Tissue-resident Memory T Cells Across Aging Niches

OPEN

Resolve how aged tissue niches differentially preserve or erode TRM function across barrier organs and CNS-adjacent sites. Boundary domains: tissue-immunity, neuroinflammation. Representative papers: The role of the CD8+ T cell compartment in ageing and neurodegenerative disorders.; From Tissue to Transcriptome: A Systematic Review of Multi-Level Evidence for Immune Dysregulation in Atrial Fibrillation.; Visual Genomics Analysis Studio as a Tool to Analyze Multiomic Data.

Priority: 0.67 Domain: immunology-aging-memory Hypotheses: 0
📊 Landscape Analysis

Landscape Summary: Tissue-resident Memory T Cells Across Aging Niches is a 0.667 priority gap in immunology-aging-memory. It has 0 linked hypotheses with average composite score 0.000. Status: open.

Key Unanswered Questions

Key Researchers

Colonna, Sevlever, et al. (TREM2 biology)

Clinical Trials

Tissue-resident Memory T Cells Across Aging Niches — INVOKE-2 (completed)

📈 Living Dashboards
0
Hypotheses
0.000
Top Score
0.000
Avg Score
0
Debates
0.00
Avg Quality
0%
Resolution
0
Mechanistic Families
Gap Resolution Progress0%

Hypothesis Score Distribution

🏆 Competing Hypotheses (Ranked by Score)

No hypotheses linked to this gap yet.

🌊 Knowledge Graph Connections

activates (24)

BAXAgingGALAgingP53AgingAgingMtorAKTAging
▸ Show 19 more

associated with (2)

StrokeAgingInflammationAging

expressed in (1)

GENESAging

inhibits (2)

DNAAgingAgingAutophagy

regulates (6)

AgingMitophagyAgingEpigeneticAgingImmune ResponseDNAAgingGENESAging
▸ Show 1 more

therapeutic target (15)

NRF2AgingAgingMitochondrial FunctionTP53AgingGENESAgingAMPKAging
▸ Show 10 more
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