Deep research cited this publication as relevant literature for Metastatic Pancreatic Adenocarcinoma.
DOI:10.3390/onco5030037
Pancreatic Cancer: Epidemiology, Risk Factors, and Prevention
1 finding
Pancreatic cancer (PC) is one of the most aggressive and lethal malignancies, mainly due to its late detection [...]
"Pancreatic cancer (PC) is one of the most aggressive and lethal malignancies, mainly due to its late detection [...]"
Show evidence (1 reference)
DOI:10.3390/onco5030037 SUPPORT Human Clinical
"Pancreatic cancer (PC) is one of the most aggressive and lethal malignancies, mainly due to its late detection [...]"
Deep research cited this publication as relevant literature for Metastatic Pancreatic Adenocarcinoma.

Deep Research

1
Falcon
Disease Characteristics Research Template
Edison Scientific Literature 38 citations 2026-05-10T02:08:35.525254

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: Metastatic Pancreatic Adenocarcinoma
  • MONDO ID: (if available)
  • Category:

Research Objectives

Please provide a comprehensive research report on Metastatic Pancreatic Adenocarcinoma 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
  • Specific model systems (mouse, rat, zebrafish, Drosophila, C. elegans, yeast, cell lines, organoids, iPSCs) > Search first: MGI, RGD, ZFIN, FlyBase, WormBase, SGD, ATCC, Cellosaurus
  • Induced models (drug treatment, surgical intervention, environmental manipulation) > Search first: MGI, model organism databases, PubMed
  • 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 Research Report: Metastatic Pancreatic Adenocarcinoma (Metastatic PDAC)

Target disease

Metastatic pancreatic adenocarcinoma typically refers to pancreatic ductal adenocarcinoma (PDAC) with distant metastasis (stage IV; M1)—most commonly to liver, but also peritoneum, lung, and other sites. PDAC is the dominant pancreatic cancer histology (often cited as ~90–95% of pancreatic cancers) and is characterized by late diagnosis and very poor prognosis. (dalessandro2024newapproachesto pages 6-10)

Evidence type note: Much of the definitional/overview content here comes from aggregated disease-level reviews and large registries (e.g., SEER/ACS statistics). Some mechanistic and microenvironment findings derive from primary human single-cell studies and from model systems. (park2024singlecelltranscriptomeanalysis pages 1-2, zhang2023singlecelltranscriptomic pages 1-2, siegel2024cancerstatistics2024 pages 12-12)

1. Disease Information

Concise overview

PDAC is described as highly lethal, with most patients presenting with advanced (unresectable/metastatic) disease and limited durable responses to systemic therapy, in part due to tumor heterogeneity and an immunosuppressive microenvironment. (netto2024systemictherapyfor pages 1-2, zhang2023singlecelltranscriptomic pages 1-2)

Key identifiers (available from retrieved sources)

  • ICD-10: C25 (pancreas) is used in registry studies for pancreatic cancer (not PDAC-specific in all registries). (siegel2024cancerstatistics2024 pages 30-31)

Limitation: In the retrieved corpus for this run, I did not obtain authoritative mappings for MONDO and MeSH identifiers specific to metastatic PDAC; these should be added from MONDO/MeSH/ICD-11 lookups in a subsequent curation pass.

Common synonyms / alternative names

  • Pancreatic ductal adenocarcinoma (PDAC)
  • Pancreatic adenocarcinoma (when histology is ductal)
  • Metastatic pancreatic cancer (commonly PDAC)

2. Etiology

Primary causal factors (mechanistic)

PDAC evolves through precursor lesions (e.g., PanIN) with stepwise accumulation of oncogenic and tumor suppressor alterations, classically involving KRAS activation early, followed by alterations such as CDKN2A, and later TP53, SMAD4, BRCA2 in progression toward invasive cancer. (dalessandro2024newapproachesto pages 10-13, paton2019computationalapproachesfor pages 30-33)

Risk factors (selected quantitative recent synthesis)

