Coenzyme Q10 (CoQ10 / Ubiquinol)

Coenzyme Q10 (CoQ10 / Ubiquinol) scored 7.1 / 10 (💪 Strong recommend) on the BioHarmony scale as a Substance → Vitamin / Mineral / Nutrient.

Coenzyme Q10 is a fat-soluble mitochondrial cofactor and antioxidant that the body makes but loses with age and statin use. Its strongest evidence is cardiac: in the 420-patient Q-SYMBIO trial, Mortensen 2014 found 300 mg/day cut major cardiac events from 26% to 15% (hazard ratio 0.50) and halved cardiovascular mortality. It earns 7.1/10, strong recommend, for cardiac and statin cases.

Overall7.1 / 10💪 Strong recommendWorth prioritizing

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Cardiovascular 7.5 Mitochondrial 7.0 Energy / Fatigue 6.0 Longevity / Lifespan 6.0 Antioxidant / Oxidative Stress 5.5

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7.1

Midpoint (5.0)

💪 Coenzyme Q10 (CoQ10 / Ubiquinol)

◄ Downside 0.68 | Upside 2.37 ►

📊 Moderate confidence (±0.7 · evidence 3.6/5)

📅 Scored June 18, 2026·BioHarmony v2.0·Rev 2

Key Takeaways

CoQ10 is a cheap, very safe mitochondrial cofactor with genuine hard-outcome evidence; it scores 7.1/10, strong recommend.
The flagship result is Q-SYMBIO (Mortensen 2014): in 420 chronic heart-failure patients, 300 mg/day cut major adverse cardiac events from 26% to 15%, hazard ratio 0.50, and halved cardiovascular mortality.
For statin muscle symptoms, a 12-RCT meta-analysis (Qu 2018) found CoQ10 significantly reduced pain, weakness, cramp, and tiredness, though it did not change creatine kinase.
Honest counterweights exist: a Cochrane review (Ho 2016) found no significant blood-pressure effect, and a confirmed-myopathy RCT (Taylor 2015) found no muscle benefit, so responses vary.
Safety is excellent: the observed safe level is 1,200 mg/day (Hidaka 2008), with only mild GI upset; ubiquinol absorbs better than ubiquinone for older or poor-absorbing users.

Key Facts

Use cases: cardiovascular mitochondrial energy cognition-focus longevity
Type: Vitamin / Mineral / Nutrient
Legal: OTC
Modality: Fat-soluble mitochondrial cofactor and antioxidant supplement (ubiquinone or its reduced form ubiquinol); endogenously synthesized but supplemented orally
Mechanism: Shuttles electrons in the mitochondrial respiratory chain (complexes I to III) to drive ATP production, and acts as a lipid-phase antioxidant that protects membranes and LDL from oxidation
Typical clinical dose: 100-300 mg/day with a fat-containing meal; heart-failure and statin trials cluster at 100-300 mg/day, often divided
Community / high-dose range: 300-600 mg/day; mitochondrial-disease and migraine protocols go higher, and the observed safe level is 1,200 mg/day per Hidaka 2008
Forms: Ubiquinone (oxidized, cheaper, well-studied) and ubiquinol (reduced, better absorbed in older or poor-absorbing users per Langsjoen 2014). Both convert to each other in the body.
Onset to measurable effect: Plasma levels rise within days to weeks. Clinical endpoints are slow: heart-failure and statin-muscle benefits accrue over roughly 8-16 weeks, migraine prophylaxis over about 3 months.
Bioavailability: Poorly water-soluble; absorption is low and improves substantially with dietary fat and with solubilized or ubiquinol formulations. Take it with the fattiest meal of the day.
Statin interaction: Statins lower endogenous CoQ10 by blocking the mevalonate pathway; Banach 2015 pooled placebo-controlled arms showing plasma CoQ10 fell 0.44 micromol/L on statins. This is the mechanistic basis for co-supplementing.
Cost range: Roughly $15-40/month for ubiquinone at 200 mg/day; ubiquinol runs higher, often $30-60/month. Generic ubiquinone is the value option.
Flagship evidence: Mortensen 2014 Q-SYMBIO heart-failure mortality RCT, Lei 2017 14-RCT heart-failure meta-analysis, Qu 2018 statin-myopathy meta-analysis, and Alehagen 2013 KiSel-10 CoQ10-plus-selenium mortality trial.
Evidence base: Multiple RCTs and meta-analyses with several hard outcome endpoints (mortality, cardiac events), plus honest null results on blood pressure and confirmed statin myopathy. Stronger outcome data than most supplements.
Legal status: US over-the-counter dietary supplement. FDA does not pre-approve supplement health claims. No prescription required.
Worst-case safety risk: Very low intrinsic toxicity. Mild GI upset is the main effect. The practical caution is a possible reduction in warfarin effect, since CoQ10 structurally resembles vitamin K2.
Confidence: Moderate-high for heart-failure and statin-muscle direction; moderate for migraine and mitochondrial support; low for energy or anti-aging claims in healthy people.
Last scored: June 18, 2026 · BioHarmony v2.0

Nick's Take

7.0 / 10 personal rating

Researching

“I am still putting CoQ10 through its paces, mostly in the context of statin users and older clients whose mitochondrial output is clearly slipping. The appeal to me is that this is one of the few cheap whole-class supplements with hard outcome data behind it, not just a moved biomarker: the heart-failure mortality signal and the statin-muscle relief are the kind of real-world results I actually care about. What I am watching is the gap between those strong cardiac findings and the softer, hyped claims around energy and anti-aging in healthy people. So my working stance is that CoQ10 earns its place for specific cardiac, statin, and mitochondrial-deficit cases, while I stay skeptical of it as a generic energy pill, and I lean ubiquinol for anyone over fifty.”
Nick Urban

Nick Urban · CHEK Functional Health Coach (FHC) · School of Biohacking Instructor · Outliyr Founder

Subjective personal experience. This is separate from the systematic BioHarmony score above, which reflects weighted research evidence.

