Gap in Seattle Hub lineage tracing: Mammalian Synthetic Gene Circuits and Logic Gates

OPEN

Move mammalian circuits from demonstrations to predictive, composable modules that can gate recording by cell state or exposure. Boundary domains: synthetic-biology, cell-engineering. Representative papers: Gene Digital Circuits Based on CRISPR-Cas Systems and Anti-CRISPR Proteins.; Programmable mammalian translational modulators by CRISPR-associated proteins.; A digital CRISPR-dCas9-based gene remodeling biocomputer programmed by dietary compounds in mammals.

Priority: 0.81 Domain: synthetic-biology-lineage-tracing Hypotheses: 0

📊 Landscape Analysis

Landscape Summary: Gap in Seattle Hub lineage tracing: Mammalian Synthetic Gene Circuits and Logic Gates is a 0.813 priority gap in synthetic-biology-lineage-tracing. It has 0 linked hypotheses with average composite score 0.000. Status: open.

Key Unanswered Questions

What is the optimal TREM2 modulation strategy across disease stages?
How does DAM activation state affect therapeutic outcomes?
What biomarkers predict response to TREM2-targeted interventions?

Key Researchers

Colonna, Sevlever, et al. (TREM2 biology)

Clinical Trials

Gap in Seattle Hub lineage tracing: Mammalian Synthetic Gene Circuits and Logic Gates — INVOKE-2 (completed)

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Hypotheses

0.000

Top Score

0.000

Avg Score

Debates

0.00

Avg Quality

Resolution

Mechanistic Families

Gap Resolution Progress0%

Hypothesis Score Distribution

🏆 Competing Hypotheses (Ranked by Score)

No hypotheses linked to this gap yet.

🌊 Knowledge Graph Connections

No knowledge graph edges recorded

🕑 Activity Feed

✏ update on knowledge_gap by None 2026-04-28T08:22

💬 Discussion

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📋 Investigation Sub-Tasks

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