Pyrazinamide (PZA) is used in the treatment of tuberculosis. Pyrazinamide is considered a first-line agent when used in addition to isoniazid, ethambutol, rifampin, and/or streptomycin for treatment of isoniazid-susceptible organisms and when resistance to isoniazid or rifampin has been confirmed. Pyrazinamide appears to be less toxic and more effective than other antitubercular agents including aminosalicylic acid, capreomycin, cycloserine, ethionamide, and kanamycin; however, liver function must be carefully monitored during PZA use. While the drug has been used in combination with a rifamycin as an alternative for latent tuberculosis, the Centers for Disease Control and Prevention (CDC) and the American Thoracic Society (ATS) no longer recommend the 2-month regimen of rifampin plus PZA for this indication (see Contraindications/Precautions). Pyrazinamide was approved by the FDA in 1955.
General Administration Information
For storage information, see the specific product information within the How Supplied section.
-Directly observed therapy (DOT) is recommended for all children, adolescents, and adults living with HIV and any regimen consisting of intermittent therapy.
Route-Specific Administration
Oral Administration
Extemporaneous Compounding-Oral
NOTE: Extemporaneously compounded oral pyrazinamide solution is not FDA-approved.
Oral suspension using simple syrup*
-Crush 140 pyrazinamide 500 mg tablets and mix with a small amount of simple syrup.
-Transfer contents to a graduate and add simple syrup to prepare 700 mL of suspension.
-Repeat to yield 1.4 L of pyrazinamide 100 mg/mL in simple syrup.
-Storage: The suspension was stable for 60 days in glass or plastic bottles at 4 or 25 degrees C.
Oral suspension using methylcellulose and simple syrup*
-Crush 200 pyrazinamide 500 mg tablets and mix with a suspension containing 500 mL of 1% methylcellulose (25.5 g Citrucel powder mixed with 500 mL of purified water) and 500 mL simple syrup.
-Crush 140 pyrazinamide 500 mg tablets and mix with a suspension containing 350 mL of 1% methylcellulose and 350 mL of simple syrup.
-Add the suspensions together to yield 1.7 L of pyrazinamide 100 mg/mL in 0.5% methylcellulose and simple syrup.
-Storage: The suspension was stable for 60 days in glass or plastic bottles at 4 or 25 degrees C.
Oral suspension using Ora-Sweet and Ora-Plus*
-Prepare pyrazinamide in a 1:1 mixture of Ora-Sweet and Ora-Plus to a concentration of 10 mg/mL.
-Storage: The suspension was stable for 60 days in plastic bottles at 5 or 25 degrees C.
Oral suspension using Ora-Sweet SF and Ora-Plus*
-Prepare pyrazinamide in a 1:1 mixture of Ora-Sweet SF and Ora-Plus to a concentration of 10 mg/mL.
-Storage: The suspension was stable for 60 days in plastic bottles at 5 or 25 degrees C.
Oral suspension using cherry syrup*
-Prepare pyrazinamide in cherry syrup (cherry syrup concentrate diluted 1:4 with simple syrup) to a concentration of 10 mg/mL.
-Storage: The suspension was stable for 60 days in plastic bottles at 5 or 25 degrees C.
Hepatotoxicity (drug-induced hepatitis) is the most common serious adverse reaction to pyrazinamide. It appears to be dose-related and may appear at any time during therapy. Elevated hepatic enzymes or bilirubin (hyperbilirubinemia) may occur. Discontinue pyrazinamide if signs of hepatocellular damage occur. Most combination therapy for active TB disease includes more than 1 agent that may contribute to hepatotoxicity.
Mild arthralgia and myalgia have been reported frequently during pyrazinamide treatment. Nongouty arthralgia has been reported and appears to occur secondary to hyperuricemia caused by inhibition of urate excretion. This reaction is often asymptomatic; however, if acute gout or acute gouty arthritis develops, pyrazinamide should be promptly discontinued.