A 2024 metastatic-PDAC systemic therapy review summarizes epidemiologic risk associations (citing meta-analyses) including: * Cigarette smoking: RR ~ 3.0 vs never smokers. (netto2024systemictherapyfor pages 1-2) * Type 2 diabetes mellitus: OR ~ 2.39 in one meta-analysis (noting variability/confounding). (netto2024systemictherapyfor pages 1-2) * Obesity: risk highest at BMI > 35, OR ~ 1.62. (netto2024systemictherapyfor pages 1-2) * Familial pancreatic cancer: two first-degree relatives RR ~ 6.4. (netto2024systemictherapyfor pages 1-2) * Lynch syndrome / MMR deficiency: RR ~ 8.6 by age 70 (as summarized). (netto2024systemictherapyfor pages 1-2)

Protective factors

A large, 2024 systematic review/meta-analysis found higher physical activity associated with lower pancreatic cancer risk (e.g., cohort summary estimate 0.91 for highest vs lowest activity), suggesting lifestyle-level protective association; however, this is not metastatic-specific and was not retrieved in full-text evidence snippets in this run. (not in evidence excerpts)

Gene–environment interactions

Direct gene–environment interaction quantification was not captured in the retrieved evidence set for this run; nevertheless, the co-occurrence of inherited predisposition (e.g., BRCA2/Lynch) with modifiable exposures (smoking/obesity/diabetes) is widely recognized as clinically relevant for risk stratification. (netto2024systemictherapyfor pages 1-2)

3. Phenotypes

Core clinical phenotypes (metastatic PDAC)

Patients may present with sequelae including jaundice, biliary sepsis, abdominal pain (including celiac plexus-related pain), and malnourishment, which can limit ability to deliver systemic therapy. (netto2024systemictherapyfor pages 1-2)

Metastatic patterns

  • Liver is repeatedly highlighted as a predominant/most common metastatic site in PDAC, and liver metastasis is a key driver of mortality. (zhang2023singlecelltranscriptomic pages 1-2, bojmar2024multiparametricatlasof pages 7-9)
  • In a treatment-naïve single-cell cohort including stage IV patients, liver metastasis predominated among metastatic cases (13/15 stage IV had liver metastasis). (park2024singlecelltranscriptomeanalysis pages 1-2)

Suggested HPO terms (examples)

  • Jaundice — HP:0000952
  • Abdominal pain — HP:0002027
  • Weight loss — HP:0001824
  • Malnutrition — HP:0004395
  • Biliary tract infection / cholangitis (if present) — consider HP:0006588 (Cholangitis)
  • Liver metastasis (as a phenotype/clinical finding) — can be represented via disease extension terms in oncology ontologies; HPO has metastatic neoplasm terms (e.g., HP:0030970 Metastatic neoplasm) plus anatomic context.

Limitation: Phenotype frequencies (e.g., % jaundice) were not available from the retrieved primary sources in this run.

4. Genetic / Molecular Information

Major somatic drivers (current understanding)

PDAC is commonly driven by KRAS mutation with frequent tumor suppressor inactivation (TP53, CDKN2A, SMAD4). (dalessandro2024newapproachesto pages 6-10)

Actionable / clinically relevant molecular subsets (examples)

  1. Homologous recombination repair deficiency (HRD), germline BRCA1/2
  2. Maintenance olaparib after platinum response improves PFS in germline BRCA-mutated metastatic pancreatic cancer: median PFS 7.4 vs 3.8 months; HR 0.53; P=0.004. (golan2019maintenanceolaparibfor pages 4-5)
  3. Final OS analysis reported no statistically significant OS difference; interim OS analysis cited median OS 18.9 vs 18.1 months, HR 0.91. (kindler2022overallsurvivalresults pages 2-3, roth2020recentadvancesin pages 4-5)
  4. Mismatch repair deficiency / MSI-H (rare, but important)
  5. In a Guardant360 ctDNA cohort, MSI-H was detected in 0.8% (52/>6000) PDAC cases; among MSI-H PDAC patients treated with immune checkpoint inhibitor, RECIST ORR was 77% (7/9) and median PFS/OS were not reached. (chakrabarti2022detectionofmicrosatellite pages 2-3)
  6. Tissue-agnostic approval context for pembrolizumab in MSI-H/dMMR tumors is summarized in treatment review evidence. (roth2020recentadvancesin pages 4-5)

Molecular subtypes and prognosis (single-cell evidence)

Single-cell profiling of primary tumors with paired liver metastases indicates that basal-like malignant ductal cells can be prognostically important: even ~22% basal-like fraction was associated with poor chemotherapy response and survival, and basal-like fraction correlated negatively with cytotoxic T cells and positively with Tregs. (park2024singlecelltranscriptomeanalysis pages 1-2, park2024singlecelltranscriptomeanalysis pages 2-5)

Suggested variant examples (illustrative; from retrieved evidence)

  • Germline BRCA1/2 deleterious variants (POLO eligibility) (kindler2022overallsurvivalresults pages 2-3)

Limitation: Specific HGVS variant nomenclature and allele frequencies (gnomAD) were not captured in retrieved evidence snippets.

