Colchicine: Complete Drug Monograph

Pharmacokinetic Profile

Half-Life

26–31 h (healthy adults)

Metabolism

Hepatic (CYP3A4); P-gp substrate

Protein Binding

~39% (albumin)

Bioavailability

~45%

Volume of Distribution

5–8 L/kg

Clinical Information

Drug Class

Antigout alkaloid; anti-inflammatory

Available Doses

0.5 mg, 0.6 mg tablets/capsules; 0.6 mg/5 mL solution

Route

Oral

Renal Adjustment

Yes — dose reduce in severe impairment

Hepatic Adjustment

Yes — monitor; reduce in severe impairment

Pregnancy

Use only if benefit justifies risk

Lactation

Present in breast milk (<10% maternal dose); exercise caution

Schedule

Not a controlled substance; Rx only

Therapeutic Index

Narrow

Generic Available

Yes

Indications

Indication	Approved Population	Therapy Type	Status
Prophylaxis of gout flares	Adults (Colcrys, Mitigare, Gloperba)	Monotherapy or adjunctive to urate-lowering therapy	FDA Approved
Acute gout flare treatment	Adults (Colcrys)	Monotherapy at first sign of flare	FDA Approved
Familial Mediterranean fever (FMF)	Adults and children ≥4 years (Colcrys)	Long-term monotherapy	FDA Approved
ASCVD risk reduction	Adults with established ASCVD or multiple CV risk factors (Lodoco)	Adjunctive to standard CV therapy	FDA Approved

Colchicine is one of the oldest medications still in clinical use, with origins tracing back thousands of years. It holds a unique position as a drug spanning rheumatology and cardiology, having gained its most recent FDA approval in June 2023 for atherosclerotic cardiovascular disease risk reduction based on the landmark COLCOT and LoDoCo2 trials. Its role in gout remains foundational, recommended as first-line therapy for acute flares by the American College of Rheumatology (2020).

Off-Label Uses

Recurrent pericarditis — Well-established adjunctive role; supported by the COPE, CORP, and CORP-2 trials. Evidence quality: High.

Acute pericarditis — First-line adjunctive therapy per ESC 2015 guidelines (COPE trial). Evidence quality: High.

Calcium pyrophosphate deposition disease (pseudogout) — Used for prophylaxis and acute flares. Evidence quality: Moderate.

Behçet’s disease — Oral and genital ulcers, joint involvement. Evidence quality: Moderate.

Post-pericardiotomy syndrome / atrial fibrillation prophylaxis after cardiac surgery — Supported by the COPPS and COPPS-2 trials. Evidence quality: Moderate.

Primary biliary cholangitis / hepatic cirrhosis — Limited evidence. Evidence quality: Low.

Dose

Dosing

Adult Dosing by Clinical Scenario

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Acute gout flare — first sign of symptoms	1.2 mg (2 tabs) then 0.6 mg 1 h later	N/A (single course)	1.8 mg per course	Must be taken at flare onset; efficacy decreases with delay Repeat course no earlier than 3 days later
Gout flare prophylaxis — during urate-lowering therapy initiation	0.6 mg once daily	0.6 mg once or twice daily	1.2 mg/day	Continue for at least 3–6 months of ULT Without regard to meals
FMF — adult maintenance	1.2 mg/day	1.2–2.4 mg/day in 1–2 divided doses	2.4 mg/day	Titrate in 0.3 mg increments based on response and tolerability
ASCVD risk reduction — established disease or high risk	0.5 mg once daily	0.5 mg once daily	0.5 mg/day	Lodoco formulation; adjunctive to statin and antiplatelet therapy No loading dose required
Recurrent pericarditis — adjunctive (off-label)	0.5 mg BID (≥70 kg) or 0.5 mg daily (<70 kg)	Same as starting	1 mg/day	Given with NSAID or aspirin; taper colchicine last Typical duration 6–12 months
Acute pericarditis — adjunctive (off-label)	0.5 mg BID (≥70 kg) or 0.5 mg daily (<70 kg)	Same as starting	1 mg/day	Per ESC 2015 guidelines; 3-month course

