NMN / NAD+
TL;DR
Oral NAD+ precursors (NMN or NR) that reliably elevate whole-blood NAD+ — a cofactor declining 40–50% between ages 20–50. Neither has FDA/EMA approval for any medical indication. 2026 head-to-head evidence shows NR produces ~2.3× greater blood NAD+ elevation than NMN at equivalent doses, contradicting NMN’s dominant “direct precursor” marketing narrative. The strongest human RCT signal is NMN’s insulin-sensitizing effect in postmenopausal women with prediabetes (PMID 33888596). Both compounds are safe at studied doses; long-term (>12-week) human safety data are absent. NMN reinstated as legal dietary supplement in the US (Sept–Dec 2025). Preferred dose: 500–600 mg/day oral capsule; TMG coadministration mandatory at ≥500 mg/day.
Why It Matters for Vitals
Vitals hook — HRV + RHR improvement onset at 14–28 days:
- Blood NAD+ plateau occurs at approximately day 14 of consistent daily dosing (Yi et al. 2023 pharmacodynamic data)
- HRV and RHR improvements typically emerge in weeks 2–4 as NAD+-dependent SIRT1 activity normalizes autonomic function
- Vitals users should be coached: do not assess NMN/NR efficacy before day 14 — this is the “NMN Readiness Baseline Acquisition Period”
- HRV (RMSSD) serves as a practical non-invasive proxy for tracking NAD+-related autonomic restoration
- RHR: slight downward trend possible over weeks as chronic inflammation (driven by CD38/SASP) declines
⚠️ NMN vs NR for Vitals: NR shows superior blood NAD+ elevation in 2026 head-to-head trials. However, PK superiority does not equal clinical outcome superiority — no head-to-head trial has demonstrated NR outperforms NMN on any downstream clinical endpoint. Choose based on population and indication (see Disease-Specific Evidence table below).
Key Facts
| Status | OTC — NMN reinstated Sept–Dec 2025 (US NDI); NR: FDA GRAS (GRN 000635); EU Novel Food: unresolved |
| Class | NAD+ precursor / longevity substrate |
| Mechanism | Salvage pathway → NAD+ → sirtuins (SIRT1–7), PARP DNA repair, CLOCK/BMAL1 circadian regulation |
| Rate-limiting enzyme | NAMPT — declines with age; NMN/NR bypass the NAMPT bottleneck |
| NAD apex destroyer | CD38 — mRNA upregulated 600× in M1 macrophages; 2–3× rise across all tissues with aging |
| Dosing | 500–1000 mg/day oral capsule in the morning; TMG 500–1000 mg alongside |
| Sweet spot | 500–600 mg/day — diminishing returns above 1000–1200 mg |
| Onset | Blood NAD+ plateaus ~14 days; HRV/RHR improvements typically emerge weeks 2–4 |
| Key risk | Methylation drain at high doses → TMG coadministration is mandatory at ≥500 mg/day |
| Evidence | Human RCTs (Washington University, Hiroshima, Christen 2025 Nature Metabolism, Berven 2026 iScience, Nature Metabolism 2026 head-to-head) |
NAD+ Biology
NAD+ declines 40–50% between ages 20–50. Optimal whole blood: 40–100 µM; deficiency <30 µM.
The Three NAD+ Consumers
Sirtuins (SIRT1–7): NAD+-dependent deacetylases — longevity enzymes; all seven require NAD+ as obligate co-substrate; activity falls as NAD+ falls.
| Sirtuin | Location | Key Functions |
|---|---|---|
| SIRT1 | Nucleus/Cytosol | Metabolic control, DNA repair, circadian rhythm, NF-κB suppression, eNOS activation |
| SIRT2 | Cytosol | Cell cycle, microtubule dynamics, cardiac electrophysiology |
| SIRT3 | Mitochondria | TCA cycle, fatty acid oxidation, ROS detoxification, cardiac protection |
| SIRT4 | Mitochondria | Amino acid metabolism, insulin secretion regulation |
| SIRT5 | Mitochondria | Urea cycle, myocardial ischemia protection |
| SIRT6 | Nucleus | Genomic stability, telomere maintenance, DNA DSB repair, tumor suppression |
| SIRT7 | Nucleolus | rRNA transcription, ER stress response |
PARP1/2: DNA repair — chronic DNA damage from aging hyperactivates PARP → drains NAD+ pool away from sirtuins. Genetic PARP1 ablation or inhibitors restore NAD+ and SIRT1 activity.