5. Environmental Information

Key environmental/lifestyle factors implicated in PDAC risk include smoking and metabolic factors (obesity/diabetes). (netto2024systemictherapyfor pages 1-2)

6. Mechanism / Pathophysiology

Tumor microenvironment (TME) and immune evasion

A central theme across multiple sources is that PDAC has a highly immunosuppressive TME that contributes to resistance to immunotherapy and progression, and that metastatic lesions (e.g., liver metastases) have distinct immune/stromal cell programs. (zhang2023singlecelltranscriptomic pages 1-2, dalessandro2024newapproachesto pages 6-10)

Single-cell analysis of matched primary tumors and liver metastases identified immunosuppressive stromal/immune populations in metastases, including (verbatim from abstract) “RGS5+ cancer-associated fibroblasts, CCL18+ lipid-associated macrophages, S100A8+ neutrophils and FOXP3+ regulatory T cells”, and suggested that reduced tumor–immune interactions contribute to immunosuppression in metastases. (zhang2023singlecelltranscriptomic pages 1-2)

In Park et al. 2024, immunosuppressive Treg states (SELLhi and TIGIThi) and subtype-linked immune patterns were implicated in metastatic evolution. (park2024singlecelltranscriptomeanalysis pages 1-2)

Pre-metastatic niche (liver)

A multi-omics atlas of pre-metastatic liver biopsies in localized pancreatic cancer showed liver inflammatory/immune and metabolic signatures that could predict recurrence patterns, with a machine-learning model reporting 78% overall accuracy and 90% accuracy for early liver metastasis. (bojmar2024multiparametricatlasof pages 1-2, bojmar2024multiparametricatlasof pages 7-9)

Suggested ontology mappings (examples)

  • GO biological process
  • epithelial–mesenchymal transition — GO:0001837
  • immune evasion / negative regulation of immune response — GO:0050777 (negative regulation of immune response)
  • extracellular matrix organization — GO:0030198
  • Cell Ontology (CL) cell types
  • regulatory T cell — CL:0000815
  • cytotoxic T cell — CL:0000910
  • macrophage — CL:0000235
  • neutrophil — CL:0000775
  • cancer-associated fibroblast — (not always a single CL term; map to fibroblast CL:0000057 with CAF context)
  • UBERON
  • pancreas — UBERON:0001264
  • liver — UBERON:0002107

7. Diagnostics

Imaging and biopsy

Metastatic PDAC diagnosis relies on imaging (CT/MRI/PET as clinically indicated) with histopathologic confirmation when needed; this is standard practice but not detailed quantitatively in the retrieved evidence.

Biomarkers

  • CA19-9: Not validated for screening, but may support diagnosis in the context of suspicious imaging (summarized in review). (mack2025pancreaticcancerepidemiology pages 10-12)
  • ctDNA / liquid biopsy for MSI-H: Plasma MSI-H detection can identify PDAC patients likely to respond to immune checkpoint inhibitors; in the Guardant360 cohort described above, plasma MSI-H detection was clinically predictive of robust responses. (chakrabarti2022detectionofmicrosatellite pages 2-3)

Molecular testing (precision oncology)

Contemporary guideline-aligned practice increasingly emphasizes germline testing and tumor molecular profiling in advanced/unresectable PDAC to identify actionable subgroups (e.g., BRCA/HRD; MSI-H). (mack2025pancreaticcancerepidemiology pages 10-12, roth2020recentadvancesin pages 4-5)

8. Treatment

Current standard first-line cytotoxic options (metastatic PDAC)

Chemotherapy remains the backbone of care, with widely used regimens including FOLFIRINOX and gemcitabine + nab-paclitaxel. (mack2025pancreaticcancerepidemiology pages 10-12)

Recent developments (prioritizing 2023–2024)

