allopurinol (Zyloprim, Aloprim)

Dosing and uses of Zyloprim, Aloprim (allopurinol)

• Adult
• Pediatric

 

Adult dosage forms and strengths

tablet

• 100mg
• 300mg

powder for injection

• 500mg/vial

 

Gout

Mild: 100 mg/day PO initially; increased weekly to 200-300 mg/day

Moderate to severe: 100 mg/day PO initially; increased weekly to 400-600 mg/day

 

Antineoplastic-Induced Hyperuricemia

PO: 600-800 mg divided q8-12hr, starting 1-2 days before chemotherapy

IV: 200-400 mg/m²/day; not to exceed 600 mg/m²/day; may administer as single infusion or in equally divided doses at 6, 8, 12 hr intervals beginning 1-2 days before chemotherapy

 

Dosing Considerations

Minimum PO dosage: 100-200 mg/day

Maximum PO dosage: 800 mg/day

 

Dosing Modifications

Renal impairment

• CrCl 10-20 mL/min: 200 mg/day
• CrCl 3-10 mL/min: 100 mg/day
• CrCl <3 mL/min: 100 mg/day at extended intervals

 

Pediatric dosage forms and strengths

tablet

• 100mg
• 300mg

powder for injection

• 500mg/vial

 

Hyperuricemia

10 mg/kg/day PO divided q12hr; not to exceed 600 mg/day

 

Antineoplastic-Induced Hyperuricemia

PO (<6 years): 150 mg/day divided q8hr

PO (6-10 years): 300 mg/day in single daily dose or divided q8hr

PO (>10 years): 600-800 mg/day, starting 1-2 days before chemotherapy

IV: 200 mg/m²/day initially, starting 1-2 days before chemotherapy

 

Zyloprim, Aloprim (allopurinol) adverse (side) effects

1-10%

Rash (1.5%)

Nausea (1.3%)

Renal failure (1.2%)

Vomiting (1.2%)

 

Frequency not defined

Amblyopia

Arthralgias

Blood dyscrasias

Bronchospasm

Cardiovascular abnormalities

Cataracts

Confusion

Decrease in libido

Dizziness

Ecchymosis

Electrolyte abnormalities

Epistaxis

Foot drop

Hematuria

Hepatotoxicity

Hypotonia

Iritis

Kidney function abnormality

Macular retinitis

Malaise

Neuritis

Pharyngitis

Pruritus

Skin edema

Stevens-Johnson syndrome

Sweating

Tinnitus

 

Warnings

Contraindications

Hypersensitivity to allopurinoL

 

Cautions

Discontinue at first sign of allergic reactions (first sign of rash, vasculitis, or Stevens-Johnson syndrome)

Myelosuppression reported; use caution when administering other drugs known to cause myelosuppression

Hepatotoxicity (reversible) reported

Not for treatment of asymptomatic hyperuricemia

Use with caution in renal impairment

Risk of hypersensitivity increased in patients treated with angiotensin-converting emzyme (ACE) inhibitors

When taken with amoxicillin or ampicillin, may increase risk of skin rash

During concomitant treatment, reduce dosages of azathioprine and mercaptopurine to 25-33% of usuaL

Risk of hypersensitivity may increase with concomitant administration of thiazides

Maintain fluid intake necessary to yield urine output of at least 2 L/day in adults

 

Pregnancy and lactation

Pregnancy category: C

Lactation: Agent is distributed into breast milk; use with caution

 

Pregnancy categories

A: Generally acceptable. Controlled studies in pregnant women show no evidence of fetal risk.

B: May be acceptable. Either animal studies show no risk but human studies not available or animal studies showed minor risks and human studies done and showed no risk.

C: Use with caution if benefits outweigh risks. Animal studies show risk and human studies not available or neither animal nor human studies done.

D: Use in LIFE-THREATENING emergencies when no safer drug available. Positive evidence of human fetal risk.

X: Do not use in pregnancy. Risks involved outweigh potential benefits. Safer alternatives exist.

NA: Information not available.

 

Pharmacology of Zyloprim, Aloprim (allopurinol)

Mechanism of action

Xanthine oxidase inhibitor; inhibits conversion of hypoxanthine to xanthine to uric acid; decreases production of uric acid without disrupting synthesis of vital purines

 

Pharmacokinetics

Bioavailability: 49-53%

Onset: 2-3 days

Peak plasma time: 0.5-2 hr

Time to peak effect: 7-14 days

 

Distribution

Protein bound: <1%

Vd: 1.6-2.4 L/kg

 

Metabolism

Metabolized in liver

Metabolites: Oxypurinol (active), allopurinol riboside (activity unknown)

 

Elimination

Half-life: Parent drug, 1-3 hr; active metabolite, 15-20 hr

Dialyzable: Yes (both hemodialysis and peritoneal dialysis)

Renal clearance: 30 mL/min

Total body clearance: 16 mL/min/kg

Excretion: Urine (80%), feces (10-20%)

 

Administration

IV Compatibilities

Y-site (partial list): Acyclovir, calcium gluconate, cefazolin, ceftriaxone, carboplatin, cisplatin, cyclophosphamide, dactinomycin, doxorubicin liposomal, fluorouracil, ifosfamide, mesna, metronidazole, mitoxantrone, morphine sulfate, potassium chloride, thiotepa, vancomycin

 

IV Incompatibities

Y-site: Amikacin, amphotericin B, carmustine, cefotaxime, chlorpromazine, cimetidine, clindamycin, cytarabine, dacarbazine, daunorubicin, diphenhydramine, doxorubicin, doxycycline, droperidol, floxuridine, gentamicin, haloperidol, hydroxyzine, idarubicin, imipenem-cilastatin, mechlorethamine, meperidine, methylprednisolone sodium succinate, metoclopramide, minocycline, nalbuphine, netilmicin, ondansetron, prochlorperazine, promethazine, sodium bicarbonate, streptozocin, tobramycin, vinorelbine

 

IV Preparation

Reconstitute with 25 mL SWI

Dilute to desired concentration with NS or D5W; do not use sodium bicarbonate-containing solutions; final concentration of ≤6 mg/mL is recommended

Store solution at 20-25°C (do not refrigerate), and use within 10 hours after reconstitution

 

IV Administration

In both adults and children, daily dose can be given as single infusion or in equally divided infusions q6hr, q8hr, or q12hr

Whenever possible, administration should be initiated 1-2 days before start of chemotherapy known to cause tumor cell lysis (including adrenocorticosteroids)