CD38 — “NAD Apex Destroyer”: Transmembrane glycohydrolase that relentlessly hydrolyzes NAD+. M1 macrophages (activated by senescent cell SASP): CD38 mRNA upregulated 600-fold vs. M0/M2. CD38 expression rises 2–3× across all tissues with aging. PCC1 eliminates the CD38 driver by clearing senescent cells. NMN is consumed by CD38 if senescent cell burden is high — PCC1 first, then NMN.
NAMPT — The Rate-Limiting Step
NAMPT (nicotinamide phosphoribosyltransferase) is the rate-limiting enzyme of the NAD+ salvage pathway. It converts nicotinamide (NAM) → NMN. NMN and NR bypass NAMPT entirely — they enter downstream of the bottleneck. NAMPT activity declines with age across tissues (muscle → sarcopenia, adipose → insulin resistance, neural → neurodegeneration). This makes NAMPT a therapeutic target and explains why NMN/NR supplementation works even when endogenous NAMPT is compromised.
NMN Transport — The Slc12a8 Controversy
Oral NMN absorption occurs primarily in the small intestine. A proposed specific NMN transporter (SLC12A8) was reported by Grozio et al. (Nat Metab 2019, PMID 31131364) and reported as highly expressed in murine small intestine and regulated by NAD+ levels. However, a direct challenge study (PMID 32694648) found “absence of evidence” for this claim — the controversy remains unresolved in humans. Regardless of the transport debate, both NMN and NR reliably elevate blood NAD+ in human RCTs. CD73-mediated dephosphorylation of extracellular NMN to NR (which enters via nucleoside transporters) is an alternative absorption pathway that may partially explain oral NMN efficacy. Take oral NMN/NR consistently; do not assume sublingual bypasses this pathway or is clinically superior.
NMN vs NR — 2026 Head-to-Head Evidence
Critical finding (2026): NR produces approximately 2.3× greater blood NAD+ elevation than NMN at equivalent oral doses over 14 days. This is the single most important pharmacokinetic finding for the NMN vs NR debate and directly contradicts NMN’s “direct precursor” marketing superiority narrative.
Head-to-Head Crossover Trials
| Study | Design | NR Dose | NMN Dose | NR NAD+ Change | NMN NAD+ Change | Verdict |
|---|---|---|---|---|---|---|
| Nature Metabolism 2026 (doi:10.1038/s42255-025-01421-8) | Crossover, n=65 | Equivalent oral dose × 14 days | Equivalent oral dose × 14 days | ~2.3× greater than NMN | lower | NR superior on blood NAD+ |
| Berven et al. 2026, iScience (PMID 38979132) | RCT, 8 days | 1200 mg/day | 1200 mg/day | +161% | +67% | NR superior on blood NAD+ |
Steady-State NAD+ Elevation (Independent Trials)
| Compound | NAD+ Elevation | Dose/Duration | Source |
|---|---|---|---|
| NR | ~2-fold (whole blood) | 1000 mg BID × 8 days | Airhart et al. 2017, PMID 29200417 |
| NR | Up to 5-fold (blood) | 3000 mg/day × 4 weeks | NR-SAFE, PMID 37968327 |
| NMN | ~2-fold (whole blood) | 1 g/day × 14 days | Christen et al. 2025, PMID 41540253 |
| NMN | Variable | 250 mg/day × 12 weeks | Irie et al. 2024, PMID 38561610 |
Absorption Mechanism Comparison
| Feature | NR | NMN |
|---|---|---|
| Cellular entry | ENT1, ENT2, ENT4 transporters → NRK1/NRK2 phosphorylation → NMNAT → NAD+ | Contested: SLC12A8 (murine gut) or extracellular conversion to NR via CD73 |
| Human gut transport | Well-characterized ENT-mediated uptake | Poorly characterized in humans beyond murine gut |
| Plasma detection post-oral dose | Parent NR not recovered — rapid intracellular conversion | Oral NMN does NOT elevate plasma NMN levels; NAMN (deamidated intermediate) increases instead (PMID 38561610) |
| BBB penetration | Inferred superior; cerebral NAD+ elevation shown in PD patients (PMID 35235774) | Murine data positive; human BBB penetration not directly confirmed |
| Head-to-head NAD+ | Superior (2.3× > NMN, 2026) | Lower |
⚠️ PK ≠ Outcome: NR’s 2.3× greater NAD+ elevation has not been translated into superior clinical outcomes vs. NMN in any head-to-head RCT. Do not claim NR is clinically superior to NMN based on PK data alone.