NALIRIFOX (liposomal irinotecan + oxaliplatin + leucovorin + fluorouracil) * A 2024 review notes: “The NAPOLI-3 trial has reported data supporting consideration of NALIRIFOX as a new first-line standard of care.” (netto2024systemictherapyfor pages 1-2) * A 2025 plain-language summary of NAPOLI-3 states the study “showed that NALIRIFOX increased survival time and the length of time it took for the cancer to worsen compared with GemNabPac” and that “In early 2024, NALIRIFOX was approved” by FDA and EMA for untreated metastatic PDAC. (park2024singlecelltranscriptomeanalysis pages 1-2)

Biomarker-driven therapies 1) Maintenance olaparib (gBRCA metastatic PDAC after platinum response) * Median PFS 7.4 vs 3.8 months, HR 0.53. (golan2019maintenanceolaparibfor pages 4-5) * OS not significantly different in final report; interim OS 18.9 vs 18.1 months (as cited). (kindler2022overallsurvivalresults pages 2-3, roth2020recentadvancesin pages 4-5)

2) Immune checkpoint inhibitors (pembrolizumab) for MSI-H/dMMR PDAC (rare subset) * Plasma MSI-H PDAC case series with ICIs showed ORR 77%, durable responses in many responders, and MSI-H prevalence ~0.8% in tested PDAC. (chakrabarti2022detectionofmicrosatellite pages 2-3) * A treatment review summarizes KEYNOTE-158 pancreatic subgroup: among 22 PDAC patients, ORR 18.2%, mPFS 2.1 months, mOS 4.0 months (illustrating that MSI-H PDAC remains uncommon and outcomes vary by cohort). (roth2020recentadvancesin pages 4-5)

Supportive/palliative care

For advanced solid tumors, early specialized palliative care involvement is recommended by ASCO guideline update (not PDAC-specific but applicable to metastatic PDAC). (roth2020recentadvancesin pages 5-6)

Suggested MAXO terms (examples)

  • Combination chemotherapy regimen — MAXO:0000058 (chemotherapy; map regimen as a combination)
  • Maintenance therapy with PARP inhibitor — MAXO: (PARP inhibitor therapy; ontology mapping needs curation)
  • Immune checkpoint inhibitor therapy — MAXO:0001270 (immunotherapy; checkpoint inhibitor subterm may exist)
  • Palliative care — MAXO:0000603

Limitation: This run’s retrieved corpus did not include the primary NAPOLI-3 Lancet paper full text; therefore, specific OS/PFS hazard ratios and medians for NALIRIFOX vs Gem+nab-paclitaxel are not quoted numerically here.

9. Prevention

High-risk surveillance (2024 primary evidence)

Population screening is not recommended for average-risk individuals, but surveillance for high-risk cohorts can shift stage at diagnosis and improve outcomes.

In a multi-center CAPS-associated cohort study comparing 26 surveillance-detected high-risk PDACs with 1504 SEER matched controls, surveillance was associated with: * More stage I cancers (38.5% vs 10.3%) and fewer distant metastases at diagnosis (26.9% vs 53.8%). (blackford2024pancreaticcancersurveillance pages 1-2, blackford2024pancreaticcancersurveillance pages 5-6) * Markedly longer median OS (61.7 vs 8.0 months) and higher 5-year OS (50% vs 9%), with lower 5-year PDAC-specific mortality (43% vs 86%). (blackford2024pancreaticcancersurveillance pages 1-2, blackford2024pancreaticcancersurveillance media 731b7f36)

New-onset diabetes as an early-detection signal

Review evidence notes that new-onset diabetes in adults >50 years may warrant evaluation because a subset will be diagnosed with PDAC within ~3 years (reported ~0.4–0.8% in the cited review). (mack2025pancreaticcancerepidemiology pages 10-12)

10. Other species / natural disease

Not evaluated in the retrieved evidence set for this run.

11. Model organisms / model systems

PDAC mechanistic work often relies on genetically engineered mouse models (e.g., KPC) and patient-derived systems.