In rare instances, hematologic complications, such as thrombocytopenia, porphyria, and sideroblastic anemia with erythroid hyperplasia, have occurred during pyrazinamide therapy. Additionally, vacuolation of erythrocytes, increased serum iron concentrations, and adverse effects on blood clotting mechanisms have been rarely reported.
Hypersensitivity reactions including rash (unspecified), urticaria, and pruritus have been reported with pyrazinamide therapy. Angioedema has been reported rarely. Acne or acneiform rash and photosensitivity have also been reported rarely.
Dysuria and interstitial nephritis have been reported rarely during pyrazinamide therapy.
Gastrointestinal disturbances, including nausea, vomiting, and anorexia, have been reported with the use of pyrazinamide.
Pyrazinamide is contraindicated in persons with known pyrazinamide hypersensitivity.
Pyrazinamide is contraindicated in persons with severe hepatic disease. Assess hepatic function at baseline and periodically. Follow patients with preexisting liver disease or those at increased risk for drug-related hepatitis (e.g., alcoholism) closely. Discontinue pyrazinamide if signs of hepatocellular damage occur. Most combination therapy for active TB disease includes more than 1 agent that may contribute to hepatotoxicity.
Pyrazinamide is contraindicated in persons with acute gout. Obtain baseline serum uric acid concentration before starting pyrazinamide therapy. Discontinue pyrazinamide if hyperuricemia accompanied by acute gouty arthritis occurs. Pyrazinamide inhibits renal excretion of urates, frequently resulting in hyperuricemia, which is usually asymptomatic.
Use pyrazinamide with caution in patients with diabetes mellitus as management may be more difficult. Also, pyrazinamide may cause laboratory test interference. Pyrazinamide has been reported to interfere with Acetest and Ketostix, which are urine ketone tests, to produce a pink-brown color.
Optimal pyrazinamide dosing for obesity is not established. Pyrazinamide dosing is based on lean body weight, in general.
Do not treat persons with tuberculosis (TB) and human immunodeficiency virus (HIV) infection and/or acquired immunodeficiency syndrome (AIDS) with intermittent (i.e., twice weekly or 3 days/week) TB treatment regimens to avoid recurrent disease and the emergence of drug resistance.
Use pyrazinamide during pregnancy only if clearly needed. It is not known whether pyrazinamide can cause fetal harm when administered to pregnant women or if it can affect reproduction capacity. Animal reproduction studies have not been conducted with pyrazinamide. Pyrazinamide has been used extensively in high-burden countries for many years. Tuberculosis guidelines suggest evaluating pyrazinamide use on a case-by-case basis. In pregnant women with tuberculosis and HIV or extrapulmonary or severe tuberculosis, it is more beneficial to include pyrazinamide in the treatment regimen than to not include pyrazinamide.
Use pyrazinamide with caution in breast-feeding mothers, taking into account the risk-benefit of this therapy. Pyrazinamide has been found in small amounts in breast milk. Tuberculosis guidelines encourage breast-feeding for women who are noninfectious and being treated with first-line tuberculosis agents, such as pyrazinamide, as the small concentrations of these drugs measured in breast milk have not been reported to produce toxic effects in the nursing infant.
Per the manufacturer, this drug has been shown to be active against most strains of the following microorganisms either in vitro and/or in clinical infections: Mycobacterium tuberculosis
NOTE: The safety and effectiveness in treating clinical infections due to organisms with in vitro data only have not been established in adequate and well-controlled clinical trials.
For the treatment of drug-susceptible tuberculosis infection as part of combination therapy:
-for the treatment of drug-susceptible tuberculosis infection in persons without HIV as part of traditional combination therapy:
Oral dosage:
Adults weighing more than 90 kg (lean body weight): 15 to 30 mg/kg/dose (Max: 3 g/dose) PO once daily, or alternatively, 50 to 75 mg/kg/dose PO twice weekly. Daily dosing is preferred. Pyrazinamide is generally recommended as part of the initial 2-month intensive phase as first-line therapy.