Pediatric Dosing (FMF Only)

Age Group	Starting Dose	Maintenance Dose	Maximum Dose	Notes
4–6 years	0.3 mg/day	0.3–1.8 mg/day	1.8 mg/day	Titrate in 0.3 mg increments; single or divided doses
6–12 years	0.9 mg/day	0.9–1.8 mg/day	1.8 mg/day	Adjust based on disease control and GI tolerability
>12 years	1.2 mg/day	1.2–2.4 mg/day	2.4 mg/day	Same as adult dosing

Renal Impairment Adjustments

Renal Function	Gout Prophylaxis	Acute Gout Flare	FMF	Notes
Mild–moderate (CrCl 30–80 mL/min)	No adjustment	No adjustment	Monitor closely; reduce if needed	Close monitoring for toxicity
Severe (CrCl <30 mL/min)	0.3 mg/day	Standard dose; repeat no more than q2wk	Start 0.3 mg/day	Contraindicated with P-gp/CYP3A4 inhibitors
Dialysis (CrCl <15 mL/min)	0.3 mg twice weekly	0.6 mg x 1 dose; repeat no more than q2wk	Start 0.3 mg/day	Not removed by hemodialysis

Clinical Pearl: Low-Dose Colchicine for Gout Flares

The older high-dose regimen (4.8 mg over 6 hours) is no longer recommended. A pivotal RCT demonstrated that the low-dose regimen (1.8 mg over 1 hour) provides equivalent efficacy with significantly fewer gastrointestinal adverse effects — GI events occurred in 26% with low-dose versus 77% with high-dose versus 20% with placebo (FDA PI).

Pharmacology

Mechanism of Action

Colchicine is a tricyclic lipid-soluble alkaloid derived from Colchicum autumnale (autumn crocus). Its primary anti-inflammatory action centres on the inhibition of β-tubulin polymerisation into microtubules, which disrupts multiple neutrophil functions including migration, adhesion, degranulation, and chemotaxis. By preventing microtubule assembly, colchicine interferes with the intracellular transport machinery that inflammatory cells require to mount an effective response at sites of crystal deposition or vascular injury.

Beyond microtubule disruption, colchicine inhibits the NLRP3 inflammasome complex in neutrophils and monocytes, thereby reducing interleukin-1β (IL-1β) release — a key driver of both gouty inflammation and atherosclerotic plaque instability. It also attenuates the NF-κB signalling pathway and suppresses superoxide production by neutrophils. These combined mechanisms explain its clinical utility across gout, autoinflammatory syndromes, pericarditis, and atherosclerotic cardiovascular disease.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Oral bioavailability ~45%; Tmax 1–1.4 h; food reduces extent by ~15% without clinical significance	Rapid onset; may be taken without regard to meals
Distribution	Vd 5–8 L/kg; protein binding 39 ± 5% (albumin); crosses placenta; enters breast milk	Large Vd reflects extensive tissue binding to intracellular tubulin; not dialyzable
Metabolism	Hepatic via CYP3A4 to 2-O-demethylcolchicine and 3-O-demethylcolchicine; P-gp substrate	Critical pathway for drug interactions; dual CYP3A4/P-gp inhibitors can cause fatal toxicity
Elimination	t½ 26.6–31.2 h (young adults); 10–20% excreted unchanged renally; primarily hepatobiliary	Long half-life supports once-daily dosing; accumulation risk in renal/hepatic impairment

Side Effects

≥10% Very Common

Adverse Effect	Incidence	Clinical Note
Diarrhoea	23% (acute gout, low-dose); up to 20% (FMF); ~10% (CV dose 0.5 mg)	Dose-dependent; early sign of toxicity if severe; reduce dose or stop if persistent
Nausea	4–17% (dose-dependent); up to 20% (FMF)	More common at higher doses and with FMF regimens; usually transient
Abdominal pain / cramping	Up to 20% (FMF)	May herald more significant GI toxicity; dose-limiting

