Summary: CBD is one of the most misunderstood supplements on the market. It works — but only at doses far higher than what's in your gummy. The problem is that those effective doses (300mg+) approach the level where 5–6% of healthy adults develop liver damage within a month. The OTC doses people act
Think of CBD like a medicine that only comes in one pill size — but that pill is 150 times the dose your body can handle safely every day. At 300mg it genuinely pushes a calming switch in the brain (a serotonin receptor called 5-HT1A). The problem is that same dose hits your liver's chemical processing machinery so hard that 1 in 20 healthy adults develop organ stress within a month at 400mg.
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Cannabidiol — sleep, anxiety, pain: evidence vs marketing
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The Plain English Version
CBD works at doses your body can't safely take every day — which is the entire problem.
Think of CBD like a medicine that only comes in one pill size — but that pill is 150 times the dose your body can handle safely every day. At 300mg, it genuinely pushes a calming switch in the brain (a specific serotonin pathway). The problem is that same dose hits your liver's chemical processing machinery so hard that 1 in 20 healthy adults develop organ stress within a month.
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§3 — Marketing Claims
"A natural solution for pain, sleep, and stress — all the benefits of cannabis without the high."
Pain Relief
A natural alternative to NSAIDs and opioids, reducing chronic and neuropathic pain through anti-inflammatory action — without side effects.
Sleep Aid
Improves sleep quality and duration. Positioned as a "natural melatonin alternative" that is non-habit-forming and free of morning grogginess.
Anxiety Relief
Reduces generalised anxiety, social anxiety, and stress-related burnout by modulating the stress response — without any psychoactive effects.
These three claims drive an enormous OTC market. The marketing is not dishonest about what CBD might do — the problem is the dose required to do it.
§5 — Evidence Review
| Claimed Benefit | Evidence | Verdict |
|---|---|---|
| Anxiety — acute, situational Masataka 2019 (N=37, 300mg/4wks); Crippa 2021 (N=120, 300mg/28d) |
MODERATE | Works — at 300mg single dose only |
| Anxiety — chronic, generalised Requires ≥150mg/day; chronic use hits hepatotoxicity ceiling |
WEAK | Too risky for daily use |
| Sleep quality Saleska 2023: 15mg CBD vs 5mg melatonin (pragmatic RCT) |
WEAK | Not superior to melatonin |
| Sleep architecture at high dose Shannon 2019 (160mg); multiple actigraphy studies |
WEAK | Subjective benefit only — anxiolysis secondary, not sleep architecture change |
| Chronic pain (monotherapy) Wang 2021 BMJ — 32 RCTs, N=5,000+ |
DEBUNKED | –0.50cm on 10cm VAS — below clinical relevance threshold |
| Anti-inflammation TRPV1 mechanism exists; unquantified at OTC doses |
WEAK | Underdosed at OTC levels — mechanism not activated |
What would change the anxiety verdict: Chronic-use RCT at 75–150mg/day with bi-weekly liver monitoring demonstrating safety at sub-hepatotoxic doses over 6+ months.
What would change the pain verdict: Adequately powered RCT showing ≥1cm VAS reduction (minimum clinically important difference) with CBD monotherapy, controlling for placebo and THC content.
–0.50cm
Pain reduction across 32 RCTs (N=5,000+) on a 10cm scale · Minimum clinically important difference: 1–2cm
The dose paradox is the entire story. The therapeutic dose gap is unbridgeable with current evidence: effective doses (300–600mg) exceed EFSA 2025's provisional daily intake limit of 2mg by 150–300 times and approach the liver damage threshold confirmed in healthy adults. STRONG
What would change this: A safe-dose bracket identified by mechanistic dose-finding studies that demonstrates anxiolytic efficacy below the hepatotoxicity floor.
OTC doses of 10–50mg have no demonstrated mechanism of action in any human clinical trial. STRONG
What would change this: A positive Phase II RCT at ≤50mg showing measurable pharmacodynamic effect via validated biomarkers.
§6 — Mechanism
CBD is not a classical cannabinoid agonist. It has very low binding affinity for the CB1 and CB2 receptors that THC targets — which is why it produces no psychoactive effect. Its pharmacological effects come from a different set of targets.
