High Alert Medication: This medication bears a heightened risk of causing significant patient harm when it is used in error.
- Adriamycin PFS
Alone or with other modalities in the treatment of various solid tumors including:
- Bronchogenic carcinoma,
- Malignant lymphomas and leukemias.
- Inhibits DNA and RNA synthesis by forming a complex with DNA; action is cell-cycle S-phase–specific.
- Also has immunosuppressive properties.
Death of rapidly replicating cells, particularly malignant ones.
Absorption: Administered IV only, resulting in complete bioavailability.
Distribution: Widely distributed; does not cross the blood-brain barrier; extensively bound to tissues.
Metabolism and Excretion: Mostly metabolized by the liver (primarily by CYP2D6 and CYP3A4). Converted by liver to an active compound. Excreted predominantly in the bile, 50% as unchanged drug. Less than 5% eliminated unchanged in the urine.
Half-life: 16.7 hr.
TIME/ACTION PROFILE (effect on blood counts)
|IV||10 days||14 days||21–24 days|
- OB: Pregnancy (may cause fetal harm);
- Lactation: Lactation.
Use Cautiously in:
- History of cardiac disease or high cumulative doses of anthracyclines;
- Depressed bone marrow reserve;
- Hepatic impairment (↓ dose if serum bilirubin >1.2 mg/dL);
- Pedi: Geri: Children, geriatric patients, mediastinal radiation, concurrent cyclophosphamide (↑ risk of cardiotoxicity);
- Rep: Women of reproductive potential and men with female partners of reproductive potential;
Adverse Reactions/Side Effects
CV: CARDIOMYOPATHY, ECG changes
Derm: alopecia, photosensitivity
Endo: sterility, prepubertal growth failure with temporary gonadal impairment (children only)
GI: diarrhea, esophagitis, nausea, stomatitis, vomiting
GU: red urine
Hemat: anemia, leukopenia, thrombocytopenia
Local: phlebitis at iv site, tissue necrosis
Resp: recall pneumonitis
Misc: hypersensitivity reactions
* CAPITALS indicate life-threatening.
Underline indicate most frequent.
- CYP2D6 inhibitors, CYP3A4 inhibitors, and P-glycoprotein inhibitors may ↑ risk of toxicity; avoid concurrent use
- CYP2D6 inducers, CYP3A4 inducers, and P-glycoprotein inducers may ↓ effect and ↑ risk of therapeutic failure; avoid concurrent use
- ↑ bone marrow depression with other antineoplastics or radiation therapy.
- Pediatric patients who have received concurrent doxorubicin and dactinomycin have an ↑ risk of recall pneumonitis at variable times following local radiation therapy.
- May ↑ skin reactions at previous radiation therapy sites.
- If paclitaxel is administered first, clearance of doxorubicin is ↓ and the incidence and severity of neutropenia and stomatitis are ↑ (problem is diminished if doxorubicin is administered first).
- Hematologic toxicity is ↑ and prolonged by concurrent use of cyclosporine ; risk of coma and seizures is also ↑.
- Incidence and severity of neutropenia and thrombocytopenia are ↑ by concurrent progesterone.
- Phenobarbital may ↑ clearance and ↓ effects of doxorubicin.
- Doxorubicin may ↓ metabolism and ↑ effects of phenytoin.
- Streptozocin may ↑ the half-life of doxorubicin (dosage ↓ of doxorubicin recommended).
- May ↑ risk of hemorrhagic cystitis from cyclophosphamide.
- May ↑ risk of hepatotoxicity from mercaptopurine.
- Cardiac toxicity may be ↑ by radiation therapy or cyclophosphamide.
- ↑ risk of cardiac toxicity with trastuzumab ; avoid use of doxorubicin for up to 7 mo after discontinuing trastuzumab.
- If dexrazoxane is administered at initiation of doxorubicin-containing regimens, may ↑ risk of therapeutic failure and tumor progression
- May ↓ antibody response to live-virus vaccines and ↑ risk of adverse reactions.
Other regimens are used
IV (Adults): 60–75 mg/m2 daily, repeat every 21 days; or 25–30 mg/m2 daily for 2–3 days, repeat every 3–4 wk or 20 mg/m2 /wk. Total cumulative dose should not exceed 550 mg/m2 without monitoring of cardiac function or 400 mg/m2 in patients with previous chest radiation or other cardiotoxic chemotherapy.
