Pyrazinamide: Comprehensive Drug Monograph

Pharmacokinetic Profile

Half-Life

9–10 hours

Metabolism

Hepatic hydrolysis to pyrazinoic acid; then hydroxylation by xanthine oxidase

Protein Binding

~10%

Bioavailability

Well absorbed orally

Volume of Distribution

Widely distributed; CSF ≈ plasma (inflamed meninges)

Clinical Information

Drug Class

Pyrazine derivative (antimycobacterial)

Available Doses

500 mg tablets

Route

Oral

Renal Adjustment

Use lower end of range; HD: 25–35 mg/kg 3×/wk post-dialysis

Hepatic Adjustment

Contraindicated in severe hepatic damage

Pregnancy

Category C — routine use not recommended; may be justified if benefit outweighs risk

Lactation

Present in breast milk; effect on infant unknown

Schedule

Rx only (not controlled)

Generic Available

Yes

Indications

Indication	Approved Population	Therapy Type	Status
Active tuberculosis — initial intensive phase	Adults and children	Combination therapy (first 2 months of standard 6-month regimen)	FDA Approved
Drug-resistant TB	Adults and children	Component of individualized multi-drug regimen	FDA Approved

Pyrazinamide is a uniquely sterilising agent that targets semi-dormant M. tuberculosis organisms residing in the acidic intracellular environment of macrophages. Its inclusion in the intensive phase was the key innovation that allowed the standard TB treatment regimen to be shortened from 9–12 months to 6 months. Pyrazinamide is always used in combination with other first-line agents (isoniazid, rifampin, ethambutol) and is typically discontinued after the initial 2-month intensive phase.

Off-Label Uses

Multidrug-resistant TB (MDR-TB): Frequently included in longer individualized MDR-TB regimens when susceptibility is confirmed or suspected. Evidence quality: High (WHO guidelines).

Dose

Dosing

Adult Weight-Based Dosing (ATS/CDC/IDSA)

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Active TB intensive phase — daily (40–55 kg)	1000 mg once daily	1000 mg once daily	2000 mg/day	Part of 4-drug regimen for 2 months Dose based on lean body weight
Active TB intensive phase — daily (56–75 kg)	1500 mg once daily	1500 mg once daily	2000 mg/day	Most common weight band Can be given as 3 × 500 mg tablets
Active TB intensive phase — daily (76–90 kg)	2000 mg once daily	2000 mg once daily	2000 mg/day	Max daily dose per CDC FDA PI allows up to 3000 mg/day
Active TB — twice-weekly DOT (40–55 kg)	2000 mg twice weekly	2000 mg twice weekly	4000 mg/dose	Only under DOT; not for HIV or cavitary disease Use only after completing 2-week daily intensive phase
Active TB — twice-weekly DOT (56–75 kg)	3000 mg twice weekly	3000 mg twice weekly	4000 mg/dose	Higher individual doses compensate for intermittent schedule
Active TB — twice-weekly DOT (76–90 kg)	4000 mg twice weekly	4000 mg twice weekly	4000 mg/dose	Max twice-weekly dose per ATS/CDC/IDSA
Active TB — three-times-weekly DOT (56–75 kg)	2500 mg 3×/week	2500 mg 3×/week	3000 mg/dose	Alternative intermittent schedule under DOT
End-stage renal disease / hemodialysis	25–35 mg/kg 3×/week	25–35 mg/kg 3×/week	Per weight band	Administer after dialysis sessions PZA is dialysable

Pediatric Dosing

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Active TB intensive phase — daily (<40 kg)	30–40 mg/kg once daily	30–40 mg/kg once daily	2000 mg/day	ATS/CDC/IDSA recommended range; duration 2 months AAP recommends 20–40 mg/kg; FDA PI: 15–30 mg/kg
Active TB — twice-weekly DOT (<40 kg)	50 mg/kg twice weekly	50 mg/kg twice weekly	2000 mg/dose	Only under directly observed therapy

Clinical Pearl: Duration Limit

Pyrazinamide is used exclusively during the initial 2-month intensive phase and then discontinued. It is NOT continued into the continuation phase. Extending pyrazinamide beyond 2 months does not improve outcomes but increases cumulative hepatotoxicity risk. The exception is drug-resistant TB, where PZA may be used for longer durations as part of an individualised regimen under specialist guidance.