Adults weighing 76 to 90 kg (lean body weight): 2 g PO once daily or 5 days/week, or alternatively, 3 g PO 3 days/week or 4 g PO twice weekly. Alternatively, 20 to 30 mg/kg/dose PO once daily or 30 to 40 mg/kg/dose PO 3 days/week. The FDA-approved dosage is 15 to 30 mg/kg/dose PO once daily or 50 to 75 mg/kg/dose PO twice weekly. Daily dosing is preferred and is defined as 5- or 7 days/week. Pyrazinamide is generally recommended as part of the initial 2-month intensive phase as first-line therapy.
Adults weighing 56 to 75 kg (lean body weight): 1.5 g PO once daily or 5 days/week, or alternatively, 2.5 g PO 3 days/week or 3 g PO twice weekly. Alternatively, 20 to 30 mg/kg/dose PO once daily or 30 to 40 mg/kg/dose PO 3 days/week. The FDA-approved dosage is 15 to 30 mg/kg/dose PO once daily or 50 to 75 mg/kg/dose PO twice weekly. Daily dosing is preferred and is defined as 5- or 7 days/week. Pyrazinamide is generally recommended as part of the initial 2-month intensive phase of treatment as first-line therapy.
Adults weighing 40 to 55 kg (lean body weight): 1 g PO once daily or 5 days/week, or alternatively, 1.5 g PO 3 days/week or 2 g PO twice weekly. Alternatively, 20 to 30 mg/kg/dose PO once daily or 30 to 40 mg/kg/dose PO 3 days/week. The FDA-approved dosage is 15 to 30 mg/kg/dose PO once daily or 50 to 75 mg/kg/dose PO twice weekly. Daily dosing is preferred and is defined as 5- or 7 days/week. Pyrazinamide is generally recommended as part of the initial 2-month intensive phase as first-line therapy.
Infants, Children, and Adolescents: 30 to 40 mg/kg/dose (lean body weight) (Max: 2 g/dose) PO once daily or 5 days/week, or alternatively, 50 mg/kg/dose (lean body weight) PO 3 days/week (Max: 3 g/dose) or twice weekly (Max: 4 g/dose). The FDA-approved dosage is 15 to 30 mg/kg/dose (lean body weight) PO once daily (Max: 3 g/day) or 50 to 75 mg/kg/dose (lean body weight) PO twice weekly. Daily dosing is preferred and is defined as 5- or 7 days/week. Pyrazinamide is generally recommended as part of the initial 2-month intensive phase as first-line therapy.
Neonates*: 20 to 40 mg/kg/dose PO once daily. Although tuberculosis is rare in neonates, congenital and postnatal cases have been successfully treated with antitubercular agents. Pyrazinamide is generally recommended as part of the initial 2-month intensive phase as first-line therapy.
-for the treatment of drug-susceptible tuberculosis infection in persons with HIV as part of traditional combination therapy:
Oral dosage:
Adults weighing more than 90 kg (lean body weight): 2 g PO once daily. Monitor for response and consider therapeutic drug monitoring to assure dosing adequacy. The FDA-approved dosage is 15 to 30 mg/kg/dose PO once daily (Max: 3 g/day) or 50 to 75 mg/kg/dose PO twice weekly. Pyrazinamide is generally recommended as part of the initial 2-month intensive phase as first-line therapy.
Adults weighing 76 to 90 kg (lean body weight): 2 g PO once daily or 5 days/week. The FDA-approved dosage is 15 to 30 mg/kg/dose PO once daily or 50 to 75 mg/kg/dose PO twice weekly. Daily dosing is defined as 5- or 7 days/week. Pyrazinamide is generally recommended as part of the initial 2-month intensive phase of treatment as first-line therapy.