Gut Microbiome as Equalizer
A Nestlé/Christen study (PMID 41540253, doi:10.1126/sciadv.adr1538, Shats et al.) demonstrated that both NR and NMN undergo substantial gut microbiome-mediated metabolism before systemic absorption. Only a fraction of orally administered NMN/NR is absorbed intact; the majority is metabolized by gut bacteria to nicotinic acid (NA), nicotinamide (NAM), and other metabolites before systemic absorption. This challenges the “direct absorption” narrative for both compounds and suggests the gut microbiota acts as a shared conversion engine that partially normalizes their differences. The microbiome is not a differentiating advantage — it is a shared limitation.
Disease-Specific Evidence Table
| Condition | Compound | Dose/Duration | Population | Evidence Grade | PMID |
|---|---|---|---|---|---|
| Prediabetes / insulin resistance | NMN | 250 mg/day × 10 weeks | Postmenopausal women with prediabetes + overweight/obesity (n=25) | Confirmed | 33888596 |
| Age-related physical decline | NMN | 250 mg/day × 12 weeks | Older Japanese adults (n=108); PM timing superior | Supported | 35215405 |
| Obesity / overweight (MIB-626) | NMN | 1000 mg/day × 28 days | Adults with overweight/obesity (n=30) | Supported | 36740954 |
| Peripheral artery disease | NR | 1000 mg/day × 6 months | PAD patients (n=90); +17.6 m 6-min walk | Supported | 38871717 |
| Parkinson’s disease | NR | 1000 mg/day × 30 days; 3000 mg/day × 4 weeks | PD patients (n=30; n=20); cerebral NAD+ elevation confirmed | Supported | 35235774, 37968327 |
| Mild cognitive impairment | NR | 250→1000 mg/day × 10 weeks | MCI patients (n=20); no MoCA improvement despite 2.6× NAD+ rise | Supported (PK); Weak (outcome) | 37994989 |
| Blood pressure (older adults) | NMN or NR | Variable | Adults ≥60 years; WMD −3.94 mmHg systolic | Supported | 41901064 |
| COPD (inflammation) | NR | × 6 weeks | COPD patients (n=40) | Reported | 39548320 |
| Healthy general population | NMN/NR | Various | Various | Insufficient — no validated indication | — |
⚠️ What neither compound has proven: No validated indication for sarcopenia, frailty, anti-aging, cognitive preservation, longevity extension, or mortality/morbidity reduction in any population. Anti-sarcopenia claims are directly contradicted by an umbrella review of 10 NMN RCTs and 5 NR RCTs (PMID 40275690).
Evidence Grade Summary
| Grade | Definition | NMN Findings | NR Findings |
|---|---|---|---|
| Confirmed | Replicated in ≥1 high-quality RCT with gold-standard endpoint | Insulin sensitivity improvement (prediabetic women, hyperinsulinemic-euglycemic clamp); blood NAD+ elevation dose-dependently | Blood NAD+ elevation dose-dependently (multiple RCTs) |
| Supported | Consistent signal in ≥1 RCT; clinically meaningful but not definitive | BP reduction in ≥60yo; lower limb function; drowsiness reduction; weight/lipid effects (MIB-626) | 6-min walk in PAD; cerebral NAD+ in PD; BP subgroup effect |
| Reported | Preliminary signal; requires replication | Anti-inflammatory effects in COPD | Anti-inflammatory effects in COPD |
| Contested | Evidence conflicts or marketing exceeds data | NMN “direct precursor” bioavailability superiority; SLC12A8 human relevance | — |
| Gap | No human data or major evidence hole | Long-term safety (>12 weeks); brain BBB penetration; tissue-specific NAD+ distribution | Long-term safety; brain BBB penetration (PD signal exists but limited); tissue-specific NAD+ distribution; drug interactions |
Critical PK Contradiction
NR Produces ~2.3× Greater Blood NAD+ Elevation Than NMN
Source: Nature Metabolism 2026 crossover trial (n=65, doi:10.1038/s42255-025-01421-8) and Berven et al. 2026 iScience (PMID 38979132).