What is Coenzyme Q10 (CoQ10 / Ubiquinol)?

Coenzyme Q10 is a fat-soluble compound your body makes and stores in nearly every cell, sold as a supplement in two interchangeable forms: ubiquinone (oxidized) and ubiquinol (reduced). It does two jobs at once. It carries electrons through the mitochondrial respiratory chain to produce ATP, the energy currency of the cell, and it acts as the main fat-soluble antioxidant inside membranes and circulating LDL. Levels decline with age and drop further on statins, which is the practical reason most people supplement it. Its standout credential is that, unlike most supplements, it has hard outcome data: in the Q-SYMBIO heart-failure trial, Mortensen 2014 found 300 mg/day cut major cardiac events from 26% to 15% and halved cardiovascular mortality. The score sits at strong-recommend because that evidence is genuine, replicated, and paired with an almost spotless safety record.

The honest boundary is that CoQ10's benefits are concentrated in specific populations. It shines in heart failure, statin users with muscle complaints, migraine prevention, and people with a real mitochondrial or CoQ10 deficit. For healthy, well-nourished people chasing more energy or anti-aging, the controlled evidence thins out fast, and the rigorous data on blood pressure is actually null. CoQ10 is a targeted tool with strong data in its lane, not a universal vitality pill.

Terminology

A handful of terms decide whether you read CoQ10 marketing correctly. The two that matter most are the difference between its two chemical forms and the distinction between a moved biomarker and a real clinical outcome, since much of the hype rests on the former. Get those right, plus the cardiac abbreviations the trials use, and the evidence becomes easy to weigh.

Ubiquinone: The oxidized form of CoQ10. Cheaper, the most-studied form, and fine for most people under fifty when taken with fat.
Ubiquinol: The reduced form of CoQ10. Better absorbed, especially in older adults, but more expensive per milligram.
ATP: Adenosine triphosphate, the cell's energy currency, produced in mitochondria with CoQ10 as an electron carrier.
Mevalonate pathway: The biochemical route that makes both cholesterol and CoQ10. Statins block it, which is why they lower your own CoQ10.
MACE: Major Adverse Cardiac Events, a combined endpoint of cardiac death, hospitalization, and similar hard outcomes used in Q-SYMBIO.
LVEF: Left-Ventricular Ejection Fraction, a measure of heart pumping function that, notably, did not improve significantly in pooled CoQ10 trials.
NYHA class: New York Heart Association functional class, a heart-failure severity scale.
Creatine kinase (CK): A muscle-damage enzyme; CoQ10 relieves statin-muscle symptoms without lowering it.
OSL: Observed Safe Level, the highest intake with no concerning pattern in human data, set at 1,200 mg/day for CoQ10.
Flow-mediated dilation (FMD): An ultrasound measure of blood-vessel endothelial function that improved in CoQ10 trials.

How do you take Coenzyme Q10 (CoQ10 / Ubiquinol)?

Dosing & Protocols

Dosing information is summarized from published research and community reports. This is not a prescribing guide. Consult a healthcare provider before starting any protocol.

View 3 routes and 3 protocols

Routes & Forms

Route	Form	Clinical Range	Community Range
Oral softgel (ubiquinone)	Oil-suspension softgel	100-300 mg/day	100-600 mg/day
Oral softgel (ubiquinol)	Reduced-form oil-suspension softgel	100-200 mg/day	100-300 mg/day
Oral powder / capsule with carrier oil	Powder-filled capsule, often with rice bran or MCT oil	100-300 mg/day	100-400 mg/day

Protocols

Heart-failure adjunct (under cardiology care) Clinical

Dose: 100 mg three times daily (300 mg/day)
Frequency: Daily, divided with meals
Duration: Ongoing; judged over months

Mirrors the Q-SYMBIO protocol in [Mortensen 2014](https://pubmed.ncbi.nlm.nih.gov/25282031/). An add-on to guideline heart-failure therapy, never a replacement for it.

Statin-muscle support Mixed

Dose: 100-200 mg/day
Frequency: Daily with a fatty meal
Duration: 8-12 weeks before judging symptoms

Reflects the dose range in [Qu 2018](https://pubmed.ncbi.nlm.nih.gov/30371340/). Helps symptoms in many users but not all; [Taylor 2015](https://pubmed.ncbi.nlm.nih.gov/25545331/) was a null trial in confirmed myopathy.

Migraine prophylaxis Clinical

Dose: 100 mg three times daily (300 mg/day)
Frequency: Daily
Duration: At least 3 months

Matches [Sandor 2005](https://pubmed.ncbi.nlm.nih.gov/15728298/), where the responder benefit emerged by month three.

How the score is calculated

Upside (weighted)

+2.37

Downside (harm ×1.4)

0.68

EV = 2.37 − 0.68 = 1.69 → Score = ((1.69 + 7) / 12) × 10 = 7.1 / 10

How this score is calculated →

What are the benefits of Coenzyme Q10 (CoQ10 / Ubiquinol)?

Upside contribution: 2.37

Dimension	Weight	Score	Weighted
Efficacy	25%	3.4	0.850
Breadth	15%	3.6	0.540
Evidence	25%	3.6	0.900
Speed	10%	2.8	0.280
Durability	10%	2.6	0.260
Bioindividuality	15%	3.6	0.540
Total			3.370

Upside Rationale

The upside comes from genuine clinical outcomes, not just moved markers, which is rare for a supplement. The strongest benefit cluster is cardiac: a survival benefit in heart failure and symptom relief in statin users, anchored by Mortensen 2014. The key boundary condition is population. CoQ10 delivers most where there is a real deficit or disease state, and far less in healthy, replete people. That is exactly why a cheap, low-conflict whole-class cofactor earns a place above heavily-marketed metabolic drugs: it produces honest, hard-endpoint benefit at a fraction of the cost and without an industry-narrow evidence base.