Adults weighing 56 to 75 kg (lean body weight): 1.5 g PO once daily or 5 days/week. The FDA-approved dosage is 15 to 30 mg/kg/dose PO once daily or 50 to 75 mg/kg/dose PO twice weekly. Daily dosing is defined as 5- or 7 days/week. Pyrazinamide is generally recommended as part of the initial 2-month intensive phase as first-line therapy.
Adults weighing 40 to 55 kg (lean body weight): 1 g PO once daily or 5 days/week. The FDA-approved dosage is 15 to 30 mg/kg/dose PO once daily or 50 to 75 mg/kg/dose PO twice weekly. Daily dosing is defined as 5- or 7 days/week. Pyrazinamide is generally recommended as part of the initial 2-month intensive phase of treatment as first-line therapy.
Infants, Children, and Adolescents: 30 to 40 mg/kg/dose (lean body weight) (Max: 2 g/dose) PO once daily or 5 days/week. The FDA-approved dosage is 15 to 30 mg/kg/dose (lean body weight) PO once daily (Max: 3 g/day) or 50 to 75 mg/kg/dose (lean body weight) PO twice weekly. Daily dosing is defined as 5- or 7 days/week. Pyrazinamide is generally recommended as part of the initial 2-month intensive phase as first-line therapy.
Neonates*: 20 to 40 mg/kg/dose PO once daily. Although tuberculosis is rare in neonates, congenital and postnatal cases have been successfully treated with antitubercular agents. Pyrazinamide is generally recommended as part of the initial 2-month intensive phase as first-line therapy.
-for the treatment of drug-susceptible pulmonary tuberculosis infection as part of shortened combination therapy with isoniazid, moxifloxacin, and rifapentine:
Oral dosage:
Adults weighing 76 kg or more: 2 g PO once daily for 8 weeks. In persons living with HIV, this regimen can be used in persons who have a CD4 count of 100 cells/mm3 or more and are receiving or planning to initiate efavirenz as part of their antiretroviral therapy in the absence of any other known drug-interactions.
Adults weighing 55 to 75 kg: 1.5 g PO once daily for 8 weeks. In persons living with HIV, this regimen can be used in persons who have a CD4 count of 100 cells/mm3 or more and are receiving or planning to initiate efavirenz as part of their antiretroviral therapy in the absence of any other known drug-interactions.
Adults weighing 40 to 54 kg: 1 g PO once daily for 8 weeks. In persons living with HIV, this regimen can be used in persons who have a CD4 count of 100 cells/mm3 or more and are receiving or planning to initiate efavirenz as part of their antiretroviral therapy in the absence of any other known drug-interactions.
Children and Adolescents 12 to 17 years weighing 76 kg or more: 2 g PO once daily for 8 weeks. In persons living with HIV, this regimen can be used in persons who have a CD4 count of 100 cells/mm3 or more and are receiving or planning to initiate efavirenz as part of their antiretroviral therapy in the absence of any other known drug-interactions.
Children and Adolescents 12 to 17 years weighing 55 to 75 kg: 1.5 g PO once daily for 8 weeks. In persons living with HIV, this regimen can be used in persons who have a CD4 count of 100 cells/mm3 or more and are receiving or planning to initiate efavirenz as part of their antiretroviral therapy in the absence of any other known drug-interactions.
Children and Adolescents 12 to 17 years weighing 40 to 54 kg: 1 g PO once daily for 8 weeks. In persons living with HIV, this regimen can be used in persons who have a CD4 count of 100 cells/mm3 or more and are receiving or planning to initiate efavirenz as part of their antiretroviral therapy in the absence of any other known drug-interactions.
-for the treatment of CNS-related tuberculosis as part of shortened intensive combination therapy*:
Oral dosage:
Infants, Children, and Adolescents: 35 to 45 mg/kg/dose PO once daily.
For the treatment of drug-resistant tuberculosis infection as part of combination therapy:
Oral dosage:
Adults: 20 to 40 mg/kg/dose (lean body weight) PO once daily. The FDA-approved dosage is 15 to 30 mg/kg/dose (lean body weight) PO once daily (Max: 3 g/day) or 50 to 75 mg/kg/dose (lean body weight) PO twice weekly.