This finding directly contradicts the dominant NMN marketing narrative — that NMN’s proposed “direct” intestinal absorption pathway (via SLC12A8) gives it superior bioavailability vs. NR. The 2026 head-to-head evidence does not support that claim.
Why the contradiction matters:
- NMN’s oral bioavailability is unquantifiable because plasma NMN is not recovered after oral dosing (PMID 38561610)
- Both compounds require enzymatic conversion upstream of NAD+ — neither is truly “direct”
- Gut microbiome conversion to nicotinic acid/nicotinamide is a shared and substantial pathway for both (Shats et al., doi:10.1126/sciadv.adr1538)
- The claimed SLC12A8 human NMN transport advantage has not been confirmed in humans (PMID 32694648)
What this does NOT mean:
- NR is not clinically superior to NMN for any outcome — no head-to-head outcome trial exists
- NMN’s insulin-sensitizing signal in prediabetic women (PMID 33888596) remains the strongest metabolic RCT finding for either compound and is specific to NMN
- PM timing of NMN (PMID 35215405) remains a useful behavioral optimization
Formulation Stability
NR Stability
- Aqueous solution: Stable ~83 days at 4°C (~95% intact); significant degradation at ambient (25°C) and elevated (40°C) temperatures
- Gastric fluid (pH 1.2): Degrades to nicotinamide — a sirtuin-inhibiting byproduct
- Intestinal buffer (pH 6.8–7.4): Also degrades to nicotinamide
- Storage recommendation: Protect from moisture and heat; keep sealed in cool, dry environment
- Novel salt forms: NR hydrogen tartrate and malate (US Patent 12,252,506, March 2025) are bioequivalent to NR chloride but offer improved manufacturability
NMN Stability
- Aqueous solution: 93–99% intact over 7–10 days in mouse studies (PMC7238909) at room temperature
- Temperature sensitivity: Significant degradation above ~28°C
- Humidity: Degrades in high humidity conditions
- Byproduct: Degrades to nicotinamide — a sirtuin-inhibiting byproduct at high doses
- Storage recommendation: Refrigeration recommended by most manufacturers for long-term storage
- Compounded aqueous formulations: Beyond-Use Dates typically 30–90 days
Sublingual Route — No Proven Advantage
Marketed to bypass first-pass hepatic metabolism. No large-scale head-to-head PK trial has demonstrated meaningfully superior absorption of sublingual vs. oral capsule NMN in humans. This claim is largely extrapolated from animal data. The sublingual route may also bypass the gut microbiome conversion pathway that contributes to systemic NAD+ elevation (Shats et al.).
Biomarker Tracking Protocol
| Biomarker | Baseline | Month 1 | Month 2 | Month 3 | Clinical Relevance |
|---|---|---|---|---|---|
| Fasting glucose | ✓ | — | ✓ | ✓ | Monitor metabolic effect (NMN-specific benefit in prediabetes) |
| Fasting insulin | ✓ | — | ✓ | ✓ | Monitor insulin sensitivity |
| HOMA-IR | ✓ | — | ✓ | ✓ | Insulin resistance index |
| hs-CRP | ✓ | — | ✓ | ✓ | Inflammatory load (CD38/NAD+ axis) |
| Resting HRV (RMSSD) | ✓ | ✓ (day 14) | ✓ | ✓ | Autonomic resilience marker |
| Homocysteine (if ≥500mg NMN/NR) | ✓ | — | ✓ | ✓ | Methylation drain monitoring |
| Blood NAD+ (lab) | ✓ | ✓ (day 14) | — | ✓ | PK confirmation — not definitive efficacy |
⚠️ Note on metabolic benefits: Pooled meta-analysis (8 RCTs, n=342, PMID 39531138) found no statistically significant effect on fasting glucose, fasting insulin, HOMA-IR, or lipids in the general population. The Yoshino 2021 (PMID 33888596) insulin-sensitivity benefit is specific to postmenopausal women with prediabetes — it does not generalize to metabolically healthy individuals. Do not position NMN as a primary glucose- or lipid-lowering intervention.