Pharmacology

Mechanism of Action

The precise mechanism of pyrazinamide’s antimycobacterial activity is not fully elucidated. It functions as a prodrug: mycobacterial pyrazinamidase (encoded by the pncA gene) converts pyrazinamide to its active form, pyrazinoic acid (POA). POA accumulates in the acidic intracellular environment of activated macrophages, where it disrupts mycobacterial membrane energetics and inhibits fatty acid synthase I, impairing mycolic acid synthesis. Pyrazinamide is uniquely active against semi-dormant, slowly metabolising bacilli in acidic conditions, which explains its critical sterilising role during the intensive phase. Resistance arises primarily through mutations in the pncA gene, reducing pyrazinamidase activity and preventing prodrug conversion. M. bovis is naturally resistant to pyrazinamide due to a pncA polymorphism.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Well absorbed orally; Tmax ~2 h; Cmax 30–50 mcg/mL at 20–25 mg/kg	Can be taken with or without food; no clinically significant food effect reported in the PI
Distribution	Widely distributed to liver, lungs, and CSF; ~10% protein bound; CSF levels ≈ plasma (inflamed meninges)	Excellent CNS penetration makes PZA valuable in TB meningitis regimens. Freely enters macrophages where acidic conditions activate the drug.
Metabolism	Hepatic hydrolysis by microsomal deaminase to pyrazinoic acid (POA); POA hydroxylated by xanthine oxidase to 5-hydroxypyrazinoic acid	POA competitively inhibits renal tubular urate secretion, causing dose-dependent hyperuricemia in nearly all patients. Xanthine oxidase involvement links PZA metabolism to uric acid handling.
Elimination	Primarily renal; ~4% excreted unchanged, ~70% as metabolites; t½ 9–10 h	Half-life may be prolonged in renal or hepatic impairment. Drug is dialysable; administer post-dialysis for ESRD patients.

Side Effects

≥10%Very Common

Adverse Effect	Incidence	Clinical Note
Hyperuricemia (asymptomatic)	43–100%	Nearly universal at therapeutic doses; caused by pyrazinoic acid inhibiting renal tubular urate secretion. Usually asymptomatic and reversible on discontinuation. Does not require treatment unless symptomatic gout develops.
Arthralgia / myalgia	~20–40%	Non-gouty joint pain is common, especially with daily dosing; usually mild and manageable with NSAIDs. Distinguish from true gout by absence of monosodium urate crystals.

1–10%Common

Adverse Effect	Incidence	Clinical Note
Nausea / vomiting / anorexia	1–5%	GI intolerance may overlap with symptoms from other TB drugs in the regimen
Hepatotoxicity (elevated transaminases)	~4–6%	Dose-related; can appear at any time during the 2-month course. PZA is considered the most hepatotoxic of the first-line TB drugs at a population level.
Gout (acute gouty arthritis)	~1–5%	Secondary to hyperuricemia; more likely in patients with pre-existing gout or renal impairment. Manage with NSAIDs or colchicine; avoid allopurinol acutely.
Rash / urticaria / pruritus	1–3%	Hypersensitivity reaction; discontinue if severe

SeriousSerious (Regardless of Frequency)

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Severe hepatitis / fulminant liver failure	~1–2% (in combination regimens)	Any time during 2-month course; may occur early	Discontinue immediately if ALT >3× ULN with symptoms or >5× ULN without symptoms. PZA was identified as the principal hepatotoxin in the now-abandoned 2-month RIF+PZA LTBI regimen.
Thrombocytopenia	Rare	Variable	Check CBC urgently; discontinue if confirmed
Sideroblastic anemia	Rare	Weeks	Discontinue; consider pyridoxine supplementation; haematology referral
Interstitial nephritis	Rare	Variable	Discontinue; renal consultation; supportive care
Photosensitivity	Rare	Days to weeks of sun exposure	Sun protection; consider discontinuation if severe

DiscontinuationDiscontinuation Rates

Standard 2-Month Course (in Multi-Drug Regimen)

<5%

Top reasons: Hepatotoxicity, GI intolerance, rash. PZA is routinely discontinued after 2 months as planned.

Abandoned 2-Month RIF+PZA LTBI Regimen

Unacceptable

Context: This regimen was abandoned after reports of fatal hepatotoxicity. The CDC and ATS no longer recommend RIF+PZA for LTBI.

Reason for Discontinuation	Incidence	Context
Hepatotoxicity	~1–3%	Usually occurs within the 2-month course; attribution can be difficult in multi-drug regimens
Intolerable arthralgia / gout	<1%	Rarely requires discontinuation; usually manageable with analgesics

Managing Hyperuricemia

Asymptomatic hyperuricemia does not require treatment or PZA discontinuation. If acute gouty arthritis develops, manage with NSAIDs or colchicine. Allopurinol or febuxostat can be used if gout is recurrent, but they may have limited efficacy against PZA-induced hyperuricemia because the primary mechanism involves inhibition of renal urate secretion rather than overproduction. Uric acid levels return to baseline within weeks of PZA discontinuation at the end of the 2-month intensive phase.