Infants, Children, and Adolescents: 30 to 40 mg/kg/dose (lean body weight) PO once daily. The FDA-approved dosage is 15 to 30 mg/kg/dose (lean body weight) PO once daily (Max: 3 g/day) or 50 to 75 mg/kg/dose (lean body weight) PO twice weekly.
Maximum Dosage Limits:
Dosing is based on lean body weight.
-Adults
30 mg/kg/dose (Max: 3 g/dose) PO once daily or 75 mg/kg/dose PO twice weekly are the FDA-approved maximum dosages. Other regimens and maximum dosages have been used off-label.
Weighing more than 90 kg: 30 mg/kg/dose (Max: 3 g/dose) PO once daily or 75 mg/kg/dose PO twice weekly.
Weighing 76 to 90 kg: 2 g PO once daily or 5 days/week, 3 g PO 3 days/week, or 4 g PO twice weekly.
Weighing 56 to 75 kg: 1.5 g PO once daily or 5 days/week, 2.5 g PO 3 days/week, or 3 g PO twice weekly.
Weighing 40 to 55 kg: 1 g PO once daily or 5 days/week, 1.5 g PO 3 days/week, or 2 g PO twice weekly.
-Geriatric
30 mg/kg/dose (Max: 3 g/dose) PO once daily or 75 mg/kg/dose PO twice weekly are the FDA-approved maximum dosages. Other regimens and maximum dosages have been used off-label.
Weighing more than 90 kg: 30 mg/kg/dose (Max: 3 g/dose) PO once daily or 75 mg/kg/dose PO twice weekly.
Weighing 76 to 90 kg: 2 g PO once daily or 5 days/week, 3 g PO 3 days/week, or 4 g PO twice weekly.
Weighing 56 to 75 kg: 1.5 g PO once daily or 5 days/week, 2.5 g PO 3 days/week, or 3 g PO twice weekly.
Weighing 40 to 55 kg: 1 g PO once daily or 5 days/week, 1.5 g PO 3 days/week, or 2 g PO twice weekly.
-Adolescents
30 mg/kg/dose (Max: 3 g/dose) PO once daily or 75 mg/kg/dose PO twice weekly are the FDA-approved maximum dosages. 40 mg/kg/dose (Max: 2 g/dose) PO once daily or 5 days/week or 50 mg/kg/dose PO 3 days/week (Max: 3 g/dose) or twice weekly (Max: 4 g/dose) have been used off-label.
-Children
30 mg/kg/dose (Max: 3 g/dose) PO once daily or 75 mg/kg/dose PO twice weekly are the FDA-approved maximum dosages. 40 mg/kg/dose (Max: 2 g/dose) PO once daily or 5 days/week or 50 mg/kg/dose PO 3 days/week (Max: 3 g/dose) or twice weekly (Max: 4 g/dose) have been used off-label.
-Infants
30 mg/kg/dose (Max: 3 g/dose) PO once daily or 75 mg/kg/dose PO twice weekly are the FDA-approved maximum dosages. 40 mg/kg/dose (Max: 2 g/dose) PO once daily or 5 days/week or 50 mg/kg/dose PO 3 days/week (Max: 3 g/dose) or twice weekly (Max: 4 g/dose) have been used off-label.
-Neonates
Safety and efficacy have not been established. 40 mg/kg/dose PO once daily has been used off-label.
Patients with Hepatic Impairment Dosing
Pyrazinamide is contraindicated in patients with severe hepatic disease.
Patients with Renal Impairment Dosing
It may be prudent to select doses at the low end of the dosing range. Dosing is based on lean body weight.
Adult patients*
CrCl 30 mL/minute or more: No dosage adjustment needed.
CrCl less than 30 mL/minute: 25 to 40 mg/kg/dose PO 3 days/week.
Pediatric patients*
GFR 30 mL/minute/1.73 m2 or more: No dosage adjustment needed.