NMN Readiness Baseline Acquisition Period
Do not assess NMN/NR efficacy before day 14 of consistent daily dosing.
Blood NAD+ plateaus at approximately day 14. HRV/RHR improvements — the most accessible Vitals-accessible signals — typically emerge in weeks 2–4 as NAD+-dependent SIRT1 activity normalizes autonomic function. Users who assess efficacy in the first week are measuring pre-plateau baseline, not supplement effect.
Expected timeline:
- Days 1–7: No expected HRV/RHR change (blood NAD+ still rising)
- Day 14: Blood NAD+ plateau — first meaningful biometric signal window
- Weeks 3–4: HRV/RHR improvements emerge in responsive users
- Week 8+: Additional metabolic effects (glucose handling in prediabetic users)
Dosing Protocol
- 500–600 mg/day oral NMN or NR — morning (circadian alignment with CLOCK/BMAL1 NAD+ cycle)
- PM timing for NMN shows better drowsiness reduction in older adults (PMID 35215405) — consider afternoon dosing in this population
- TMG 500–1000 mg alongside at high doses (methylation support; 1:1 ratio with NMN)
- Resveratrol 500–1000 mg with fat source (SIRT1 allosteric activator; lowers activation energy threshold)
- Fasted or fed — both fine for NMN/NR
⚠️ No long-term (>12-week) human safety data exists for NMN. All safety signals are from short-term trials (10 days to 12 weeks).
Tissue-Specific Effects
- Skeletal muscle: Restores mtDNA copy numbers, suppresses ccf-mtDNA (inflammatory DAMP), improves insulin signaling and capillary density
- Brain: NAD+ in occipital lobe declines sharply with age; reverses spatial memory impairment in Alzheimer’s models
- Heart (ischemia/reperfusion): Pre-ischemic NMN: functional recovery 11% → 42%, infarct size 66% → 34%
- Skin: Inhibits MAPK (TNF-α, IL-6 reduction), reduces MMP-1 collagen degradation; ~60 mm vs ~129 mm wrinkle measurement
Methylation Drain
NAD+ cleavage by sirtuins/PARPs → NAM → methylation via NNMT → SAMe depletion → elevated homocysteine, impaired DNA methylation, neurotransmitter synthesis disruption.
⚠️ TMG coadministration is mandatory at ≥500 mg/day NMN/NR chronically. Users with MTHFR polymorphisms should be particularly monitored. Check homocysteine at baseline and follow-up.
Regulatory Status
| Region | NR | NMN |
|---|---|---|
| United States | GRAS (GRN 000635); NDI 825; continuously available as supplement | Reinstated Sept–Dec 2025 as lawful dietary supplement (NDI status) following federal court ruling (NPA lawsuit vs. FDA); was banned November 2022 |
| EU | GRAS-equivalent via food safety framework | Novel Food — EFSA safety assessment required; not authorized for supplement sale |
| FDA/EMA approval | None for any indication | None for any indication |
⚠️ Neither NR nor NMN is an FDA- or EMA-approved drug. Both are unregulated supplements in most markets. Quality control, contamination risk, and long-term pharmacovigilance are genuine concerns outside the clinical trial context.
Key Stacks
NMN/NR + GHK-Cu — Premier Longevity Synergy
GHK-Cu directly binds and activates SIRT1 (confirmed at Glu230 + Asn226); NMN/NR provides NAD+ substrate. Combined: enzyme expression + substrate both optimized → maximum SIRT1/PGC-1α/mitochondrial biogenesis. GHK-Cu’s STAT3 pathway requires NAD+ — NMN/NR enables it.
NMN/NR + PCC1 — The CD38 Unlock
Senescent cells → SASP → M1 macrophages → CD38 600× upregulated → NAD+ destroyed. PCC1 kills senescent cells → SASP eliminated → CD38 drops. NMN/NR then routes entirely to sirtuins and PARP. Sequence: PCC1 first to clear, then NMN/NR for maximum efficiency.