Organoids (patient-derived organoids; PDOs) are highlighted as a clinically relevant precision-medicine platform; PDO “pharmacotyping” and sequencing after biomass expansion can improve mutation detection and predict chemotherapy response (e.g., declines in CA19-9 and RECIST responses in neoadjuvant settings). (roth2020recentadvancesin pages 5-6)

12. Recent statistics and data (quick-reference table)

Topic Finding (numeric) Population/Setting Source (first author, year, journal) URL Notes (e.g., biomarker subset)
surveillance Stage I 38.5% (10/26); Stage II 30.8% (8/26) vs matched SEER Stage I 10.3% (155/1504); Stage II 25.1% (377/1504) High-risk individuals under CAPS surveillance vs matched SEER PDAC controls Blackford, 2024, JAMA Oncology https://doi.org/10.1001/jamaoncol.2024.1930 Lower stage at diagnosis in surveillance cohort (blackford2024pancreaticcancersurveillance pages 1-2, blackford2024pancreaticcancersurveillance pages 5-6)
surveillance Distant metastasis at diagnosis 26.9% (7/26) vs 53.8% (809/1504) High-risk surveillance cohort vs matched SEER controls Blackford, 2024, JAMA Oncology https://doi.org/10.1001/jamaoncol.2024.1930 Fewer M1 cases with surveillance (blackford2024pancreaticcancersurveillance pages 5-6)
surveillance Median OS 61.7 months vs 8.0 months; 5-year OS 50% vs 9% High-risk surveillance cohort vs matched SEER controls Blackford, 2024, JAMA Oncology https://doi.org/10.1001/jamaoncol.2024.1930 Overall survival advantage with selective surveillance (blackford2024pancreaticcancersurveillance pages 1-2, blackford2024pancreaticcancersurveillance pages 5-6, blackford2024pancreaticcancersurveillance media 731b7f36)
surveillance 5-year PDAC-specific mortality 43% vs 86% High-risk surveillance cohort vs matched SEER controls Blackford, 2024, JAMA Oncology https://doi.org/10.1001/jamaoncol.2024.1930 Cancer-specific mortality lower in surveillance cohort (blackford2024pancreaticcancersurveillance pages 1-2, blackford2024pancreaticcancersurveillance pages 5-6, blackford2024pancreaticcancersurveillance media 731b7f36)
therapy MSI-H prevalence 0.8% (52/>6000 tested); ORR 77% (7/9); 78% alive at cutoff (7/9) PDAC patients with MSI-H detected by Guardant360 liquid biopsy; 9 treated with ICI Chakrabarti, 2022, Journal for ImmunoTherapy of Cancer https://doi.org/10.1136/jitc-2021-004485 Plasma-detected MSI-H subset; median PFS and OS not reached; metastatic disease in 80% of cohort (chakrabarti2022detectionofmicrosatellite pages 2-3)
therapy Median PFS 7.4 vs 3.8 months; HR 0.53 (95% CI 0.35-0.82); P=0.004 gBRCA-mutated metastatic pancreatic cancer without progression after ≥16 weeks first-line platinum Golan, 2019, New England Journal of Medicine https://doi.org/10.1056/NEJMoa1903387 POLO maintenance olaparib vs placebo (golan2019maintenanceolaparibfor pages 4-5)
therapy Interim median OS 18.9 vs 18.1 months; HR 0.91 (95% CI 0.56-1.46); P=.68 Same POLO randomized population at primary PFS data cutoff Kindler, 2022, Journal of Clinical Oncology https://doi.org/10.1200/JCO.21.01604 Final OS paper reporting prior interim OS analysis (kindler2022overallsurvivalresults pages 2-3)
risk factor Smoking RR 3.0 Pancreatic cancer risk factors review Netto, 2024, Current Oncology https://doi.org/10.3390/curroncol31090385 Most significant modifiable risk factor listed in review (netto2024systemictherapyfor pages 1-2)
risk factor Type 2 diabetes OR 2.39 Pancreatic cancer risk factors review Netto, 2024, Current Oncology https://doi.org/10.3390/curroncol31090385 Meta-analysis estimate cited in review (netto2024systemictherapyfor pages 1-2)
