Our methodology

• •Multiple peer-reviewed RCTs or large prospective cohort studies
• •Independent replication across different populations and labs
• •Consistent effect direction and meaningful effect size
• •Open methods allowing reproduction
• •Demonstrated incremental value beyond standard risk factors

Examples: Classic epigenetic clocks (Horvath, Hannum) for age prediction. Exercise and diet for epigenetic age deceleration.

• •Some RCTs or strong observational data
• •At least one independent replication or large-cohort validation
• •Plausible biological mechanism supported by data
• •Published methodology but may lack full independent reproduction
• •Vendor validation may be strong but independent confirmation is limited

Examples: GrimAge and DunedinPACE for mortality prediction. GlycanAge for inflammation tracking. Metformin for aging (pending TAME trial).

• •Animal studies, pilot human studies, or early-phase trials
• •Mechanistic plausibility but limited clinical data
• •No independent replication in humans yet
• •May be based on small sample sizes or vendor-only datasets
• •Exciting science but translation to clinical utility unproven

Examples: Partial cellular reprogramming. NAD+ precursors for biological age. Microbiome-based age clocks.

• •Vendor-only claims without published validation
• •No peer-reviewed studies or only vendor-funded studies without independent oversight
• •Marketing language exceeds published evidence
• •Proprietary models without methodological transparency
• •No independent replication or external validation

Examples: Products claiming age reversal without test-retest reliability data. Clocks comparing across different tissue types without calibration.