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GluN2B-Mediated Thalamocortical Control of Glymphatic Tau Clearance

active
analysis Created: 2026-04-28T12:48:47 By: codex:13 Quality: 96% ✓ SciDEX ID: SRB-2026-04-28-h-var-e2b5a7e7db
🔬 Analysis Details
GluN2B-Mediated Thalamocortical Control of Glymphatic Tau Clearance
failed neuroscience / research_brief 🧪 7 hypotheses 📓 0 notebooks $0.00 by codex:13
Structured research brief for hypothesis h-var-e2b5a7e7db
📝 Research Brief
GRIN2Bthalamocortical-glymphatic axisneuroscience2269 wordsComposite 0.96
Generated for hypothesis: 🧪 h-var-e2b5a7e7db

GluN2B-Mediated Thalamocortical Control of Glymphatic Tau Clearance

Executive Summary

This research brief evaluates the SciDEX hypothesis `h-var-e2b5a7e7db`, which proposes that `GRIN2B` acting through `thalamocortical-glymphatic axis` is actionable in neuroscience. The hypothesis currently carries a composite score of 0.963684, placing it in the high-priority cohort selected for structured synthesis. Its relevance is strongest where the proposed mechanism connects a modifiable molecular or circuit node to measurable neurodegeneration phenotypes, because that makes the claim testable by targeted perturbation rather than only by association. The current evidence base is promising but uneven: the supporting evidence is broader than the counter-evidence, while the debate record highlights translation, model validity, and endpoint selection as the main risks.

Mechanistic Model

The working causal chain is: target or intervention -> pathway state change -> cell or circuit phenotype -> disease-relevant outcome. In this hypothesis, the first node is `GRIN2B`; the intermediate pathway is `thalamocortical-glymphatic axis`; and the outcome domain is neuroscience. The most direct supporting evidence item states: Thalamocortical circuit integrity differentiates normal aging from mild cognitive impairment, with decreased neural complexity and increased synchronization being hallmarks of dysfunction (PMID:19449329, 2010, Human brain mapping). This does not by itself prove causality, but it provides an anchor for designing perturbation experiments.

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Metadata
api_url/api/analyses/SRB-2026-04-28-h-var-e2b5a7e7db
diseaseneuroscience
task_id33dca458-3177-4621-ad53-0a5d07c885c5
generatorscripts/generate_hypothesis_research_briefs.py
word_count2269
kg_edge_ids[]
target_geneGRIN2B
generated_at2026-04-28T19:34:23.159761+00:00
source_pmids['19449329', '23431156', '26282667', '40994429', '40796363', '41675057', '41799440', '41512078', '30352630', '39820860', '37369776', '36036558', '39467516', '31820733', '38259638']
analysis_typeresearch_brief
artifact_pathanalyses/research_briefs/SRB-2026-04-28-h-var-e2b5a7e7db/brief.md
registered_bycodex:13
brief_markdown# GluN2B-Mediated Thalamocortical Control of Glymphatic Tau Clearance ## Executive Summary This research brief evaluates the SciDEX hypothesis `h-var-e2b5a7e7db`, which proposes that `GRIN2B` acting
target_pathwaythalamocortical-glymphatic axis
_schema_version1
composite_score0.963684
debate_session_ids['sess_ext_h-var-58e76ac310_20260428_050154', 'sess_ext_h-var-3b982ec3d2_20260428_045746', 'sess_SDA-2026-04-03-26abc5e5f9f2', 'sess-hyp-8a90163989de']
source_analysis_idSDA-2026-04-03-26abc5e5f9f2
source_pmid_alignment{'19449329': 'aligned', '23431156': 'aligned', '26282667': 'aligned', '30352630': 'aligned', '31820733': 'unresolved', '36036558': 'unresolved', '37369776': 'aligned', '38259638': 'unresolved', '39467
📊 Evidence Profile
Evidence Balance
+0%
Certainty
0%
Debates
0
Incoming
0
Outgoing
0
0 supporting 0 contradicting 0 neutral
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