risk factor BMI >35 OR 1.62 Pancreatic cancer risk factors review Netto, 2024, Current Oncology https://doi.org/10.3390/curroncol31090385 Obesity-associated risk estimate (netto2024systemictherapyfor pages 1-2)
risk factor Family history RR 6.4 Two first-degree relatives with PDAC Netto, 2024, Current Oncology https://doi.org/10.3390/curroncol31090385 Familial pancreatic cancer risk estimate (netto2024systemictherapyfor pages 1-2)
risk factor Lynch syndrome RR 8.6 by age 70 Inherited susceptibility setting Netto, 2024, Current Oncology https://doi.org/10.3390/curroncol31090385 MMR-deficient hereditary risk estimate (netto2024systemictherapyfor pages 1-2)
epidemiology/prognosis 80% present with metastatic or unresectable disease PDAC overall presentation pattern Netto, 2024, Current Oncology https://doi.org/10.3390/curroncol31090385 Review framing advanced disease burden (netto2024systemictherapyfor pages 1-2)
epidemiology/prognosis 5-year survival rate ~10% PDAC overall Netto, 2024, Current Oncology https://doi.org/10.3390/curroncol31090385 Review summary statistic (netto2024systemictherapyfor pages 1-2)
epidemiology/prognosis Stage III 29% (6/21); Stage IV 71% (15/21); liver metastasis in 13/15 stage IV; median OS 9.7 months (range 0.6-47.8) Treatment-naive primary PDAC with and without paired liver metastasis samples Park, 2024, Molecular Cancer https://doi.org/10.1186/s12943-024-02003-0 Single-cell cohort informing metastatic evolution and TME (park2024singlecelltranscriptomeanalysis pages 1-2)
epidemiology/prognosis Basal-like malignant ductal cell proportion as low as 22% associated with poor survival; multivariable HR 24.9 (95% CI 2.02-310), P=0.012 Combined scRNA-seq cohorts / deconvoluted TCGA PDAC data Park, 2024, Molecular Cancer https://doi.org/10.1186/s12943-024-02003-0 Prognostic molecular subtype signal, relevant to metastatic behavior and chemotherapy response (park2024singlecelltranscriptomeanalysis pages 2-5)
epidemiology/prognosis 5-year survival below 10%; distant metastasis at initial diagnosis >80% PDAC with matched primary tumors and liver metastases Zhang, 2023, Nature Communications https://doi.org/10.1038/s41467-023-40727-7 Single-cell liver metastasis study describing metastatic burden (zhang2023singlecelltranscriptomic pages 1-2)
epidemiology/prognosis Incident pancreatic cancer cases projected in US 2024: 66,440; deaths: 51,750 United States, all pancreatic cancer Siegel, 2024, CA: A Cancer Journal for Clinicians https://doi.org/10.3322/caac.21820 Broader population context for burden; not metastatic-specific (siegel2024cancerstatistics2024 pages 12-12, siegel2024cancerstatistics2024 pages 30-31)
epidemiology/prognosis Pancreas incidence rising 0.6%-1.0% annually during 2015-2019 United States incidence trends Siegel, 2024, CA: A Cancer Journal for Clinicians https://doi.org/10.3322/caac.21820 Population trend relevant to rising PDAC burden (siegel2024cancerstatistics2024 pages 12-12)
mechanism/prognosis Prediction model accuracy 78% overall; 90% for early liver metastasis Pre-metastatic liver biopsies from localized pancreatic cancer patients Bojmar, 2024, Nature Medicine https://doi.org/10.1038/s41591-024-03075-7 Multi-omics pre-metastatic liver atlas; prognostic for metastatic outcome after surgery (bojmar2024multiparametricatlasof pages 1-2, bojmar2024multiparametricatlasof pages 7-9)
mechanism/prognosis Future liver metastasis within 3 years occurs in >40% after surgery Resected pancreatic cancer Bojmar, 2024, Nature Medicine https://doi.org/10.1038/s41591-024-03075-7 Background statistic motivating pre-metastatic niche profiling (bojmar2024multiparametricatlasof pages 1-2)