IV (Children): 30 mg/m2 /day for 3 days every 4 wk.
IV (Adults): Serum bilirubin 1.2–3 mg/dL– ↓ dose by 50%; Serum bilirubin 3.1–5 mg/dL– ↓ dose by 75%.
Availability (generic available)
Powder for injection: 10 mg/vial, 20 mg/vial, 50 mg/vial, 150 mg/vial
Solution for injection: 2 mg/mL
- Monitor BP, pulse, respiratory rate, and temperature frequently during administration. Report significant changes.
- Monitor for bone marrow depression. Assess for bleeding (bleeding gums, bruising, petechiae, guaiac stools, urine, and emesis) and avoid IM injections and taking rectal temperatures if platelet count is low. Apply pressure to venipuncture sites for 10 min. Assess for signs of infection during neutropenia. Anemia may occur. Monitor for increased fatigue, dyspnea, and orthostatic hypotension.
- Monitor intake and output ratios, and report occurrence of significant discrepancies. Encourage fluid intake of 2000–3000 mL/day. Allopurinol and alkalinization of the urine may be used to decrease serum uric acid levels and to help prevent urate stone formation.
- Severe and protracted nausea and vomiting may occur as early as 1 hr after therapy and may last 24 hr. Administer parenteral antiemetics 30–45 min prior to therapy and routinely around the clock for the next 24 hr as indicated. Monitor amount of emesis and notify health care professional if emesis exceeds guidelines to prevent dehydration.
- Monitor for development of signs of cardiac toxicity, which may be either acute and transient (ST segment depression, flattened T wave, sinus tachycardia, and extrasystoles) or late onset (usually occurs 1–6 mo after initiation of therapy) and characterized by intractable HF (peripheral edema, dyspnea, rales/crackles, weight gain). Chest x ray, echocardiography, ECGs, and radionuclide angiography may be ordered prior to and periodically during therapy. Cardiotoxicity is more prevalent in children younger than 2 yr and geriatric patients. Dexrazoxane may be used to prevent cardiotoxicity in patients receiving cumulative doses of >300 mg/m2 .
- Assess injection site frequently for redness, irritation, or inflammation during and for up to 2 hr after completion of infusion. Doxorubicin is a vesicant but may infiltrate painlessly even if blood returns on aspiration of infusion needle. Severe tissue damage may occur if doxorubicin extravasates. If extravasation occurs, stop infusion immediately, restart, and complete dose in another vein. Local infiltration of antidote is not recommended. If extravasation is suspected, intermittent application of ice to site for 15 min. 4 times daily for 3 days may be useful. Because of the progressive nature of extravasation reactions, close observation and plastic surgery consultation are recommended. Blistering, ulceration, and/or persistent pain are indications for wide excision surgery, followed by split-thickness skin grafting. May use dexrazoxane to treat extravasation. Administer first infusion of dexrazoxane as soon as possible within 6 hr of extravasation. Remove ice packs for at least 15 min prior to and during dexrazoxane administration. Recommended dose of dexrazoxane for day 1 is 1000 mg/m2 (up to 2000 mg); the dose for day 2 is 1000 mg/m2 (up to 2000 mg); the dose for day 3 is 500 mg/m2 (up to 1000 mg). Dexrazoxane is administered as an IV infusion over 1–2 hr. If swelling, redness, and/or pain persists beyond 48 hr, immediate consultation for possible debridement is indicated.
- Assess oral mucosa frequently for development of stomatitis. Increased dosing interval and/or decreasing dose is recommended if lesions are painful or interfere with nutrition.
Lab Test Considerations:
Verify negative pregnancy test before starting therapy.
Monitor CBC and differential prior to and periodically during therapy. WBC nadir occurs 10–14 days after administration, and recovery usually occurs by the 21st day. Thrombocytopenia and anemia may also occur. Increased dosing interval and/or decreased dose is recommended if ANC is <1000 cells/mm3 and/or platelet count is <50,000 cells/mm3 .
- Monitor renal (BUN and serum creatinine) and hepatic (AST, ALT, LDH, and serum bilirubin) function prior to and periodically during therapy. Dose reduction is required for bilirubin >1.2 m g/dL or serum creatinine >3 m g/dL.
- May cause ↑ serum and urine uric acid concentrations.