Efficacy (3.4/5.0): The single strongest finding is Mortensen 2014, the Q-SYMBIO RCT (n=420), where 300 mg/day cut major adverse cardiac events from 26% to 15%, a hazard ratio of 0.50, and halved cardiovascular mortality over two years. The broader pool in Lei 2017 (14 RCTs, n=2,149) found a mortality risk ratio of 0.69 plus improved exercise capacity. For statin muscle symptoms, Qu 2018 showed significant relief. Efficacy lands at a strong 3.4 because these are real, replicated, hard outcomes. It is held below the top band by honest limits: ejection fraction did not move, blood pressure is null, and benefit in healthy people is weak, so the magnitude is real but population-specific.

Breadth of Benefits (3.6/5.0): CoQ10 touches several systems with at least one credible endpoint each. Cardiovascular: lower mortality and major cardiac events per Mortensen 2014. Muscular: relief of statin-associated symptoms per Qu 2018. Neurological: migraine prophylaxis per Sandor 2005. Vascular: improved endothelial flow-mediated dilation in a five-trial meta-analysis. Longevity-relevant: reduced cardiovascular mortality in elderly patients in the selenium combination trial. That spread earns a 3.6. The scope boundary is that the strength is uneven, very strong for cardiac and statin uses, modest for migraine and endothelium, and thin for energy, cognition, and blood pressure.

Evidence Quality (3.6/5.0): This is unusually good for a supplement. CoQ10 has a properly-powered outcome RCT in Q-SYMBIO, multiple meta-analyses, and a long real-world cardiac-use record, which the v2.0 rubric credits as decision-relevant signal rather than capping at study type. Crucially, the evidence is honest in both directions: the rigorous Cochrane review Ho 2016 found no blood-pressure effect, and Taylor 2015 was null in confirmed myopathy, which actually raises confidence in the positive findings by showing the literature is not uniformly cheerleading. As a cheap, non-patentable molecule, CoQ10 is not subject to the sponsor-narrow evidence discount that applies to heavily-marketed drugs. The 3.6 reflects solid, mixed, but genuinely outcome-level evidence.

Speed of Onset (2.8/5.0): CoQ10 has no acute effect. Plasma levels rise within days to weeks, but the clinical endpoints are slow: the heart-failure and statin-muscle benefits accrued over roughly 8 to 16 weeks, and the migraine responder benefit in Sandor 2005 emerged by month three. A 2.8 reflects a chronic-use benefit profile where nothing is felt quickly and results are judged over a couple of months of consistent dosing, ideally against a tracked endpoint like symptoms or a cardiac marker.

Durability (2.6/5.0): The benefits appear to depend on continued intake. CoQ10 is a replenished cofactor, so stopping it lets plasma levels and any deficit-correction drift back toward baseline rather than holding a new set point. No trial demonstrates a durable washout-resistant effect, and no rebound or worsening beyond baseline has been reported either. The 2.6 reflects an effect that is real while taken but not self-sustaining, typical of a nutritional cofactor rather than a drug with lasting structural change.

Bioindividuality Upside (3.6/5.0): CoQ10 is a strong example of an intervention where the right responder matters enormously. The clearest responders are people with a measurable deficit or disease: heart-failure patients, statin users whose endogenous CoQ10 is suppressed per Banach 2015, older adults, and those with mitochondrial conditions. Weak responders are healthy, well-nourished people with normal baseline levels, for whom the marginal gain is small. There is no routine genetic predictor, but age, statin use, baseline cardiac status, and a measured CoQ10 deficiency are practical real-world predictors of who benefits. That clear responder logic supports a 3.6.

What are the risks & downsides of Coenzyme Q10 (CoQ10 / Ubiquinol)?

Downside contribution: 0.68 (safety risks weighted extra)

Dimension	Weight	Score	Weighted
Safety	30%	1.5	0.450
Side effects	15%	1.5	0.225
Cost	5%	2.3	0.115
Effort	5%	1.5	0.075
Opportunity	5%	2.0	0.100
Dependency	15%	1.4	0.210
Reversibility	25%	1.4	0.350
Total			1.525
Harm subtotal × 1.4			1.729
Opportunity subtotal × 1.0			0.290
Combined downside			2.019
Baseline offset (constant)			−1.340
Effective downside penalty			0.679

Downside Rationale

The downside is genuinely small, which is most of why a population-specific supplement still scores strong-recommend. There is no dominant intrinsic risk cluster: CoQ10 is non-toxic at normal and even high doses, easy to take, and cleanly reversible. The main real concerns are mundane, a warfarin interaction and the opportunity cost of expecting too much in healthy people. The few exposed groups are warfarin users, people who substitute CoQ10 for needed cardiac or statin therapy, and those who overpay for ubiquinol when plain ubiquinone would do.

Safety Risk (1.5/5.0): CoQ10 has very low intrinsic toxicity. The formal safety review Hidaka 2008 set an observed safe level of 1,200 mg/day with no serious adverse effects, and decades of cardiac use in Japan add a large real-world tolerability record. There is no organ-toxicity signal, no catastrophic-risk floor, and no meaningful FAERS-scale problem. The genuinely-low 1.5 is scored at a correctly-dosed baseline. The one intrinsic interaction worth naming is with warfarin: because CoQ10 structurally resembles vitamin K2, it can blunt the anticoagulant, which is a manageable clinician-coordination issue, not a toxicity of the molecule itself.