Int

Drug Interactions

Pyrazinamide has a relatively narrow drug interaction profile compared to rifampin or isoniazid. It is not a significant CYP450 inducer or inhibitor. The principal interactions relate to its effects on uric acid metabolism and additive hepatotoxicity with other hepatotoxic agents.

MajorRifampin (2-month LTBI regimen)

MechanismAdditive / synergistic hepatotoxicity

EffectUnacceptably high rate of severe and fatal hepatitis when used as a 2-month regimen for LTBI

ManagementThis 2-drug LTBI regimen (RIF+PZA) is no longer recommended by the CDC or ATS. PZA+RIF remains acceptable as part of multi-drug active TB treatment for the standard 2-month intensive phase.

CDC MMWR 2003

ModerateProbenecid

MechanismPZA reduces the uricosuric effect of probenecid

EffectLoss of probenecid’s ability to lower uric acid; worsening hyperuricemia

ManagementAvoid probenecid during PZA therapy; use alternative urate-lowering agent if needed

FDA PI

ModerateCyclosporine

MechanismPZA may decrease cyclosporine plasma levels by unknown mechanism

EffectRisk of sub-therapeutic immunosuppression

ManagementMonitor cyclosporine levels closely; adjust dose as needed

Case report

MinorUrine Ketone Tests (Acetest / Ketostix)

MechanismPZA produces a pink-brown colour reaction with nitroprusside-based tests

EffectFalse-positive urine ketone results

ManagementUse alternative ketone testing methods during PZA therapy

FDA PI

Mon

Monitoring

Hepatic Enzymes (ALT, AST)Baseline; every 2–4 weeks during PZA therapy
RoutinePZA is the most hepatotoxic first-line TB drug. Obtain baseline LFTs for all patients. Patients with pre-existing liver disease, alcohol use, or HIV should have LFTs checked every 2 weeks during the 2-month course. Hold all hepatotoxic TB drugs if ALT >3× ULN with symptoms or >5× ULN without symptoms.
Serum Uric AcidBaseline; periodically during therapy
RoutineHyperuricemia is expected in nearly all patients. Routine monitoring allows early detection of extreme elevations. Clinical intervention is only needed if symptomatic gout develops. Levels normalise after PZA discontinuation.
Clinical Symptom ReviewMonthly (at minimum)
RoutineAsk about anorexia, nausea, vomiting, dark urine, jaundice, abdominal pain, joint pain, and rash at each visit.
Joint SymptomsAt each visit
Trigger-basedDistinguish between PZA-associated non-gouty arthralgia (common, mild, bilateral) and acute gout (sudden, severe, monoarticular). If gout is suspected, aspirate joint for crystal analysis when feasible.
Sputum CulturesBaseline and monthly until conversion
RoutineConfirm susceptibility including PZA susceptibility testing. Persistent culture positivity at 2 months warrants reassessment.

Contraindications & Cautions

Absolute Contraindications

Severe hepatic damage (FDA PI)
Known hypersensitivity to pyrazinamide
Acute gout (FDA PI)

Relative Contraindications (Specialist Input Recommended)

Chronic liver disease or active hepatitis: Use only under close supervision with frequent LFT monitoring if PZA is essential to the regimen
History of gout: Risk of flare; consider prophylactic colchicine or NSAID; ensure uric acid monitoring
Concurrent hepatotoxic drugs: Additive liver toxicity risk with isoniazid, rifampin, alcohol, methotrexate
Pregnancy: ATS/CDC/IDSA state that routine use is not recommended in pregnancy, but benefits may outweigh unquantified risks in some situations

Use with Caution

Renal impairment: Select doses at the lower end of the range; administer post-dialysis in ESRD
Elderly patients: Start at low end of dosing range; higher risk of hepatotoxicity and hyperuricemia complications
Diabetes mellitus: PZA may interfere with urine ketone testing (Acetest/Ketostix); use alternative methods
Porphyria: Rare exacerbation has been reported

FDA Warning Hepatotoxicity

Hepatotoxicity is the principal adverse effect of pyrazinamide. It appears to be dose-related and may occur at any time during therapy. Patients should have baseline hepatic enzyme determinations before initiating PZA. Those with pre-existing liver disease or increased risk of drug-related hepatitis (including alcohol users) should receive frequent liver function monitoring. Discontinue PZA if evidence of significant hepatic damage develops.

Patient Counselling

Purpose of Therapy

Pyrazinamide is one of four antibiotics used together to treat tuberculosis. It works best in the first 2 months of treatment by killing TB bacteria that are hiding inside your cells. After 2 months, your doctor will stop pyrazinamide but you will continue taking other TB medicines for several more months.