5-HT1A Receptor
At 300mg+, CBD partially activates this serotonin receptor. This is the source of its anxiolytic effect — the only claim with MODERATE evidence. Only active at high acute doses.
TRPV1 Ion Channel
Modulates pain perception channels. Bell-shaped dose response: moderate doses produce analgesic effects; at very high doses this pathway becomes anxiogenic — too much CBD can increase anxiety.
Adenosine Reuptake
Inhibiting adenosine reuptake increases extracellular adenosine, contributing to sedation and anti-inflammatory signalling. This is partly why high-dose CBD is associated with subjective sleepiness.
CYP3A4 / CYP2C19
CBD potently inhibits these liver enzymes. This is NOT a therapeutic mechanism — it is the source of severe drug interactions (clobazam +500%) and the primary pathway for liver damage at therapeutic doses.
The fundamental problem: The only mechanisms with human clinical support require doses that are acutely unsafe for chronic use and now non-compliant with European food safety standards. There is no therapeutic window that is both effective AND safe for daily use.
§8 — Translation Gap
The Lab
Clinical trials use pharmaceutical-grade isolate at 150–600mg/day under clinical monitoring with regular liver function tests.
Real World
OTC consumers take 10–50mg/day — doses below any demonstrated mechanism of action threshold in any human trial.
The Lab
Clinical trials use ≥98% pure isolate with zero THC — pharmacologically predictable, third-party verified.
Real World
21–35% of commercial CBD products contain detectable THC (Johns Hopkins 2022). Only 24% are accurately labelled. Consumer products are pharmacologically unpredictable.
The Lab
Florian 2025 (JAMA) used 400mg/day — a dose consumers genuinely attempt for anxiety and sleep — with regular liver monitoring.
Real World
5.6% of healthy adults developed liver damage with no external symptoms. The injury went undetected without blood tests. No clinical supervision exists at consumer level.
§9 — Exactly How to Use It
| Who | Dose | Timing | Form | Notes |
|---|---|---|---|---|
| Acute situational anxiety only Clinically diagnosed SAD or high-stakes event |
300mg single dose | 60–90 min pre-stressor | Isolate oil + high-fat meal, or water-soluble | No loading. No repeat dosing. Not for daily use. |
| Chronic / daily anxiety | NOT RECOMMENDED | — | — | Chronic hepatotoxicity risk. No safe chronic dose established. |
| Athletes (competitive) | AVOID | — | — | 21–35% of products contain undisclosed THC. WADA strict liability. |
| OTC general wellness | 2mg/day max | With high-fat meal | Isolate oil only (≥98% purity) | EFSA 2025 provisional ADI. No demonstrated efficacy at this dose. |
Oil Isolate (fed)
~24% absorption
Only reliable form for dose-controlled acute use. Take with high-fat meal — boosts absorption from 6% to 24%.
Water-Soluble
>30% estimated; Cmax ~5.7× vs isolate
Consistent dosing without food dependency — but note the paradox: higher absorption means more CBD hitting the liver per milligram.
SNEDDS / Nanoemulsion
~7× AUC vs standard oil
Pharmaceutical-grade. Highest absorption. Not available OTC in standardised form.
Gummies
Highly variable / poor
Marketing format. Typical doses are sub-threshold. No OTC gummy has demonstrated pharmacological activity.
Full / Broad Spectrum
Unknown — variable THC
Avoid. High THC contamination risk, WADA violation risk, unpredictable pharmacokinetics.
Vapes
Variable — unregulated
Avoid. Unregulated inhalation products. No standardised dose. No safety profile for chronic use.
Absorption tip: A high-fat meal quadruples plasma CBD when using oil isolate. Water-soluble formulations eliminate this food dependency — but do not make CBD safer at therapeutic doses. Higher bioavailability means higher liver exposure per milligram.
§10 — Safety
CBD potently inhibits CYP3A4 and CYP2C19 liver enzymes. Any drug cleared by these pathways will accumulate to dangerous levels.