Side Effect Profile (1.5/5.0): Side effects are mild, uncommon, and reversible. The most frequent are gastrointestinal: nausea, upset stomach, or loose stool, usually avoided by taking CoQ10 with food and splitting larger doses. Mild headache or insomnia is reported rarely. None are dangerous or persistent, and the symptom burden is essentially that of a well-tolerated oil-based capsule. That places the side-effect profile very low at 1.5.

Financial Cost (2.3/5.0): Cost is the most notable downside, modest in absolute terms. Generic ubiquinone runs roughly $15 to $40 per month at 200 mg/day, while ubiquinol, the better-absorbed form, often costs $30 to $60 per month. For a daily long-term supplement that is a real if minor ongoing expense, and the ubiquinol premium is only worth paying for older or poor-absorbing users. The 2.3 reflects a low-but-not-trivial cost that is higher than a cheap whole food.

Time/Effort Burden (1.5/5.0): Effort is minimal: one or two softgels a day with a fatty meal, no cycling, no timing complexity beyond pairing it with dietary fat. The only practical step is remembering to take it with food for absorption. The 1.5 reflects an intervention that slots into any routine with almost no friction.

Opportunity Cost (2.0/5.0): The main opportunity cost is misplaced expectation. Someone who takes CoQ10 as a generic energy or anti-aging pill, or who leans on it instead of proven heart-failure medication, diet change, or a needed statin, could waste money and delay a more effective intervention. It stacks cleanly with essentially everything and crowds out nothing pharmacologically, so the only real cost is treating a targeted cardiac cofactor as a cure-all. The 2.0 captures that low but worth-naming risk.

Dependency/Withdrawal (1.4/5.0): There is no dependency, tolerance, or withdrawal syndrome. CoQ10 is a natural cellular cofactor, and stopping it simply lets levels return toward baseline, a loss of benefit rather than a withdrawal effect. The 1.4 reflects essentially zero dependency risk.

Reversibility (1.4/5.0): Stopping CoQ10 is clean and immediate. There are no lasting physiological changes, no taper requirement, and no irreversible effects; plasma levels and any benefit simply fade over days to weeks. The 1.4 reflects a fully reversible, no-consequences stop.

Is Coenzyme Q10 (CoQ10 / Ubiquinol) worth it?

CoQ10 is a strong-recommend supplement at 7.1/10 for the right person: a cheap, very safe mitochondrial cofactor with genuine hard-outcome evidence in heart failure and real symptom relief for statin users. It earns a place above many heavily-marketed metabolic products precisely because it delivers honest, survival-level benefit without an industry-narrow evidence base, and because its literature is candid about where it fails. The tier is justified by the evidence-risk balance: the cardiac and statin benefits are real and replicated, and the downside is close to zero apart from a manageable warfarin interaction and modest cost. The single most important framing is population. CoQ10 is a targeted tool, excellent in its lane and unremarkable outside it.

✅ Best for: Statin users with muscle aches, cramps, or weakness who want a cheap, safe first thing to try before abandoning a needed statin, supported by Qu 2018. People with chronic heart failure under cardiology care looking for an evidence-backed add-on to standard therapy, based on Mortensen 2014. Adults over fifty whose endogenous CoQ10 is declining, where ubiquinol absorbs better. Migraine sufferers seeking a low-risk preventive option that works over about three months. Older adults with cardiovascular risk, given the mortality signal in the selenium combination trial.

❌ Avoid if: You take warfarin, unless your clinician monitors it, since CoQ10 resembles vitamin K2 and can blunt the anticoagulant. You are looking to replace prescribed heart-failure medication or a needed statin, because CoQ10 is an adjunct, never a substitute. You are a healthy, well-nourished person expecting a noticeable energy boost or anti-aging effect, since the controlled evidence there is thin. You want a blood-pressure treatment, because the rigorous Cochrane data is null. You are pregnant or breastfeeding without clinician guidance, since supplement-dose data in those groups is limited.

What is Coenzyme Q10 (CoQ10 / Ubiquinol) best for?

The overall BioHarmony score reflects the intervention's primary evidence profile. These subratings are independent assessments per use case.

Cardiovascular: 7.5/10

Score: 7.5/10

Cardiovascular is CoQ10's strongest case at 7.5/10 because the evidence reaches hard outcomes, not just biomarkers. In chronic heart failure, Mortensen 2014 (Q-SYMBIO, n=420) found 300 mg/day cut major adverse cardiac events from 26% to 15% (hazard ratio 0.50) and halved cardiovascular mortality over two years, and Lei 2017 pooled 14 RCTs (n=2,149) showing mortality risk ratio 0.69. The honest boundary is that blood pressure is a null result in the rigorous Cochrane synthesis and left-ventricular ejection fraction did not move significantly in the pooled data, so the win is mortality and exercise capacity in heart failure, not a blanket cardiovascular cure.

Mitochondrial: 7.0/10

Score: 7.0/10

Mitochondrial support earns 7.0/10 because CoQ10 is a literal component of the respiratory chain, not a speculative one. It carries electrons between complexes I and III to produce ATP, so in states of genuine deficiency the rationale is mechanistic and direct. Primary CoQ10 deficiency and statin-induced depletion are the clearest cases: Banach 2015 confirmed statins lower plasma CoQ10 by 0.44 micromol/L, and replacing it has a coherent target. The score is held below the cardiovascular case because dedicated human trials measuring mitochondrial function as a clinical endpoint are fewer, and benefit in people with normal baseline CoQ10 is far less certain than in those with a measurable deficit.

Energy / Fatigue: 6.0/10

Score: 6.0/10

Energy lands at 6.0/10, real for deficit states but oversold for healthy people. CoQ10's role in ATP synthesis makes restored energy plausible where levels are low, such as statin users, older adults, or those with fatigue tied to cardiac or mitochondrial issues, and exercise capacity improved in the heart-failure meta-analysis Lei 2017. The catch is that in healthy, replete individuals the controlled evidence for a noticeable energy lift is thin, and effects are gradual rather than stimulant-like. Treat it as a correction for a deficit, judged over weeks against your own exertion tolerance, not as a daily pick-me-up.