Table: This table compiles high-yield numeric findings relevant to metastatic pancreatic ductal adenocarcinoma, including prognosis, surveillance outcomes, biomarker-defined therapy subsets, and major risk-effect sizes. It is designed as a citation-ready reference for rapid evidence extraction.

Included visual evidence

Figure/Table region showing the Kaplan–Meier OS comparison and 5-year OS for high-risk surveillance vs SEER controls is available from the JAMA Oncology 2024 cohort study. (blackford2024pancreaticcancersurveillance media 731b7f36, blackford2024pancreaticcancersurveillance media 8143d526)

Key abstract-supported quotations (verbatim)

  • Single-cell liver metastasis microenvironment: “RGS5+ cancer-associated fibroblasts, CCL18+ lipid-associated macrophages, S100A8+ neutrophils and FOXP3+ regulatory T cells.” (zhang2023singlecelltranscriptomic pages 1-2)
  • Plasma MSI-H predicts immunotherapy response: “The overall response rate by Response Evaluation Criteria in Solid Tumors was 77% (7/9).” (chakrabarti2022detectionofmicrosatellite pages 2-3)
  • Pre-metastatic liver atlas concept: “Multi-parametric analysis of pre-metastatic liver biopsies” to classify metastatic risk/timing/site. (bojmar2024multiparametricatlasof pages 1-2)

Evidence gaps / items to complete for knowledge base curation

1) Authoritative ontology IDs (MONDO, MeSH, ICD-11) for metastatic pancreatic ductal adenocarcinoma were not retrieved in this run and should be added from ontology databases. 2) NALIRIFOX pivotal trial (NAPOLI-3) primary publication numeric endpoints (OS/PFS hazard ratios, medians, AE rates) were not captured in the retrieved full text. 3) Phenotype frequency (HPO) and detailed diagnostic performance metrics (e.g., CA19-9 sensitivity/specificity; ctDNA sensitivity) require targeted retrieval. 4) Comparative biology/other species and more standardized MAXO mappings require additional sourcing.

References

  1. (dalessandro2024newapproachesto pages 6-10): Franco Nicolás D'Alessandro. New approaches to understand the role of potassium channels and their interaction with tumor microenvironment (tme) for innovative targeted therapy. Other, Dec 2024. URL: https://doi.org/10.25434/d-alessandro-franco-nicol-s_phd2024-12-20, doi:10.25434/d-alessandro-franco-nicol-s_phd2024-12-20. This article has 0 citations.

  2. (park2024singlecelltranscriptomeanalysis pages 1-2): Joo Kyung Park, Hyoung-oh Jeong, Hyemin Kim, Jin Ho Choi, Eun Mi Lee, Seunghoon Kim, Jinho Jang, David Whee-Young Choi, Se-Hoon Lee, Kyoung Mee Kim, Kee-Taek Jang, Kwang Hyuck Lee, Kyu Taek Lee, Min Woo Lee, Jong Kyun Lee, and Semin Lee. Single-cell transcriptome analysis reveals subtype-specific clonal evolution and microenvironmental changes in liver metastasis of pancreatic adenocarcinoma and their clinical implications. Molecular Cancer, May 2024. URL: https://doi.org/10.1186/s12943-024-02003-0, doi:10.1186/s12943-024-02003-0. This article has 36 citations and is from a highest quality peer-reviewed journal.

  3. (zhang2023singlecelltranscriptomic pages 1-2): Shu Zhang, Wen Fang, Siqi Zhou, Dongming Zhu, Ruidong Chen, Xin Gao, Zhuojin Li, Yao Fu, Yixuan Zhang, Fa Yang, Jing Zhao, Hao Wu, Pin Wang, Yonghua Shen, Shanshan Shen, Guifang Xu, Lei Wang, Chao Yan, Xiaoping Zou, Dijun Chen, and Ying Lv. Single cell transcriptomic analyses implicate an immunosuppressive tumor microenvironment in pancreatic cancer liver metastasis. Nature Communications, Aug 2023. URL: https://doi.org/10.1038/s41467-023-40727-7, doi:10.1038/s41467-023-40727-7. This article has 194 citations and is from a highest quality peer-reviewed journal.

  4. (siegel2024cancerstatistics2024 pages 12-12): Rebecca L. Siegel, Angela N. Giaquinto, and Ahmedin Jemal. Cancer statistics, 2024. CA: A Cancer Journal for Clinicians, 74:12-49, Jan 2024. URL: https://doi.org/10.3322/caac.21820, doi:10.3322/caac.21820. This article has 12709 citations and is from a domain leading peer-reviewed journal.

  5. (netto2024systemictherapyfor pages 1-2): Daniel Netto, Melissa Frizziero, Victoria Foy, Mairéad G. McNamara, Alison Backen, and Richard A. Hubner. Systemic therapy for metastatic pancreatic cancer—current landscape and future directions. Current Oncology, 31:5206-5223, Sep 2024. URL: https://doi.org/10.3390/curroncol31090385, doi:10.3390/curroncol31090385. This article has 6 citations.

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