CYP2C19 inhibition drives active metabolite plasma levels up by up to 500%. Risk of extreme sedation and toxicity. Avoid; requires clobazam dose reduction under physician supervision if co-prescribed (e.g. in Dravet syndrome treatment — the only approved CBD indication).
Hepatotoxic synergy with CBD's direct liver effects — exponentially elevated liver enzyme risk. Contraindicated. Requires frequent liver function monitoring if clinically co-prescribed.
CYP2C9 inhibition increases warfarin plasma levels → elevated INR → increased bleeding risk. Avoid. Requires frequent INR monitoring if clinician deems use necessary.
CYP3A4 + P-glycoprotein inhibition → elevated immunosuppressant levels → organ toxicity risk in transplant patients. Avoid without close clinical supervision.
CNS depression potentiation — increased psychomotor impairment and sedation. Avoid combination.
CYP2C19 inhibition increases SSRI plasma levels. Monitor; dose adjustment may be needed.
| Guideline | Limit | Source |
|---|---|---|
| EFSA Provisional ADI (2025) | 2 mg/day (70kg adult, ≥98% isolate) | EFSA Novel Food Safety Assessment |
| Henderson et al. Upper Limit (2023) | 70 mg/day | Food & Chemical Toxicology — reproductive safety margins |
| Hepatotoxicity threshold (clinical) | ~400 mg/day — 5.6% ALT/AST >3× ULN | Florian 2025, JAMA Internal Medicine (RCT N=201) |
| Effective anxiolytic dose | 300–600 mg single dose | Masataka 2019; Crippa 2021 |
Critical: The only dose range with clinical anxiolytic evidence (300–600mg) violates EFSA's ADI by 150–300× and falls at or above the confirmed hepatotoxicity threshold. There is no currently established safe chronic daily dose that also produces measurable clinical effect.
§12 — Conviction
Exception: MODERATE for acute situational anxiety at 300mg, single-dose only
Overall conviction is LOW because OTC doses have no demonstrated mechanism, chronic daily use is ruled out by hepatotoxicity data, pain monotherapy fails on effect size, and the sleep claim is dominated by a safer, cheaper alternative.
The MODERATE carve-out stands: 300mg single-dose CBD has two well-designed RCTs behind it for diagnosed SAD. This is a real effect — but it is narrow, requires a clinical-grade compound, and is not safe for daily use.
A Phase III, adequately powered, long-term (6+ month) RCT using standardised water-soluble CBD at intermediate OTC doses (75–150mg/day) in a diagnosed population — either Generalised Anxiety Disorder or chronic neuropathic pain — with bi-weekly liver enzyme monitoring and objective biomarker tracking (actigraphy for sleep, validated pain scale for analgesia). The trial must demonstrate both chronic liver safety at these doses AND clinical efficacy above the MCID threshold. Without this, no firm recommendation for OTC daily use can be made.
The regulatory trajectory is moving away from CBD: EFSA 2025's 2mg/day ADI and the Florian 2025 JAMA hepatotoxicity trial are paradigm-shifting in the wrong direction for the supplement industry.
§7 — Where Studies Disagree
Masataka 2019 + Crippa 2021
300mg/day over 4 weeks significantly reduces Social Anxiety Disorder symptoms in clinically diagnosed populations.
Lichenstein 2022 Meta-Analysis
No consistent anxiolytic effects in healthy populations. No benefit in cocaine use disorder. Mixed results across populations.
Shannon 2019 (160mg)
Participants reported increased sleep duration and improved sleep quality vs placebo over several weeks.
Multiple Actigraphy Studies
Objective sleep tracking shows no significant difference in sleep architecture, duration, or quality compared to placebo at 150mg/day for 2 weeks.
Patient Registries & Surveys
Large observational datasets show massive patient-perceived reductions in chronic pain, often reported as clinically meaningful by users.
Wang 2021 BMJ (32 RCTs, N=5,000+)
–0.50cm on a 10cm pain scale from CBD monotherapy — below the 1–2cm minimum clinically important difference.
Current direction: The weight of evidence is moving away from CBD, not toward it. EFSA 2025 and Florian 2025 (JAMA) are paradigm-shifting. The regulatory trajectory is contraction.