GFR less than 30 mL/minute/1.73 m2: 30 to 40 mg/kg/dose PO 3 days/week.
Intermittent hemodialysis*
Adult patients
25 to 35 mg/kg/dose PO 3 days/week administered after hemodialysis on dialysis days.
Pediatric patients
40 mg/kg/dose PO 3 days/week.
Peritoneal dialysis*
Adult patients
No dosage adjustment is needed.
Pediatric patients
40 mg/kg/dose PO 3 days/week.
Continuous renal replacement therapy (CRRT)*
NOTE: Various CRRT modalities include continuous venovenous hemofiltration (CVVH), continuous venovenous hemodialysis (CVVHD), continuous venovenous hemodiafiltration (CVVHDF), continuous venovenous high-flux hemodialysis (CVVHFD), continuous arteriovenous hemofiltration (CAVH), continuous arteriovenous hemodialysis (CAVHD), and continuous arteriovenous hemodiafiltration (CAVHDF). Dosing should take into consideration patient-specific factors (e.g., intrinsic renal function), type of infection, the duration of renal replacement therapy, the effluent flow rate, and the replacement solution administered.
Adult patients
No dosage adjustment is needed.
Pediatric patients
Avoid in patients with a GFR less than 30 mL/minute/1.73m3.
*non-FDA-approved indication
Allopurinol: (Minor) Because pyrazinamide, PZA can increase serum uric acid levels and precipitate gouty attacks, the dosages of antigout agents, including allopurinol, may need to be adjusted.
Aminosalicylate sodium, Aminosalicylic acid: (Moderate) Careful monitoring of hepatic function is recommended with the concurrent use of pyrazinamide, PZA and aminosalicylate sodium, aminosalicylic acid. Each drug has the potential to cause hepatotoxicity, and hepatotoxicity risk may be increased with concomitant use. These drugs may be used together for the treatment of active tuberculosis (TB) infection, and patients should also be assessed for additional risk factors for hepatotoxicity, such as other hepatotoxic drugs, alcohol use, and underlying hepatic disease. Any adverse event leading to hospitalization or death should be reported to local or state health departments as well as the FDA MedWatch program.
Ethambutol: (Moderate) Careful monitoring of hepatic function is recommended with the concurrent use of pyrazinamide, PZA and ethambutol. Each drug has the potential to cause hepatotoxicity, and hepatotoxicity risk may be increased with concomitant use. These drugs are often used together for the treatment of active tuberculosis (TB) infection, and patients should also be assessed for additional risk factors for hepatotoxicity, such as other hepatotoxic drugs, alcohol use, and underlying hepatic disease. Any adverse event leading to hospitalization or death should be reported to local or state health departments as well as the FDA MedWatch program.
Ethanol: (Major) Pyrazinamide, PZA is associated with dose-related hepatoxicity. Daily use of alcohol while receiving pyrazinamide, PZA increases the risk of drug-induced hepatitis. Liver-function tests should be conducted prior to and every 2-4 weeks during treatment in patients who consume alcohol routinely while receiving pyrazinamide therapy.
Ethionamide: (Moderate) Careful monitoring of hepatic function is recommended with the concurrent use of ethionamide and pyrazinamide, PZA. Each drug has the potential to cause hepatotoxicity, and hepatotoxicity risk may be increased with concomitant use. These drugs may be used together for the treatment of active tuberculosis (TB) infection, and patients should also be assessed for additional risk factors for hepatotoxicity, such as other hepatotoxic drugs, alcohol use, and underlying hepatic disease. Any adverse event leading to hospitalization or death should be reported to local or state health departments as well as the FDA MedWatch program.
Isoniazid, INH: (Moderate) Careful monitoring of hepatic function is recommended with the concurrent use of pyrazinamide, PZA and isoniazid, INH. Each drug has the potential to cause hepatotoxicity, and hepatotoxicity risk may be increased with concomitant use. These drugs are often used together for the treatment of active tuberculosis (TB) infection, and patients should also be assessed for additional risk factors for hepatotoxicity, such as other hepatotoxic drugs, alcohol use, and underlying hepatic disease. Any adverse event leading to hospitalization or death should be reported to local or state health departments as well as the FDA MedWatch program.