1–10% Common

Adverse Effect	Incidence	Clinical Note
Vomiting	Up to 17% (high-dose); 0% (recommended low-dose gout)	Essentially absent with current low-dose gout regimen; more common in FMF dosing
Pharyngolaryngeal pain	3%	Reported in the acute gout flare trial (FDA PI)
Headache	1–10%	Reported in PK studies at ~10%; lower in clinical trials
Fatigue	1–4%	Generally mild and transient
Myalgia	~21% (CV trials, colchicine) vs 19% (placebo)	From LoDoCo2 Netherlands cohort; distinguish from neuromuscular toxicity

Serious Serious (Regardless of Frequency)

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Myelosuppression (pancytopenia, aplastic anaemia)	Rare	Weeks to months of chronic use	Hold colchicine; obtain urgent CBC; haematology referral
Neuromuscular toxicity / rhabdomyolysis	Rare; higher risk with CYP3A4/P-gp inhibitors or statins	Weeks to months; cumulative	Discontinue colchicine; check CK and renal function; resolves within 1 week to months
Disseminated intravascular coagulation (DIC)	Very rare; usually in overdose	24–72 h post-overdose (phase 2)	Emergency supportive care; ICU admission
Multi-organ failure (overdose)	Dose ≥0.5 mg/kg usually fatal	24–72 h post-ingestion	No specific antidote; aggressive supportive care; not dialyzable
Sensorimotor neuropathy	Rare; cumulative toxicity	Months of chronic therapy	Discontinue; monitor for resolution; nerve conduction studies
Pneumonia (CV indication)	~0.9% vs 0.4% placebo (COLCOT)	Variable	Standard infectious disease workup and treatment

Discontinuation Discontinuation Rates

Acute Gout (Low-Dose Regimen)

37% any drug-related TEAE vs 27% placebo

Top reasons: Diarrhoea (23%), nausea (4%), pharyngolaryngeal pain (3%)

CV Indication — LoDoCo2 Run-In Phase

~7% withdrew during open-label run-in due to GI intolerance

Top reasons: GI upset; ongoing discontinuation rates comparable to placebo during blinded phase

Reason for Discontinuation	Incidence	Context
Diarrhoea	Most common reason across all indications	Dose-dependent; GI effects are the primary driver of treatment cessation
Nausea / vomiting	Second most common	Predominantly seen at FMF doses (1.2–2.4 mg/day) and the obsolete high-dose gout regimen
Myalgia / muscle weakness	Uncommon but may prompt cessation	Warrants CK check to exclude rhabdomyolysis, especially with concurrent statin use

Managing GI Side Effects

Gastrointestinal symptoms are the most frequent adverse effects and should be treated as dose-limiting signals. If diarrhoea becomes persistent or severe, reduce the dose or temporarily hold colchicine. Severe GI symptoms may herald the onset of more dangerous systemic toxicity, particularly in patients with concomitant CYP3A4/P-gp inhibitor use or renal impairment. Reassuringly, the low-dose cardiovascular regimen (0.5 mg daily) shows GI event rates that are barely distinguishable from placebo.

Int

Drug Interactions

Colchicine is a substrate of both CYP3A4 and P-glycoprotein (P-gp). Inhibition of either pathway raises colchicine plasma levels; dual inhibition of both CYP3A4 and P-gp has resulted in fatal colchicine toxicity at standard therapeutic doses. All potential interacting medications must be reviewed before initiating colchicine.

Major Clarithromycin

MechanismDual CYP3A4 + P-gp inhibition

EffectMarked increase in colchicine levels; fatal toxicity reported

ManagementContraindicated in renal/hepatic impairment; if unavoidable in normal function, reduce colchicine to 0.3 mg single dose and do not repeat for 3 days

FDA PI

Major Cyclosporine

MechanismPotent P-gp inhibition

EffectFatal colchicine toxicity reported at therapeutic doses

ManagementContraindicated with renal/hepatic impairment; reduce prophylaxis dose to 0.3 mg/day or every other day

FDA PI

Major Ketoconazole / Itraconazole

MechanismStrong CYP3A4 inhibition

EffectSignificant increase in colchicine exposure

ManagementReduce colchicine dose per PI table; contraindicated with renal/hepatic impairment

FDA PI

Major HIV Protease Inhibitors (ritonavir, atazanavir, etc.)

