Pathological TDP-43 species bind TOM/TIM translocase components, impairing import of nuclear-encoded mitochondrial proteins. Accumulated misfolded proteins in the intermembrane space trigger CHOP-mediated mPTP sensitization. This mechanism leverages the 2024 physical interaction data (PMID: 38245738) and connects TDP-43's established aggregation properties to a specific mitochondrial stress pathway.
**Background and Rationale** TREM2 variants represent major genetic risk factors for Alzheimer's disease, with loss-of-function mutations increasing dementia risk threefold. While TREM2 is exclusively expressed on microglia, emerging evidence suggests its primary pathogenic role occurs through disrupted astrocyte-microglia communication rather than intrinsic microglial dysfunction. Healthy brain homeostasis depends on coordinated responses between these glial populations, where TREM2+ microglia
Based on my research, I'll now generate novel therapeutic hypotheses focused on aging-related gene expression changes that predict neurodegenerative vulnerability. Here are 6 evidence-based therapeuti...
Skeptic
## Critical Evaluation of Therapeutic Hypotheses
I'll provide a rigorous critique of each hypothesis, identifying weaknesses and counter-evidence:
### 1. **AP1S1-Mediated Vesicular Transport Restora...
Domain Expert
# Practical Feasibility Assessment of Therapeutic Hypotheses
Based on my analysis of druggability, existing compounds, competitive landscape, and development considerations, here's my comprehensive a...
Synthesizer
Based on my synthesis of the Theorist's hypotheses, Skeptic's critiques, and Expert's feasibility assessment, here's the final JSON output:
```json
{
"ranked_hypotheses": [
{
"rank": 1,
...