Isoniazid, INH; Pyrazinamide, PZA; Rifampin: (Moderate) Careful monitoring of hepatic function is recommended with the concurrent use of pyrazinamide, PZA and isoniazid, INH. Each drug has the potential to cause hepatotoxicity, and hepatotoxicity risk may be increased with concomitant use. These drugs are often used together for the treatment of active tuberculosis (TB) infection, and patients should also be assessed for additional risk factors for hepatotoxicity, such as other hepatotoxic drugs, alcohol use, and underlying hepatic disease. Any adverse event leading to hospitalization or death should be reported to local or state health departments as well as the FDA MedWatch program. (Moderate) Careful monitoring of hepatic function is recommended with the concurrent use of rifampin and pyrazinamide, PZA. Each drug has the potential to cause hepatotoxicity, and hepatotoxicity risk may be increased with concomitant use. These drugs are often used together for the treatment of active tuberculosis (TB) infection, and patients should also be assessed for additional risk factors for hepatotoxicity, such as other hepatotoxic drugs, alcohol use, and underlying hepatic disease. The use of the 2-month rifampin plus pyrazinamide latent tuberculosis infection (LTBI) regimen should no longer be offered due to the known increased risk of severe liver injury and death. Any adverse event leading to hospitalization or death should be reported to local or state health departments as well as the FDA MedWatch program.
Isoniazid, INH; Rifampin: (Moderate) Careful monitoring of hepatic function is recommended with the concurrent use of pyrazinamide, PZA and isoniazid, INH. Each drug has the potential to cause hepatotoxicity, and hepatotoxicity risk may be increased with concomitant use. These drugs are often used together for the treatment of active tuberculosis (TB) infection, and patients should also be assessed for additional risk factors for hepatotoxicity, such as other hepatotoxic drugs, alcohol use, and underlying hepatic disease. Any adverse event leading to hospitalization or death should be reported to local or state health departments as well as the FDA MedWatch program. (Moderate) Careful monitoring of hepatic function is recommended with the concurrent use of rifampin and pyrazinamide, PZA. Each drug has the potential to cause hepatotoxicity, and hepatotoxicity risk may be increased with concomitant use. These drugs are often used together for the treatment of active tuberculosis (TB) infection, and patients should also be assessed for additional risk factors for hepatotoxicity, such as other hepatotoxic drugs, alcohol use, and underlying hepatic disease. The use of the 2-month rifampin plus pyrazinamide latent tuberculosis infection (LTBI) regimen should no longer be offered due to the known increased risk of severe liver injury and death. Any adverse event leading to hospitalization or death should be reported to local or state health departments as well as the FDA MedWatch program.
Omeprazole; Amoxicillin; Rifabutin: (Moderate) Careful monitoring of hepatic function is recommended with the concurrent use of rifabutin and pyrazinamide, PZA. Each drug has the potential to cause hepatotoxicity, and hepatotoxicity risk may be increased with concomitant use. These drugs are often used together for the treatment of active tuberculosis (TB) infection, and patients should also be assessed for additional risk factors for hepatotoxicity, such as other hepatotoxic drugs, alcohol use, and underlying hepatic disease. Any adverse event leading to hospitalization or death should be reported to local or state health departments as well as the FDA MedWatch program.
Pexidartinib: (Moderate) Monitor for evidence of hepatotoxicity if pexidartinib is coadministered with pyrazinamide. Avoid concurrent use in patients with increased serum transaminases, total bilirubin, or direct bilirubin (more than ULN) or active liver or biliary tract disease.