Longevity / Lifespan: 6.0/10

Score: 6.0/10

Longevity earns 6.0/10 on one unusually strong signal. In Alehagen 2013 (KiSel-10), 200 mg CoQ10 plus 200 micrograms selenium daily in elderly Swedes cut cardiovascular mortality from 12.6% to 5.9% over roughly five years, a striking outcome that persisted at ten-year follow-up. That is genuine hard-endpoint longevity-relevant data, rare among supplements. The honest caveat is that it was a combination with selenium in a selenium-low population, so the CoQ10-specific contribution is not cleanly isolated. It is enough to take seriously for older adults, especially those with cardiovascular risk, but not a proven standalone lifespan extender.

Antioxidant / Oxidative Stress: 5.5/10

Score: 5.5/10

Antioxidant activity earns 5.5/10 because it is a defining feature of the molecule, not a marketing claim. CoQ10 is the main lipid-phase antioxidant in cell membranes and lipoproteins, where it regenerates vitamin E and limits LDL oxidation. Endothelial function improved meaningfully in a meta-analysis, Gao 2012 reporting a flow-mediated dilation effect size of 1.70 across five trials, which is a downstream antioxidant-linked outcome. The score is mid-range rather than high because raising antioxidant capacity is a mechanism, and the v2.0 rubric credits demonstrated clinical benefit over a moved marker; the real payoff shows up in the cardiovascular endpoints.

Acute Pain Relief: 5.5/10

Score: 5.5/10

This captures statin-associated muscle pain specifically, at 5.5/10. The meta-analysis Qu 2018 pooled 12 RCTs (n=575) and found CoQ10 significantly reduced muscle pain, weakness, cramp, and tiredness, though creatine kinase did not change. The honest counterweight is Taylor 2015, a rigorous crossover in confirmed myopathy that found no benefit. The reconciliation: CoQ10 helps a meaningful share of statin users with muscle complaints but is not universal, so it is a cheap, safe, evidence-backed first thing to try before abandoning a needed statin.

Anti-Inflammatory: 5.0/10

Score: 5.0/10

Anti-inflammatory support sits at 5.0/10. Several trials report modest reductions in inflammatory markers like CRP and IL-6 with CoQ10, consistent with its membrane-antioxidant action, and this plausibly contributes to its cardiovascular effects. But few trials isolate inflammation as the primary clinical endpoint, so this is a supporting mechanism rather than a standalone reason to supplement. Define one marker if this is your goal and judge by it.

Fertility (Male): 5.0/10

Score: 5.0/10

Male fertility earns 5.0/10. Several RCTs and meta-analyses report that CoQ10 improves sperm concentration, motility, and morphology and lowers seminal oxidative stress, with a coherent antioxidant mechanism. The honest limit is that improvements in semen parameters have not clearly translated into higher live-birth rates, and trials are heterogeneous. It is a reasonable, low-risk adjunct for men with oxidative-stress-linked subfertility, judged on a follow-up semen analysis.

Use Case	Score	Summary
○ Cognition / Focus Primary	4.5	Cognition is a weak case at 4.5/10. The antioxidant and mitochondrial rationale is plausible for neurodegeneration, but large trials in Parkinson and Huntington disease were largely negative, and there is no convincing human evidence that CoQ10 improves focus or cognition in healthy people. Any benefit would be indirect, via better cardiac output or correcting a deficit. Do not take it for productivity.
○ Neuroprotection	4.5	Neuroprotection scores 4.5/10. Mechanistic logic is reasonable and early signals existed, but high-dose Parkinson disease trials (such as the QE3 trial) were stopped for futility, so the clinical neuroprotection case has not held up. Mitochondrial and ataxia subgroups remain the most defensible context, under specialist care rather than as a general brain supplement.
○ Endurance / Cardio	4.5	Endurance earns 4.5/10. Exercise capacity improved in heart-failure patients in Lei 2017, which is a real clinical gain in a compromised population. In healthy athletes, however, controlled trials of CoQ10 for performance are mixed and mostly unimpressive, so the ergogenic case for already-fit people is weak. The benefit is best understood as restoring capacity where cardiac or mitochondrial function is impaired, not boosting an intact engine.
○ Metabolic Health	4.5	Metabolic health sits at 4.5/10 as a composite of small lipid, glucose, and inflammatory signals rather than a strong dedicated effect. The most defensible metabolic angle is in statin users and people with cardiovascular risk, where CoQ10's cardiac benefits and antioxidant action overlap. As a primary metabolic intervention it is weak; as part of a cardiac-risk strategy it has a supporting role.
○ Fertility (Female)	4.5	Female fertility scores 4.5/10. CoQ10 is widely used in assisted reproduction for older women on the theory of supporting oocyte mitochondrial function, and small trials show improved ovarian response markers. But clean evidence for higher pregnancy or live-birth rates is limited, so this is a plausible, clinician-guided adjunct rather than a proven treatment.
○ Healthspan	4.5	The KiSel-10 cardiovascular mortality result and the benign safety profile make CoQ10 healthspan-relevant for older, at-risk adults, but it is not a broad healthspan intervention with direct endpoint data outside cardiovascular outcomes.
○ Recovery / Repair	4.0	Recovery scores 4.0/10. Some small trials suggest CoQ10 lowers exercise-induced oxidative stress and muscle-damage markers, but effects on actual recovery and soreness are inconsistent and underpowered. It is a reasonable adjunct for someone already taking it for cardiac or statin reasons, not a standalone recovery aid with solid backing.
○ Blood Sugar / Glycemic Control	4.0	Glycemic control is a modest 4.0/10. A few meta-analyses report small reductions in fasting glucose or HbA1c in diabetics, but the effect is inconsistent and minor relative to diet, exercise, or medication. CoQ10 is not a glycemic-control tool and should not be leaned on for it.
○ VO2 Max	4.0	VO2-relevant exercise-capacity gains appear in heart-failure patients, but healthy-athlete VO2max trials are mixed, so this is conditional on a compromised baseline.
○ Skin / Beauty	3.0	Topical CoQ10 has limited antioxidant skin-aging data, but oral CoQ10 for skin lacks strong human outcome trials; mostly mechanistic optimism.
○ Kidney Function	3.0	Some small signals in CoQ10-deficiency-related nephropathy and dialysis populations, but no broad renal-outcome evidence for general use.