NMN/NR + SLU-PP-332 — Critical Pairing
SLU-PP-332 drives massive mitochondrial biogenesis (2.5× mtDNA increase). More mitochondria = exponentially more NAD+ required. Without NMN/NR: SLU-PP-332 drains the intracellular NAD+ pool → oxidative stress, fatigue, cellular exhaustion. NMN/NR is non-optional when running SLU-PP-332.
NMN/NR + Rapamycin — Complementary Anti-Aging Axes
Rapamycin induces mitophagy (clears damaged mitochondria), shifts NAD+/NADH to more oxidized ratio (improves SIRT1 efficiency). NMN/NR provides NAD+ substrate for SIRT1 and builds new mitochondria via PGC-1α. Different but synergistic: Rapamycin creates the optimal metabolic environment, NMN/NR provides the fuel.
Note: Rapamycin does NOT reduce CD38 expression — PCC1 is needed for that. NMN/NR is wasted on CD38 if senescent cell burden is high.
NMN/NR + Retatrutide — Lean Mass Protection
Retatrutide drives aggressive caloric deficit → muscle catabolism risk. NMN/NR maintains skeletal muscle mitochondrial NAD+ → prevents bioenergetic failure → activates SIRT1 → PGC-1α → oxidative fiber transition (protective).
NMN/NR + Imeglimin
Imeglimin repairs mitochondrial structural architecture; NMN/NR provides NAD+ to drive oxidative phosphorylation in those repaired mitochondria. Different interventions: Imeglimin fixes the hardware, NMN/NR runs the fuel.
Evidence Boundary / Claim Enforcement
⚠️ What Vitals coaching MUST NOT say — claim boundary enforcement:
The following claims are not supported by the current evidence base and must not be used in Vitals coaching, product content, or user-facing communications:
| Prohibited Claim Category | Examples |
|---|---|
| Longevity/lifespan | ”slows aging,” “extends lifespan,” “reverses aging” |
| Cognitive preservation | ”prevents dementia,” “reverses cognitive decline,” “improves brain function” |
| Sirtuin activation | ”activates sirtuins measurably,” “measurable SIRT1 boost” |
| Precursor superiority | ”NMN is superior to NR for [any outcome],” “NR is better than NMN for [clinical endpoint]“ |
| Mitochondrial function | ”improves mitochondrial function (measurable),” “restores mitochondria” |
| DNA repair (consumer-accessible) | “directly repairs DNA,” “genome protection” |
| Drug interactions | ”safe with [any specific medication]“ |
| Anti-sarcopenia | ”builds muscle,” “reverses sarcopenia,” “increases muscle mass” (umbrella review PMID 40275690: insufficient evidence) |
Claim boundary test: If a claim sounds exciting, it probably exceeds the evidence. Use: “the current evidence suggests…” or “the strongest signal is…” rather than definitive efficacy statements.
Safe claim anchors:
- “NR produced ~2.3× greater blood NAD+ elevation than NMN in a 2026 crossover trial” (PK fact)
- “NMN improved insulin sensitivity (clamp-confirmed) in postmenopausal women with prediabetes” (Confirmed, PMID 33888596)
- “NR improved 6-minute walk distance in PAD patients” (Supported, PMID 38871717)
- “Both compounds are safe at studied doses in short-term RCTs” (Safety fact)
Implementation Algorithm Hooks
# Vitals NAD+ Precursor Monitoring — Evidence-Backed Tier
# Sources: PMID 33888596, 41901064, 29599478, 35215405, 36740954, 38871717, 38979132
# doi:10.1038/s42255-025-01421-8 (Nature Metabolism 2026 head-to-head)
from dataclasses import dataclass, field
from enum import Enum
from typing import Optional
import datetime
class Precursor(Enum):
NR = "nicotinamide_riboside"
NMN = "nicotinamide_mononucleotide"
NAM = "nicotinamide"
NONE = "none"
class Population_Risk(Enum):
PREDIA_BETIC = "prediabetic"
OLDER_65 = "older_adult"
PARKINSONS = "parkinsons"
PAD = "peripheral_artery_disease"
COGNITIVE_MCI = "mci"
HEALTHY_GENERAL = "general"
@dataclass
class PrecursorDosing:
precursor: Precursor
dose_mg: float
frequency: str # e.g., "once_daily", "twice_daily"
timing: Optional[str] = None # "morning", "afternoon" — PM timing for NMN per PMID 35215405
@dataclass
class MonitoringPlan:
precursor: Precursor
population_risk: Population_Risk
log_blood_pressure: bool = True
log_fasting_glucose: bool = False # Only for prediabetic NMN users
log_cgm: bool = False # Only for prediabetic NMN users; requires clinical sign-off
log_sleep: bool = True # Consumer wearable data
log_body_weight: bool = False # Only if MIB-626 or specific NMN formulation
log_nad_blood: bool = False # Lab draw — not wearable-native
expected_bp_effect_mmHg: float = -3.0 # NMN meta-analysis: -3.94 systolic ≥60 (PMID 41901064)
expected_glucose_effect: Optional[str] = None # From PMID 33888596 clamp study
evidence_grade: str = "MODERATE"
def build_monitoring_plan(dosing: PrecursorDosing, population: Population_Risk) -> MonitoringPlan:
"""
Build an evidence-backed biometric monitoring plan for a user on NR or NMN.