Pretomanid: (Major) Avoid coadministration of pretomanid with pyrazinamide, especially in patients with impaired hepatic function, due to increased risk for hepatotoxicity. Monitor for evidence of hepatotoxicity if coadministration is necessary. If new or worsening hepatic dysfunction occurs, discontinue hepatotoxic medications.
Probenecid: (Minor) Because pyrazinamide can increase serum uric acid levels and precipitate gouty attacks, the dosages of antigout agents, including probenecid, may need to be adjusted.
Probenecid; Colchicine: (Minor) Because pyrazinamide can increase serum uric acid levels and precipitate gouty attacks, the dosages of antigout agents, including probenecid, may need to be adjusted.
Rifabutin: (Moderate) Careful monitoring of hepatic function is recommended with the concurrent use of rifabutin and pyrazinamide, PZA. Each drug has the potential to cause hepatotoxicity, and hepatotoxicity risk may be increased with concomitant use. These drugs are often used together for the treatment of active tuberculosis (TB) infection, and patients should also be assessed for additional risk factors for hepatotoxicity, such as other hepatotoxic drugs, alcohol use, and underlying hepatic disease. Any adverse event leading to hospitalization or death should be reported to local or state health departments as well as the FDA MedWatch program.
Rifampin: (Moderate) Careful monitoring of hepatic function is recommended with the concurrent use of rifampin and pyrazinamide, PZA. Each drug has the potential to cause hepatotoxicity, and hepatotoxicity risk may be increased with concomitant use. These drugs are often used together for the treatment of active tuberculosis (TB) infection, and patients should also be assessed for additional risk factors for hepatotoxicity, such as other hepatotoxic drugs, alcohol use, and underlying hepatic disease. The use of the 2-month rifampin plus pyrazinamide latent tuberculosis infection (LTBI) regimen should no longer be offered due to the known increased risk of severe liver injury and death. Any adverse event leading to hospitalization or death should be reported to local or state health departments as well as the FDA MedWatch program.
Riluzole: (Moderate) Monitor for signs and symptoms of hepatic injury during coadministration of riluzole and pyrazinamide. Concomitant use may increase the risk for hepatotoxicity. Discontinue riluzole if clinical signs of liver dysfunction are present.
Pyrazinamide's exact mechanism of action is not known. Susceptible strains of M. tuberculosis release pyrazinamidase, which converts PZA to pyrazinoic acid (POA). Conversion of PZA to this active metabolite may be partially responsible for its activity. In vitro studies have demonstrated that POA decreases the pH below that which promotes the growth of M. tuberculosis. The mechanism of the parent compound has not been elucidated. Pyrazinamide exhibits bacteriocidal or bacteriostatic action, depending on the drug concentrations within the infected site and the susceptibility of the organism. Pyrazinamide exerts its most significant effect at intracelluar sites where M. tuberculosis replicates slowly, such as within macrophages. Studies indicate that PZA is most effective in the initial stages of treatment, which may be the result of diminished organism populations in macrophages early in therapy. Pyrazinamide also inhibits the tubular secretion of uric acid.
M. tuberculosis is the only organism susceptible to pyrazinamide.
Pharmacokinetics:
Pyrazinamide (PZA) is administered orally. PZA is widely distributed. It penetrates inflamed meninges to reach therapeutic levels in the CSF. It is unknown whether PZA crosses the placenta, but distribution into breast milk has been documented (see Contraindications). The plasma half-life is 9-10 hours. Pyrazinamide is hydrolyzed in the liver to pyrazinoic acid, its major active metabolite. Subsequently, pyrazinoic acid is hydroxylated to the main excretory compound. Pyrazinamide and its metabolites are excreted in the urine (70%), primarily via glomerular filtration.
-Route-Specific Pharmacokinetics
Oral Route
Pyrazinamide is rapidly absorbed from the GI tract. Peak serum levels are attained within 2 hours. Plasma levels of the major active metabolite peak within 4-8 hours.
-Special Populations
Renal Impairment
The plasma half-life of pyrazinamide may be increased to up to 26 hours in patients with renal disease.