MechanismStrong CYP3A4 inhibition (most also inhibit P-gp)

EffectAnticipated significant rise in colchicine levels

ManagementAll PIs except fosamprenavir are contraindicated with renal/hepatic impairment; reduce colchicine dose per PI table

FDA PI

Moderate Diltiazem / Verapamil

MechanismModerate CYP3A4 inhibition

EffectIncreased colchicine levels; neuromuscular toxicity reported

ManagementReduce colchicine dose; monitor for myopathy symptoms

FDA PI

Moderate HMG-CoA Reductase Inhibitors (statins)

MechanismAdditive myotoxicity (shared tubulin/mitochondrial pathways)

EffectIncreased risk of myopathy and rhabdomyolysis

ManagementMonitor for muscle symptoms; check CK if symptomatic; LoDoCo2/COLCOT showed combination is generally well tolerated at 0.5 mg/day

FDA PI / LoDoCo2

Moderate Erythromycin

MechanismModerate CYP3A4 inhibition

EffectElevated colchicine exposure

ManagementReduce colchicine dose; use azithromycin as alternative macrolide (minimal CYP3A4 effect)

FDA PI

Minor Grapefruit Juice

MechanismIntestinal CYP3A4 inhibition

EffectModest increase in colchicine bioavailability

ManagementAdvise patients to avoid grapefruit juice during colchicine therapy

FDA PI

Mon

Monitoring

CBC with Differential Baseline, then every 3–6 months for chronic use
Routine Monitor for myelosuppression, leukopenia, thrombocytopenia, or pancytopenia. More frequent monitoring if co-administered with interacting drugs.
Renal Function Baseline, then at least annually
Routine Serum creatinine and estimated CrCl. Colchicine accumulates in renal impairment; dose adjustment required if CrCl falls below 30 mL/min.
Hepatic Function Baseline, then as clinically indicated
Routine LFTs before initiation. Clearance is significantly reduced in hepatic impairment, prolonging half-life and increasing toxicity risk.
Creatine Kinase (CK) If muscle symptoms develop
Trigger-based Check CK and renal function if patient reports new muscle pain, weakness, or tenderness, particularly with concurrent statin or fibrate therapy.
GI Symptoms Every visit; ongoing self-monitoring
Routine Diarrhoea, nausea, vomiting, and abdominal pain are dose-limiting and may signal early toxicity. Severe GI symptoms warrant dose reduction or interruption.
Drug Interaction Review At initiation and every prescription change
Trigger-based Screen for new CYP3A4 inhibitors, P-gp inhibitors, and myotoxic agents. Particular vigilance with antibiotics (macrolides, azole antifungals) and immunosuppressants.

Contraindications & Cautions

Absolute Contraindications

Concurrent use of strong CYP3A4 inhibitors or P-gp inhibitors in patients with renal or hepatic impairment — fatal toxicity has been reported at therapeutic doses in this combination.
Severe hepatic impairment (for the Lodoco ASCVD indication) — contraindicated per Lodoco PI.
Renal failure (CrCl <15 mL/min) (for the Lodoco ASCVD indication) — contraindicated per Lodoco PI.
Combined renal and hepatic impairment — patients with both organ impairments should not receive colchicine.
Preexisting blood dyscrasias (for the Lodoco ASCVD indication).

Relative Contraindications (Specialist Input Recommended)

Severe renal impairment (CrCl <30 mL/min) without concurrent CYP3A4/P-gp inhibitors — dose reduction and close monitoring required; specialist co-management advisable.
Moderate-to-severe hepatic impairment — reduced clearance and prolonged half-life increase toxicity risk; dose reduction and close monitoring.
Concurrent use of multiple myotoxic agents (statins + fibrates + colchicine) — document risk-benefit discussion.
Elderly patients — at increased risk of neuromuscular toxicity even with normal renal and hepatic function; lower starting doses preferred.

