Geniposide for Alzheimer's disease - immune biomarker targeting and therapeutic potential

Dimension	Score	Rationale
Mechanistic Clarity	7/10	Multi-target via immune biomarker modulation; AMPK/NF-κB pathway involvement well-characterized
Clinical Evidence	2/10	No clinical trials yet; computational prediction only; pre-clinical stage
Preclinical Evidence	7/10	Consistent neuroprotection in APP/PS1, MPTP models; multiple pathway activations demonstrated
Replication	4/10	Moderate replication across independent labs; limited species diversity in studies
Effect Size	3/10	Moderate pre-clinical effects; doses used (50-100 mg/kg) may not translate to human equivalents
Safety/Tolerability	8/10	Gardenia fruit has dietary use; geniposide shows low toxicity in acute studies
Biological Plausibility	6/10	Computational binding to GFAP, VGF, NPY, CCK, NFKBIA validated; pathway evidence supports mechanism
Actionability	3/10	Research compound; no standardized supplement; purification required from Gardenia source

Compound	Primary Target	Mechanism	Evidence Level
Curcumin	Aβ aggregation, NF-κB	Multi-target anti-inflammatory	Clinical trials
Geniposide	GFAP, VGF, NPY, CCK, NFKBIA	Immune biomarker modulation	Pre-clinical + computational
Resveratrol	Sirt1, AMPK	Anti-oxidant, anti-inflammatory	Clinical trials
Sulforaphane	Nrf2	Antioxidant response	Pre-clinical

Factor	Curcumin	Geniposide
Source	Turmeric (Curcuma longa)	Gardenia (Gardenia jasminoides)
Class	Polyphenol	Iridoid glycoside
Primary targets	Aβ, tau, NF-κB	GFAP, VGF, NPY, CCK, NFKBIA
Bioavailability	Poor (<1%)	Unknown
Clinical evidence	Multiple RCTs	None
Evidence level	40/80	45/80

¶ Geniposide for Alzheimer's Disease