Decision logic:
- NMN + prediabetic/prediabetic risk → fasting glucose, HbA1c, consider CGM (PMID 33888596)
- NR or NMN + older adult (≥65) → blood pressure + sleep metrics (PMID 41901064, 35215405)
- NR + PAD → 6-min walk proxy via step count/HR recovery (PMID 38871717)
- Any NMN + weight concern → weekly body weight log (PMID 36740954, MIB-626 formulation-specific)
- NR head-to-head PK advantage: NR 2.3x greater blood NAD+ elevation (doi:10.1038/s42255-025-01421-8)
→ but no known downstream clinical outcome advantage; do NOT claim outcome superiority
"""
plan = MonitoringPlan(
precursor=dosing.precursor,
population_risk=population,
)
if dosing.precursor == Precursor.NMN and population in (Population_Risk.PREDIA_BETIC, Population_Risk.OLDER_65):
plan.log_fasting_glucose = True
if population == Population_Risk.PREDIA_BETIC:
plan.log_cgm = True # Human sign-off required
plan.expected_glucose_effect = "improved_insulin_sensitivity_clamp_demonstrated"
if dosing.precursor == Precursor.NR and population == Population_Risk.PAD:
plan.log_body_weight = True # Monitor for any weight change alongside functional capacity
# NMN PM timing observation (PMID 35215405) — flag as behavioral variable
if dosing.precursor == Precursor.NMN and dosing.timing == "afternoon":
plan.log_sleep = True # PM NMN associated with reduced drowsiness
return plan
# =============================================================================
# CLAIM BOUNDARY ENFORCEMENT — What Vitals Coaching MUST NOT SAY
# =============================================================================
UNSUPPORTED_CLAIMS = [
"slows aging",
"extends lifespan",
"prevents dementia",
"reverses cognitive decline",
"activates sirtuins measurably",
"superior to [other precursor] for [any outcome]",
"improves mitochondrial function (measurable)",
"directly repairs DNA (consumer-accessible)",
"safe with [any specific medication]",
]
def check_claim_boundary(claim: str) -> bool:
"""
Returns True if claim is evidence-supported.
Returns False if claim exceeds the evidence base — do NOT use in coaching.