Use with Caution

Mild-to-moderate renal impairment (CrCl 30–80 mL/min) — standard dosing acceptable but monitor closely for toxicity.
Mild hepatic impairment — no dose adjustment required; monitor LFTs.
Pregnancy — use only if potential benefit justifies the risk; crosses the placenta.
Lactation — present in breast milk at <10% of the maternal weight-adjusted dose; observe infant for GI symptoms.
Fertility — colchicine may transiently impair fertility (reversible upon discontinuation).

FDA Safety Communication Fatal Overdose and Drug Interaction Warnings

Fatal overdoses, both accidental and intentional, have been reported in adults and children who have ingested colchicine. Colchicine should be kept out of the reach of children. Life-threatening and fatal drug interactions have been reported when colchicine was co-administered with P-gp and/or strong CYP3A4 inhibitors, including clarithromycin and cyclosporine, particularly in patients with renal or hepatic impairment. Acute overdose exceeding 0.5 mg/kg (approximately 35 mg in a 70 kg adult) is usually fatal.

Patient Counselling

Purpose of Therapy

Colchicine works by reducing inflammation in the body. Depending on the reason it was prescribed, it may be used to treat or prevent gout attacks, to control familial Mediterranean fever symptoms, to reduce the risk of heart attacks and strokes in people with established heart disease, or to treat inflammation around the heart (pericarditis). It is not a painkiller and should not be used for general pain relief.

How to Take

Take colchicine exactly as prescribed. It may be taken with or without food. For an acute gout flare, take two tablets (1.2 mg) at the very first sign of a flare and then one tablet (0.6 mg) one hour later. Do not take more than this amount. For preventive use or heart disease, take the prescribed dose at the same time each day. If a dose is missed, take it as soon as remembered but do not double the next dose.

Diarrhoea & GI Upset

Tell patient Loose stools, nausea, and stomach cramps are the most common side effects. These are usually mild and improve within a few days. If prescribed a low dose (0.5 mg daily for heart disease), GI effects are usually minimal.

Call prescriber If diarrhoea becomes severe, persistent, or is accompanied by vomiting or abdominal pain. This may indicate the dose is too high or that toxicity is developing.

Muscle Pain or Weakness

Tell patient Rarely, colchicine can cause muscle damage, especially if taken with certain cholesterol-lowering medications. Report any new muscle aches, tenderness, or unexplained weakness.

Call prescriber Immediately if experiencing significant muscle pain or weakness, dark-coloured urine, or numbness/tingling in hands or feet.

Drug Interactions

Tell patient Inform every healthcare provider that you take colchicine, especially before being prescribed antibiotics (particularly clarithromycin or erythromycin), antifungal medicines, heart medications, or HIV treatments. Avoid grapefruit juice.

Call prescriber Before starting any new medication, including over-the-counter drugs and herbal supplements.

Safe Storage & Overdose Risk

Tell patient Colchicine can be fatal in overdose, even in amounts that seem small. Store securely and keep out of the reach of children at all times.

Call prescriber If more than the prescribed amount is accidentally taken, or if a child ingests any amount, seek emergency medical attention immediately.

Signs of Infection

Tell patient Colchicine can rarely affect blood cell counts, which may make infections harder to fight. Be alert for unusual bruising, persistent sore throat, or unexplained fevers.

Call prescriber If experiencing fever, chills, persistent sore throat, unusual bruising or bleeding, or signs of infection that do not improve.

Ref

Sources

Regulatory (PI / SmPC)

Colcrys (colchicine) Prescribing Information. Takeda Pharmaceuticals America, Inc. Revised October 2022. DailyMed Primary FDA-approved PI for gout and FMF indications; source for dosing, adverse reactions, and drug interaction data.
Lodoco (colchicine 0.5 mg) Prescribing Information. Agepha Pharma USA, LLC. 2023. FDA FDA-approved PI for the cardiovascular disease indication; source for ASCVD dosing and contraindications.
FDA Safety Communication: Colchicine (marketed as Colcrys) Information. FDA, 2009. FDA.gov Documents the transition from unapproved to approved colchicine products and highlights fatal drug interactions.