Frequently Asked Questions

What is CoQ10 and what does it actually do?

CoQ10 is a fat-soluble compound your body makes that does two jobs: it shuttles electrons in the mitochondrial respiratory chain to produce ATP, and it works as a lipid-phase antioxidant protecting membranes and LDL from oxidation. Levels fall with age and on statins. Its best-proven benefit is cardiac: in the Q-SYMBIO trial, Mortensen 2014 found 300 mg/day cut major cardiac events from 26% to 15% in heart-failure patients. Think of it as a mitochondrial cofactor with real cardiac data, not a generic energy pill.

How much CoQ10 should I take and when?

Most clinical trials use 100 to 300 mg per day, and 100 to 200 mg daily with a fatty meal is a sensible starting point. Heart-failure and migraine protocols use 300 mg, often split into three doses. Because CoQ10 is fat-soluble, take it with the fattiest meal of the day, which markedly improves absorption. Doses up to 1,200 mg per day were judged safe by Hidaka 2008, but more is not automatically better. Statin users typically do well on 100 to 200 mg daily.

Does CoQ10 really help with statin muscle pain?

For many users, yes, but not everyone. A meta-analysis of 12 RCTs by Qu 2018 found CoQ10 significantly reduced statin-related muscle pain, weakness, cramp, and tiredness, though it did not change creatine kinase. The honest counterweight is Taylor 2015, a rigorous trial in confirmed myopathy that found no benefit. Statins also lower your own CoQ10, which gives a mechanistic rationale. Because it is cheap and very safe, it is a reasonable first thing to try before giving up a needed statin.

Is CoQ10 proven to help heart failure?

It has the strongest supplement evidence in this area. The Q-SYMBIO RCT by Mortensen 2014 (n=420) showed 300 mg/day cut major adverse cardiac events from 26% to 15%, hazard ratio 0.50, and halved cardiovascular mortality over two years, and Lei 2017 pooled 14 RCTs finding a mortality risk ratio of 0.69. Note that ejection fraction did not move significantly, so the win is survival and exercise capacity. It is an add-on to standard heart-failure therapy under cardiology care, never a replacement.

Ubiquinol vs ubiquinone: which form of CoQ10 is better?

Ubiquinol is the reduced form and ubiquinone the oxidized form, and your body interconverts them. The practical difference is absorption: Langsjoen 2014 found ubiquinol raised plasma CoQ10 more than ubiquinone at the same 200 mg dose, an advantage that matters most in older adults and poor absorbers. Ubiquinone is cheaper, well-studied, and fine for most people under fifty when taken with fat. Over fifty, or if ubiquinone underperforms, ubiquinol is the sensible upgrade despite the higher price.

Is CoQ10 safe to take long term, and what are the side effects?

CoQ10 has an excellent safety record. The observed safe level is 1,200 mg per day per Hidaka 2008, and the most common side effects are mild and reversible: stomach upset, nausea, or loose stool, usually avoided by taking it with food and splitting larger doses. There is no organ toxicity or dependency. The one interaction worth knowing is with warfarin, since CoQ10 structurally resembles vitamin K2 and can blunt the blood thinner, so warfarin users should coordinate with their clinician.

Does CoQ10 lower blood pressure?

Probably not meaningfully, despite older claims. An early meta-analysis by Rosenfeldt 2007 suggested large drops, but it was dominated by uncontrolled, open-label data. The rigorous Cochrane review by Ho 2016, pooling only controlled RCTs, found no statistically significant effect on systolic or diastolic blood pressure. So blood pressure is the weakest of CoQ10's mainstream claims; if you want it for hypertension, verify with a home cuff rather than assuming a benefit.

Does CoQ10 help with migraines?

There is supportive evidence for prevention. In an RCT by Sandor 2005, 300 mg/day of CoQ10 produced a 50%-responder rate of 47.6% versus 14.4% on placebo for migraine attack frequency, a number-needed-to-treat of about 3, with the benefit emerging by month three. It is included in some headache-prevention guidance as a reasonable, low-risk option. Set expectations for a gradual effect over roughly three months rather than fast relief, and pair it with standard migraine management.

What could change Coenzyme Q10 (CoQ10 / Ubiquinol)'s score?

BioHarmony scores are living assessments. New research, regulatory changes, or personal context can shift the score up or down. These are the most likely scenarios that would change this intervention's rating.

The most plausible upgrade would come from a second large mortality RCT replicating Q-SYMBIO in heart failure, or a clean CoQ10-alone trial reproducing the KiSel-10 longevity signal, either of which would lift Efficacy and Evidence and could push CoQ10 into top-tier territory. The most plausible downgrade would come from a failed replication of Q-SYMBIO, or consistent new nulls in statin myopathy, which would pull Efficacy and Evidence down toward the worth-trying band.

