Alirocumab (Praluent) vs Canagliflozin

Head-to-head evidence comparison — which supplement is right for you?

Quick answer✓ Generally fine to combine

Alirocumab (Praluent) vs Canagliflozin: Canagliflozin has the stronger overall evidence (4.5 vs 4.5/10); they're alternatives for support heart health — the best pick depends on your goals. Take the 60-second quiz for a pick tailored to your goals.

Canagliflozin Edges Ahead

Canagliflozin wins 1 of 3 categories. Both are solid choices — the best pick depends on your specific goals.

Alirocumab (Praluent)0 wins

Canagliflozin1 win

Which is right for you? Take the 60-second quiz Open in the full comparison tool

Ali4.5

Alirocumab (Praluent)

Mostly mechanism / observationalLimited safety

Cgz4.5

Canagliflozin

Mostly mechanism / observationalLimited safety

Evidence

Evidence Score

Tie4.5/10

Studies: 9

Meta-analyses: 1

Level: Strong

Evidence Score

Tie4.5/10

Studies: 7

Meta-analyses: 1

Level: Emerging

Research findings

Verdict

Mostly mechanism / observational

Top outcomes

LDL cholesterolMostly mechanism / observational3
Cardiovascular outcomesMostly mechanism / observational3

Verdict

Mostly mechanism / observational

Top outcomes

Cardiovascular & heart failureMostly mechanism / observational5
Glucose & weightMostly mechanism / observational3
Lifespan & aging (preclinical)Too few graded studies2

Shared outcomes (1)

Outcomes where both Alirocumab (Praluent) and Canagliflozin have evidence — compare verdict strength side-by-side.

Cardiovascular & heart failureMostly mechanism / observational3Mostly mechanism / observational5

Dosage & timing

Recommended Dosage:

Prescription dosing is 75 mg or 150 mg subcutaneously every 2 weeks (a 300 mg every-4-weeks option exists), titrated by a clinician to the LDL-C target. A prescription drug; not a self-administered supplement regimen.

Best Time:

any

Can take on empty stomach

Best Form:

Subcutaneous prefilled pen/syringe (alirocumab)

Recommended Dosage:

Off-label use mirrors diabetes dosing (e.g. 100–300 mg once daily before the first meal) under a clinician. A prescription drug; not an approved longevity regimen.

Best Time:

morning

Can take on empty stomach

Best Form:

Oral tablet (canagliflozin)

Safety

Limited safetyTie

Drug Interactions:

Statins (mild)
Other lipid-lowering agents (ezetimibe) (mild)

Side Effects:

Injection-site reactionNasopharyngitis / flu-like symptomsHypersensitivity / allergic reaction

Contraindications:

Known serious hypersensitivity to alirocumab or excipients
Pregnancy (limited data; lipid lowering generally deferred in pregnancy)

Limited safetyTie

Drug Interactions:

Diuretics (moderate)
Insulin / sulfonylureas (moderate)

Side Effects:

Genital yeast infectionVolume depletion / dizzinessEuglycemic diabetic ketoacidosis

Contraindications:

Type 1 diabetes (ketoacidosis risk)
Severe renal impairment / dialysis

Shared goals

Support heart healthAlirocumab (Praluent)

Alirocumab (Praluent)80/100

Canagliflozin70/100

What you'll notice

📉 Large LDL-C reductionpositive

Within weeks

❤️ Fewer cardiovascular eventspositive

Months to years

🫀 Possible mortality benefitpositive

Years

💉 Injection-site reactionstrade-off

At each injection

⏳ Lifespan extension (male mice)positive

Unknown in humans

❤️ Cardiovascular & kidney protectionpositive

Months to years

📉 Modest weight & BP reductionpositive

Weeks to months

⚠️ Genital infections / ketoacidosistrade-off

Throughout use

Key studies

Alirocumab and Cardiovascular Outcomes after Acute Coronary Syndrome.

The New England journal of medicine (2018) · Rct · n=18924

ODYSSEY OUTCOMES randomized trial of ~18,900 patients 1–12 months after acute coronary syndrome on intensive statins

Efficacy and safety of alirocumab in reducing lipids and cardiovascular events.

The New England journal of medicine (2015) · Rct · n=2341

ODYSSEY LONG TERM randomized trial in high-cardiovascular-risk patients on maximally tolerated statins

ODYSSEY FH I and FH II: 78 week results with alirocumab treatment in 735 patients with heterozygous familial hypercholesterolaemia.

European heart journal (2015) · Rct · n=735

Pooled ODYSSEY FH I and FH II randomized trials in 735 heterozygous familial-hypercholesterolemia patients

All Alirocumab (Praluent) studies

Canagliflozin extends life span in genetically heterogeneous male but not female mice.

JCI insight (2020) · Animal

NIA Interventions Testing Program: canagliflozin extended lifespan in male mice

Empagliflozin, Cardiovascular Outcomes, and Mortality in Type 2 Diabetes.

The New England journal of medicine (2015) · Rct · n=7020

EMPA-REG OUTCOME randomized trial (empagliflozin, same class)

Empagliflozin in Heart Failure with a Preserved Ejection Fraction.

The New England journal of medicine (2021) · Rct

EMPEROR-Preserved randomized trial (empagliflozin)

All Canagliflozin studies

Frequently asked questions

Is Alirocumab (Praluent) better than Canagliflozin?

Canagliflozin has a higher evidence score (4.5/10 vs 4.5/10) and wins in 1 of 3 categories.

Is Alirocumab (Praluent) or Canagliflozin better for support heart health?

For support heart health, Alirocumab (Praluent) has a higher relevance score (80 vs 70).

Can I take Alirocumab (Praluent) and Canagliflozin together?

No known interactions between Alirocumab (Praluent) and Canagliflozin have been documented in our database. However, always consult a healthcare provider before combining supplements.

Still deciding between Alirocumab (Praluent) and Canagliflozin?

The right pick depends on your goals. Answer a few quick questions for a personalised recommendation — or dig into the full evidence on each.

Get your personalised pick Alirocumab (Praluent) details Canagliflozin details