§11 — What the Simple Answer Misses
For Sleep
Melatonin dominates the category
0.3–1mg sublingual melatonin taken 60–90 minutes before bed has stronger evidence, a safety profile in a different universe, and costs 5–10% of a comparable CBD product. CBD sleep effects are secondary anxiolysis — the mechanism only works because high-dose CBD reduces anxiety, not because it changes sleep architecture.
For Athletes
The WADA permit is misleading
CBD isolate is technically permitted. But 1 in 4 commercial products contains detectable THC — and WADA strict liability means the athlete bears full responsibility for a positive test, regardless of what the label says. The safer anxiolytic for athletes with performance anxiety: L-theanine 200mg + caffeine, or ashwagandha 600mg/day.
For Chronic Pain
Not a pharmaceutical substitute
The best available evidence — 32 RCTs, 5,000 patients — shows CBD monotherapy produces 0.5cm reduction on a 10cm pain scale. The clinical relevance threshold is 1–2cm. CBD is not a substitute for prescribed analgesia, physiotherapy, or structured rehabilitation for chronic pain.
The One Valid Use Case
Acute situational anxiety — with caveats
Single-dose 300mg CBD for a high-stakes anxiety event (exam, public speaking, diagnosed SAD) has MODERATE evidence. But: isolate only, with a high-fat meal, off CYP-metabolised medications, not pregnant, not an athlete. This is a pharmaceutical-grade compound requiring a clinical-grade risk-benefit calculation.
| Option | Effective Dose | Monthly Cost | Evidence Strength |
|---|---|---|---|
| CBD isolate oil — acute anxiety | 300mg per use (occasional) | £20–40 per bottle (~10 doses) | MODERATE |
| Melatonin (sleep — superior alternative) | 0.3–1mg sublingual | £5–10/month | STRONG |
| CBD OTC general wellness (10–30mg) | Sub-therapeutic (no effect) | £20–40/month | NONE AT THIS DOSE |
| L-theanine + caffeine (anxiolytic for athletes) | 200mg + 100mg pre-performance | £10–15/month | MODERATE |
Melatonin (2026-03-22)
5mg melatonin directly outperforms 15mg CBD for sleep. For sleep, use 0.3–1mg sublingual melatonin 60–90 min before bed. Not CBD.
Ashwagandha (2026-03-19)
600mg/day KSM-66 ashwagandha is the safer daily cortisol/anxiety adaptogen. MODERATE conviction. No hepatotoxicity ceiling.
Caffeine + L-Theanine (2026-03-22)
L-theanine 200mg + caffeine is the safer athlete anxiolytic alternative. No WADA risk, no hepatotoxicity, MODERATE evidence.
§13 — Sources
Key: –0.50cm pain VAS reduction from CBD monotherapy — below 1–2cm MCID. Highest-quality pain evidence available.
Key: 5.6% ALT/AST >3× ULN at 400mg/day in healthy adults within 28 days. No external symptoms — liver injury undetected without monitoring.
Key: Significant anxiolytic and burnout benefit at 300mg/day — supports MODERATE conviction for acute anxiety at therapeutic dose.
Key: 300mg/day significant SAD symptom reduction over 4 weeks in clinically diagnosed population. Core evidence for MODERATE conviction carve-out.
Key: 15mg CBD ≤ 5mg melatonin for sleep improvement. Directly kills CBD sleep claim at typical OTC doses.
Key: UL 70mg/day based on reproductive safety. ADI 0.43mg/kg (~30mg/70kg).
Key: Paradigm-shifting regulatory assessment. Effective doses violate ADI by 150–300×. European regulatory trajectory is contraction.
Key: 69% of products mislabelled; 21% contained detectable THC. Foundation of WADA violation risk argument.
How strong is the evidence for the claims in this review? Higher = more confidence the claims are supported. This does not measure how large the effect is or how important it is compared with other levers.
Is this worth your time, money, effort, risk, and trust for this goal? Different from Verdict Score (evidence strength) and Leverage Map (relative importance) — Action ROI is the worth-it call once friction is priced in.
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