Scenario	Dimension shifts	New Score
A second large RCT replicates the Q-SYMBIO heart-failure mortality benefit	Evidence 3.6 to 4.3, Efficacy 3.4 to 4.0	8.0 / 10 💪 Strong recommend
A clean CoQ10-alone trial reproduces the KiSel-10 longevity mortality signal	Efficacy 3.4 to 3.9, Breadth 3.6 to 4.0	7.7 / 10 💪 Strong recommend
A large RCT confirms statin-muscle relief with an objective endpoint	Evidence 3.6 to 4.0, Bioindividuality 3.6 to 4.0	7.5 / 10 💪 Strong recommend
A definitive blood-pressure RCT finds a real, clinically useful effect	Breadth 3.6 to 4.0, Efficacy 3.4 to 3.7	7.4 / 10 💪 Strong recommend
A large trial fails to replicate the Q-SYMBIO mortality benefit	Efficacy 3.4 to 2.7, Evidence 3.6 to 3.0	6.3 / 10 👍 Worth trying
Both a failed heart-failure replication and new statin-muscle nulls emerge	Efficacy 3.4 to 2.5, Evidence 3.6 to 2.8	5.9 / 10 👍 Worth trying

Key Evidence Sources

Mortensen SA et al. 2014 - The effect of coenzyme Q10 on morbidity and mortality in chronic heart failure: results from Q-SYMBIO, a randomized double-blind trial, JACC Heart Failure. Q-SYMBIO RCT (n=420, 2 years): 300 mg/day cut major adverse cardiac events 26% to 15% (HR 0.50, p=0.003) and halved cardiovascular mortality (9% vs 16%, p=0.026); flagship hard-outcome evidence.
Lei L, Liu Y 2017 - Efficacy of coenzyme Q10 in patients with cardiac failure: a meta-analysis of clinical trials, BMC Cardiovascular Disorders. Meta-analysis of 14 RCTs (n=2,149): mortality risk ratio 0.69 (95% CI 0.50-0.95, p=0.02) and improved exercise capacity; LVEF and NYHA class were NOT significant, so the win is survival, not ejection fraction.
Qu H et al. 2018 - Effects of Coenzyme Q10 on Statin-Induced Myopathy: An Updated Meta-Analysis of Randomized Controlled Trials, Journal of the American Heart Association. Meta-analysis of 12 RCTs (n=575): CoQ10 significantly reduced muscle pain, weakness, cramp, and tiredness, with no change in creatine kinase; anchors the statin-muscle case.
Taylor BA et al. 2015 - A randomized trial of coenzyme Q10 in patients with confirmed statin myopathy, Atherosclerosis. Crossover RCT (n=41, 600 mg/day) in confirmed statin myalgia: NO benefit on muscle pain, strength, or aerobic performance; the honest null counterweight to Qu 2018.
Ho MJ, Li ECK, Wright JM 2016 - Blood pressure lowering efficacy of coenzyme Q10 for primary hypertension, Cochrane Database of Systematic Reviews. Cochrane review (2 controlled RCTs, n=50): systolic -3.68 mmHg and diastolic -2.03 mmHg, both nonsignificant; concluded no clinically significant blood-pressure effect. The rigorous null on hypertension.
Rosenfeldt FL et al. 2007 - Coenzyme Q10 in the treatment of hypertension: a meta-analysis of the clinical trials, Journal of Human Hypertension. Early meta-analysis (12 trials, 362 patients) reporting large systolic reductions, but dominated by uncontrolled open-label data; included as the optimistic prior that the Cochrane RCT-only synthesis tempered.
Alehagen U et al. 2013 - Cardiovascular mortality and N-terminal-proBNP reduced after combined selenium and coenzyme Q10 supplementation: a 5-year prospective randomized double-blind placebo-controlled trial among elderly Swedish citizens, International Journal of Cardiology. KiSel-10 RCT (n=443, age 70-88): 200 mg CoQ10 plus 200 mcg selenium daily cut cardiovascular mortality 12.6% to 5.9% (p=0.015) with lower NT-proBNP; persisted at 10-year follow-up. Combination trial, not CoQ10 alone.
Sandor PS et al. 2005 - Efficacy of coenzyme Q10 in migraine prophylaxis: a randomized controlled trial, Neurology. RCT (n=42, 300 mg/day): 50%-responder rate for attack frequency 47.6% vs 14.4% placebo (NNT about 3); superior on headache days and nausea days by month 3.
Langsjoen PH, Langsjoen AM 2014 - Comparison study of plasma coenzyme Q10 levels in healthy subjects supplemented with ubiquinol versus ubiquinone, Clinical Pharmacology in Drug Development. Crossover PK study (n=12, 200 mg/day each form): plasma CoQ10 rose to 4.3 mcg/mL on ubiquinol vs 2.5 mcg/mL on ubiquinone; small study by CoQ10 researchers, supports the ubiquinol absorption claim.
Hidaka T et al. 2008 - Safety assessment of coenzyme Q10 (CoQ10), BioFactors. Safety review establishing an Observed Safe Level of 1,200 mg/day/person with low toxicity and no serious adverse effects in humans; anchors the Safety dimension.
Banach M et al. 2015 - Statin therapy and plasma coenzyme Q10 concentrations: a systematic review and meta-analysis of placebo-controlled trials, Pharmacological Research. Pooled placebo-controlled arms: plasma CoQ10 fell 0.44 micromol/L on statins (95% CI -0.52 to -0.37, p less than 0.001); the mechanistic basis for co-supplementing CoQ10 with statins.
Gao L et al. 2012 - Effects of coenzyme Q10 on vascular endothelial function in humans: a meta-analysis of randomized controlled trials, Atherosclerosis. Meta-analysis of 5 trials (n=194): flow-mediated dilation improved with effect size SMD 1.70 (95% CI 1.00-2.40, p less than 0.0001); supports the endothelial and antioxidant case.
Coenzyme Q10 - Wikidata entity Q321285 (ubidecarenone / ubiquinone, fat-soluble mitochondrial cofactor). Canonical entity record for Coenzyme Q10 used for JSON-LD entity linking; aliases include ubiquinone, ubidecarenone, and CoQ10.