How to Take

Take pyrazinamide once daily with or without food, as directed by your doctor. Swallow the tablets whole with water. Complete the full 2-month course even if you feel better.

Liver Problems

Tell patientLiver damage is the most serious risk. Avoid alcohol during treatment. Attend all blood test appointments so your doctor can monitor your liver.

Call prescriberImmediately if you develop loss of appetite, nausea that does not go away, vomiting, dark urine, yellowing of eyes or skin, abdominal pain, or unusual tiredness.

Joint Pain & Gout

Tell patientJoint aches are common during pyrazinamide treatment because the drug raises uric acid levels. Mild joint pain can usually be managed with over-the-counter pain relievers. Stay well hydrated.

Call prescriberIf you develop sudden severe pain, redness, or swelling in a single joint (especially the big toe, ankle, or knee) — this may be a gout attack that needs specific treatment.

Stomach Upset

Tell patientNausea, vomiting, and loss of appetite can occur. Taking pyrazinamide with food may help.

Call prescriberIf vomiting is persistent and prevents you from keeping doses down, or if abdominal pain is severe.

Skin & Sun Sensitivity

Tell patientRarely, pyrazinamide can make your skin more sensitive to sunlight. Use sunscreen and protective clothing while taking this medicine.

Call prescriberIf you develop a rash, hives, or blistering skin reaction.

Ref

Sources

Regulatory (PI / SmPC)

Pyrazinamide Tablets, USP prescribing information. Various manufacturers. Drugs.com PIPrimary regulatory source for approved indications, dosing, contraindications, adverse reactions, and PK data used throughout this monograph.
DailyMed. Pyrazinamide tablet — drug label information. National Library of Medicine. DailyMedSupplementary FDA label source for generic pyrazinamide formulations.

Key Clinical Trials & Systematic Reviews

Pasipanodya JG, Gumbo T. Clinical and toxicodynamic evidence that high-dose pyrazinamide is not more hepatotoxic than the low doses currently used. Antimicrob Agents Chemother. 2010;54(7):2847–2854. DOIMeta-analysis and pharmacodynamic study demonstrating that PZA hepatotoxicity rates are similar across dose ranges, and arthralgia is dose-dependent.
Jasmer RM, Saukkonen JJ, Blumberg HM, et al. Short-course rifampin and pyrazinamide compared with isoniazid for latent tuberculosis infection. Ann Intern Med. 2002;137(8):640–647. DOIStudy contributing to the evidence base that led to withdrawal of the 2-month RIF+PZA LTBI regimen due to unacceptable hepatotoxicity.

Guidelines

Nahid P, Dorman SE, Alipanah N, et al. Official ATS/CDC/IDSA clinical practice guidelines: treatment of drug-susceptible tuberculosis. Clin Infect Dis. 2016;63(7):e147–e195. DOIComprehensive active TB treatment guidelines providing weight-band dosing tables for PZA in daily and intermittent regimens.
Saukkonen JJ, Cohn DL, Jasmer RM, et al. An official ATS statement: hepatotoxicity of antituberculosis therapy. Am J Respir Crit Care Med. 2006;174(8):935–952. DOIATS consensus on monitoring, risk factors, and management of anti-TB hepatotoxicity, including PZA-specific guidance.
CDC. Update: Fatal and severe liver injuries associated with rifampin and pyrazinamide for latent tuberculosis infection. MMWR. 2001;50(34):733–735. CDCCDC safety alert documenting fatal hepatitis cases that led to withdrawal of the 2-month RIF+PZA LTBI regimen.

Mechanistic / Basic Science

Zhang Y, Mitchison D. The curious characteristics of pyrazinamide: a review. Int J Tuberc Lung Dis. 2003;7(1):6–21. PubMedComprehensive review of PZA’s unique mechanism of action in acidic environments and the role of pncA mutations in resistance.
LiverTox: Clinical and Research Information on Drug-Induced Liver Injury. Pyrazinamide. NIDDK, 2020. NCBINIH resource on PZA hepatotoxicity patterns, severity spectrum, and comparison to other first-line TB drugs.

Pharmacokinetics / Special Populations

Savic RM, Weiner M, Mac Kenzie WR, et al. Pyrazinamide safety, efficacy, and dosing for treating drug-susceptible pulmonary tuberculosis. Am J Respir Crit Care Med. 2024. DOIPhase 3 PK/PD analysis from S31/A5349 evaluating PZA exposure-response relationships and proposing optimised dosing strategies.
Stamathakis G, Montes C, Trouvin JH, et al. Pyrazinamide and pyrazinoic acid pharmacokinetics in patients with chronic renal failure. Clin Nephrol. 1988;30(4):230–234. PubMedPK study in renal impairment supporting post-dialysis dosing recommendations for ESRD patients.