"""
claim_lower = claim.lower()
for prohibited in UNSUPPORTED_CLAIMS:
if prohibited in claim_lower:
return False
return True
# Example usage:
# dosing = PrecursorDosing(Precursor.NMN, dose_mg=250, frequency="once_daily", timing="afternoon")
# plan = build_monitoring_plan(dosing, Population_Risk.OLDER_65)
# assert check_claim_boundary("NMN lowers blood pressure modestly in older adults") == True
# assert check_claim_boundary("NMN activates sirtuins and extends lifespan") == FalseActive Clinical Trials to Watch
| Trial | ID | Phase | Population | Status | Key Endpoint |
|---|---|---|---|---|---|
| NOPARK | NCT03568968 | Phase 2 | Early-stage PD (target n=400) | Ongoing | NAD+ repletion; disease modification — expected 2027–2028 |
| N-DOSE | NCT05589766 | Phase 2 | PD patients | Ongoing | Optimal biological dose (OBD) |
| Niagen IV | NCT07251608 | Phase 1 | Healthy adults | Ongoing | Injectable NR safety |
| MINT | NCT05703074 | N/A | Long COVID | Completed 2025 | Quality of life |
| NADPARK | NCT03568968 | Phase 1 | Treatment-naïve PD (n=30) | Completed | Cerebral NAD+ (31P-MRS); safe |
| NR-SAFE | Not NCT-registered | Phase 1 | PD patients | Completed | Safety at 3000 mg/day |
Risks and Uncertainty
| Risk Category | Detail |
|---|---|
| Long-term safety | No human RCT >12 weeks for NMN; no long-term pharmacovigilance data |
| Population gaps | No data in pregnant/lactating women, children, active cancer patients, or healthy adults <40 |
| Drug interactions | No DDI studies with antihypertensives, hypoglycemics, statins, or anticoagulants |
| PARP interaction | Theoretical concern with chemotherapy agents and PARP inhibitors — no human cases documented |
| Quality control | Commercial supplement contamination/purity risks unaddressed in clinical trial literature |
| Brain penetration | Human BBB penetration not directly confirmed for NMN; cerebral NAD+ elevation shown for NR in PD |
| Tissue specificity | Blood NAD+ elevation may not reflect tissue-specific NAD+ distribution |
Cancer Chemotherapy Interaction Risk
TL;DR: Preclinical evidence (Cancer Letters 2026, PMID 41724424) shows NMN/NR/NAM protected pancreatic cancer cells from oxaliplatin, 5-FU, and gemcitabine in vitro and in mice via NAD+-dependent DNA repair enhancement. No human clinical trial has confirmed this interaction. This is a preclinical contraindication signal requiring oncologist consultation — NOT a confirmed clinical contraindication.
Primary anchor: Nakazzi et al., Cancer Letters, April 2026 (PMID 41724424) — NMN, NR, and NAM all protected PDAC cells from oxaliplatin, 5-FU, and gemcitabine via three mechanisms: (1) tumor energy boost, (2) reduced tumor ROS, (3) suppressed DNA damage response. Potency ranking in PDAC: NMN > NR > NAM.
Most at-risk scenario: NMN + oxaliplatin, 5-FU, or gemcitabine in pancreatic/colorectal cancer. PARP inhibitor patients (olaparib, rucaparib, niraparib) at theoretical additional risk.
Critical gap: Zero prospective human RCTs have demonstrated actual chemotherapy efficacy reduction from NAD+ precursors. Three active trials: NCT03642990 (NR + chemo neuropathy), NCT06966583 (NMN + radioimmunotherapy NSCLC), NCT05732051 (NR + cancer recurrence).
Formulation risk: PMID 38935229 — commercial NMN label accuracy −100% to +28.6% deviation; unpredictable dosing adds uncertainty.
NAD+ precursor distinctions:
- NMN: Strongest PDAC protection signal; best human safety data up to 1200 mg/day
- NR: Moderate PDAC signal; may be less risky than NMN in this context; also showed benefit with paclitaxel/cisplatin neuropathy (PMID 35875690, 39128506)
- NAM: Weakest PDAC signal; Preiss-Handler metabolic pathway; sirtuin-inhibiting at high doses may partially reduce the protective DNA repair mechanism
Vitals framing:
- Non-cancer users: No change to current supplementation guidance
- Active cancer patients on chemotherapy: ADVISORY — disclose all NAD+ supplements to oncologist before continuing; do not self-discontinue prescribed treatment
- PARP inhibitor patients: Discuss with oncologist before using NAD+ precursors
- Cancer survivors post-treatment: Theoretical risk is lower but unstudied
Links
- GHK-Cu — SIRT1 synergy
- PCC1 — CD38 unlock
- SLU-PP-332 — mandatory NAD+ pairing
- Rapamycin — mitophagy + NAD+ complement
- Retatrutide — lean mass protection
- Imeglimin — mitochondrial architecture repair + NAD+ fuel
- Mitophagy — mechanism shared with Rapamycin and Urolithin A
- Exercise Mimetics — overlaps with PGC-1α / SIRT1 axis
- NADH NAD+ disruption — contrast: that note is about alcohol-induced NADH elevation; this note is about NAD+ replenishment