Key Clinical Trials

Tardif J-C, Kouz S, Waters DD, et al. Efficacy and safety of low-dose colchicine after myocardial infarction. N Engl J Med. 2019;381(26):2497–2505. doi:10.1056/NEJMoa1912388 The COLCOT trial: demonstrated 23% relative risk reduction in MACE with 0.5 mg colchicine daily post-MI.
Nidorf SM, Fiolet ATL, Mosterd A, et al. Colchicine in patients with chronic coronary disease. N Engl J Med. 2020;383(19):1838–1847. doi:10.1056/NEJMoa2021372 The LoDoCo2 trial: demonstrated 31% relative risk reduction in MACE with 0.5 mg colchicine daily in chronic coronary disease.
Terkeltaub RA, Furst DE, Bennett K, et al. High versus low dosing of oral colchicine for early acute gout flare. Arthritis Rheum. 2010;62(4):1060–1068. doi:10.1002/art.27327 AGREE trial: established that low-dose colchicine (1.8 mg total) is equally effective to high-dose (4.8 mg) with significantly fewer GI adverse effects.
Imazio M, Brucato A, Cemin R, et al. A randomized trial of colchicine for acute pericarditis. N Engl J Med. 2013;369(16):1522–1528. doi:10.1056/NEJMoa1208536 ICAP trial: demonstrated that colchicine as adjunct to conventional therapy reduces pericarditis recurrence (16.7% vs 37.5% placebo); established weight-based dosing for pericarditis.

Guidelines

FitzGerald JD, Dalbeth N, Mikuls T, et al. 2020 American College of Rheumatology guideline for management of gout. Arthritis Care Res. 2020;72(6):744–760. doi:10.1002/acr.24180 Current ACR guideline recommending colchicine as first-line therapy for acute gout flares and prophylaxis during ULT initiation.
Virani SS, Newby LK, Arnold SV, et al. 2023 AHA/ACC/ACCP/ASPC/NLA/PCNA Guideline for the Management of Patients With Chronic Coronary Disease. J Am Coll Cardiol. 2023;82(9):833–955. doi:10.1016/j.jacc.2023.04.003 AHA/ACC guideline incorporating low-dose colchicine as a consideration for residual inflammatory risk reduction in chronic coronary disease.

Mechanistic / Basic Science

Leung YY, Yao Hui LL, Kraus VB. Colchicine — update on mechanisms of action and therapeutic uses. Semin Arthritis Rheum. 2015;45(3):341–350. doi:10.1016/j.semarthrit.2015.06.013 Comprehensive review of colchicine’s mechanisms including microtubule inhibition, inflammasome suppression, and NF-κB pathway effects.
Deftereos SG, Beber S, Giannopoulos G, et al. Colchicine pharmacokinetics and mechanism of action. Curr Pharm Des. 2018;24(6):659–663. doi:10.2174/1381612824666180123110042 Concise review covering PK parameters, CYP3A4/P-gp dependence, and primary anti-inflammatory mechanisms.

Pharmacokinetics / Special Populations

Ferron GM, Rochdi M, Jusko WJ, Scherrmann JM. Oral absorption characteristics and pharmacokinetics of colchicine in healthy volunteers after single and multiple doses. J Clin Pharmacol. 1996;36(10):874–883. doi:10.1002/j.1552-4604.1996.tb04753.x Established key PK parameters including bioavailability (~45%), Vss (419 L), and terminal half-life (57.8 h IV).
Rochdi M, Sabouraud A, Girre C, Venet R, Scherrmann JM. Pharmacokinetics and absolute bioavailability of colchicine after i.v. and oral administration in healthy human volunteers and elderly subjects. Eur J Clin Pharmacol. 1994;46(4):351–354. doi:10.1007/BF00194404 Demonstrated similar bioavailability (44–45%) in elderly versus young adults, but higher peak levels and AUC in elderly patients with reduced renal function.
Ben-Chetrit E, Levy M. Colchicine: 1998 update. Semin Arthritis Rheum. 1998;28(1):48–59. doi:10.1016/S0049-0172(98)80028-0 Foundational review of colchicine’s PK and clinical pharmacology including Vd, protein binding, and hepatobiliary excretion pathway.