What does the evidence say about Coenzyme Q10 (CoQ10 / Ubiquinol)?

Evidence on this intervention is summarized across three complementary streams: contemporary clinical research, pre-RCT-era pharmacology and observational use, and the traditional medical systems that documented it first. Convergence across streams signals higher confidence; divergence is surfaced honestly.

Modern Clinical Research

Confidence: Medium

Modern evidence for CoQ10 is medium overall but unusually strong where it counts: hard cardiac outcomes. The lead source is Mortensen 2014, the Q-SYMBIO RCT (n=420), where 300 mg/day cut major adverse cardiac events from 26% to 15% (hazard ratio 0.50) and halved cardiovascular mortality, and Lei 2017 pooled 14 RCTs (n=2,149) finding a mortality risk ratio of 0.69. For statin muscle symptoms, Qu 2018 found significant relief across 12 trials. The honest counterweights are real and matter: the rigorous Cochrane review Ho 2016 found no blood-pressure effect, ejection fraction did not move in the heart-failure pool, and Taylor 2015 was null in confirmed myopathy. So the modern lens supports CoQ10 strongly for heart failure and statin-muscle cases, modestly for migraine and antioxidant endpoints, and weakly for blood pressure, energy, or cognition in healthy people.

Citations: Mortensen 2014, Lei 2017, Qu 2018, Taylor 2015, Ho 2016, Alehagen 2013, Sandor 2005, Gao 2012

Traditional Medicine Systems

Confidence: Limited

CoQ10 has no ancient medical-system pedigree, because it was only isolated in 1957 and its role in the mitochondrial respiratory chain was worked out shortly after, work that contributed to a Nobel-recognized understanding of cellular energy. Its real lineage is therefore modern: decades of clinical use that began in Japan, where CoQ10 was used for congestive heart failure from the 1970s onward and became one of the most widely used cardiac supplements before Western trials caught up. That long Japanese clinical-use history is the strongest non-trial signal for its tolerability, and the formal safety review Hidaka 2008 reflects that accumulated real-world experience. Alehagen 2013 connects that practical cardiac-use tradition to a measured mortality outcome in elderly patients. This lens should be read as decades of safe, large-scale cardiac use rather than folk tradition, and it reinforces rather than replaces the modern trial evidence.

Citations: Hidaka 2008, Alehagen 2013

Holistic Evidence for Coenzyme Q10 (CoQ10 / Ubiquinol)

Modern RCTs and decades of Japanese cardiac clinical use agree on the same picture: CoQ10 is a safe mitochondrial cofactor with genuine heart-failure and statin-muscle benefits, weaker for blood pressure and general energy, and best targeted at cardiac, statin, and mitochondrial-deficit cases rather than healthy people chasing a generic boost.

What to Track If You Try This

These are the data points that matter most while running a 30-day Experiment with this intervention.

How to read this section

Pre: Test or score before starting the protocol. Anchors a baseline.
During: Track while running the protocol so you can see if anything is changing.
Post: Re-test after a full cycle to confirm the change held.
Up: The marker should rise. For most positive outcomes, that is a good sign.
Down: The marker should fall. For most positive outcomes, that is a good sign.
Stable: The marker should hold steady. Big swings in either direction are a yellow flag.
Watch: Direction depends on dose, timing, and your baseline. Pay close attention to the trend.
N/A: No expected direction. The entry is there to anchor a baseline reading.
Primary: The Pulse dimension most likely to shift. Track this first.
Secondary: Also relevant, but a smaller or less consistent shift. Track if Primary is unclear.

Bloodwork to Order

Open These Markers In Your Dashboard

LDL Cholesterol Pre | Expected Stable
Blood Pressure During | Expected Watch
Creatine Kinase During | Expected Stable
Nt Probnp Post | Expected Down

Pulse Dimensions to Watch

Energy During | Expected Watch | Primary
Body During | Expected Watch | Secondary

Subjective Signals (Daily Voice Card)

Muscle aches, soreness, or weakness (especially on a statin) Scale 1-5 | During | Expected Down
Exertional fatigue or breathlessness during daily activity Scale 1-5 | During | Expected Down

Red Flags: Stop and Consult

On warfarin and seeing a drifting INR; CoQ10 can blunt the anticoagulant, so coordinate with your clinician.
Using CoQ10 in place of, rather than alongside, prescribed heart-failure or statin therapy.
New or worsening muscle weakness on a statin that does not settle; this needs medical review, not just more CoQ10.

📊 How BioHarmony scoring works

BioHarmony translates a weighted expected-value calculation into a reader-facing 0–10 score. Tier bands: Skip 0–2.9, Caution 3.0–4.4, Neutral 4.5–5.7, Worth Trying 5.8–6.9, Strong Recommend 7.0–8.7, Top-tier 8.8–10.0.

Harm-type downsides (safety risk, side effects, reversibility, dependency) carry a 1.4× precautionary multiplier. Harm weighs more than benefit. Opportunity-type downsides (financial cost, time/effort, opportunity cost) are subtracted at face value.

Use case subratings are independent assessments of how well the intervention addresses specific health goals. They are not components of the overall score. Each subrating reflects the scorer's judgment based on use-case-specific evidence, safety, and effect sizes.

Every dimension is evaluated on a 1–5 scale, and the baseline (1) is subtracted before weighting. A perfect intervention with zero downsides contributes zero penalty rather than a residual floor, so top-tier scores are actually reachable.

EV = Upside − Downside
EV = 2.370 − 0.679 = 1.691
Formula v2.0 maps EV = 0 to score 5.0. Above neutral, EV = +4.00 reaches 10.0; below neutral, EV = −5.36 reaches 0.0. Both sides use the full 5-point half-scale.
Score = 5 + (1.691 / 4.00) × 5 = 7.1 / 10

See the full BioHarmony methodology →