- High Alert: Fatalities have occurred with incorrect administration of chemotherapeutic agents. Before administering, clarify all ambiguous orders; double-check single, daily, and course-of-therapy dose limits; have second practitioner independently double-check original order, calculations, and infusion pump settings.
- High Alert: Do not confuse doxorubicin hydrochloride with doxorubicin liposomal (Doxil) or with daunorubicin hydrochloride or with idarubicin. Clarify orders that do not include both generic and brand names.
Solution should be prepared in a biologic cabinet. Wear gloves, gown, and mask while handling medication. Discard IV equipment in specially designated containers.
- Aluminum needles may be used to administer doxorubicin but should not be used during storage, because prolonged contact results in discoloration of solution and formation of a dark precipitate. Solution is red.
- IV Push: Dilution: Dilute each 10 mg with 5 mL of 0.9% NaCl (nonbacteriostatic) for injection. Shake to dissolve completely. Do not add to IV solution. Reconstituted medication is stable for 24 hr at room temperature and 48 hr if refrigerated. Protect from sunlight. Concentration: 2 mg/mL.
- Rate: Administer each dose over 3–5 min through Y-site of a free-flowing infusion of 0.9% NaCl or D5W. Facial flushing and erythema along involved vein frequently occur when administration is too rapid.
- Intermittent Infusion: Has also been mixed in 100–250 mL of 0.9% NaCl.
- Rate: Infuse over 30–60 min.
- Y-Site Compatibility:
- arsenic trioxide
- calcium chloride
- calcium gluconate
- etoposide phosphate
- leucovorin calcium
- 0.9% NaCl
- potassium acetate
- potassium chloride
- sodium acetate
- zoledronic acid
- Y-Site Incompatibility:
- amphotericin B deoxycholate
- amphotericin B lipid complex
- amphotericin B liposome
- gemtuzumab ozogamicin
- magnesium sulfate
- potassium phosphate
- sodium phosphate
- Explain purpose of doxorubicin to patient.
- Instruct patient to notify health care professional promptly if fever; sore throat; signs of infection; bleeding gums; bruising; petechiae; blood in stools, urine, or emesis; increased fatigue; dyspnea; or orthostatic hypotension occurs. Caution patient to avoid crowds and persons with known infections. Instruct patient to use soft toothbrush and electric razor and to avoid falls. Caution patient not to drink alcoholic beverages or take medication containing aspirin or NSAIDs, because these may precipitate gastric bleeding.
- Instruct patient to report pain at injection site immediately.
- Instruct patient to inspect oral mucosa for erythema and ulceration. If ulceration occurs, advise patient to use sponge brush, rinse mouth with water after eating and drinking, and confer with health care professional if mouth pain interferes with eating. Pain may require treatment with opioid analgesics. The risk of developing stomatitis is greatest 5–10 days after a dose; usual duration is 3–7 days.
- Instruct patient to notify health care professional immediately if irregular heartbeat, shortness of breath, swelling of lower extremities, or skin irritation (swelling, pain, or redness of feet or hands) occurs.
- Discuss the possibility of hair loss with patient. Explore methods of coping. Regrowth usually occurs 2–3 mo after discontinuation of therapy.
- Instruct patient not to receive any vaccinations without advice of health care professional.
- Inform patient that medication may cause urine to appear red for 1–2 days.
- Instruct patient to notify health care professional if skin irritation occurs at site of previous radiation therapy.
- Advise family and/or caregivers to take precautions (i.e., latex gloves) in handling body fluids for at least 5 days post-treatment.
- Instruct patient to notify health care professional of all Rx or OTC medications, vitamins, or herbal products being taken and to consult health care professional before taking other Rx, OTC, or herbal products.
- Inform patient that doxorubicin may increase risk of developing secondary cancers.
- Rep: May have teratogenic effects. Advise females of reproductive potential to use effective contraception during and for 6 mo after last dose and to avoid breast feeding during and for 10 days after last dose. Advise males with female partners of reproductive potential to use effective contraception during and for at least 3 mo after last dose of doxorubicin. Inform patient before initiating therapy that this medication may cause irreversible gonadal suppression, or irreversible amenorrhea or early menopause.
- Emphasize the need for periodic lab tests to monitor for side effects.
- Decrease in size or spread of malignancies in solid tumors.
- Improvement of hematologic status in leukemias.
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