CYCLOPHOSPHAMIDE- cyclophosphamide injection, powder, lyophilized, for solution
Baxter Healthcare Corporation
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DESCRIPTION
Cyclophosphamide is a synthetic antineoplastic drug chemically related to the nitrogen mustards. The chemical name for cyclophosphamide is 2-[bis(2-chloroethyl)amino]tetrahydro-2H-1,3,2-oxazaphosphorine 2-oxide monohydrate, and has the following structural formula:
Cyclophosphamide has a molecular formula of C7H15Cl2N2O2P•H2O and a molecular weight of 279.1. Cyclophosphamide is soluble in water, saline, or ethanol.
Cyclophosphamide for Injection, USP, (lyophilized) is a sterile white cake available as 500 mg, 1 g, and 2 g strength vials.
- 500 mg vial contains 534.5 mg cyclophosphamide monohydrate equivalent to 500 mg cyclophosphamide and 375 mg mannitol
- 1 g vial contains 1069.0 mg cyclophosphamide monohydrate equivalent to 1 g cyclophosphamide and 750 mg mannitol
- 2 g vial contains 2138.0 mg cyclophosphamide monohydrate equivalent to 2 g cyclophosphamide and 1500 mg mannitol
Cyclophosphamide Tablets, USP, are for oral use and contain 25 mg or 50 mg cyclophosphamide (anhydrous). Inactive ingredients in Cyclophosphamide Tablets are: acacia, FD&C Blue No. 1, D&C Yellow No. 10 Aluminum Lake, lactose, magnesium stearate, starch, stearic acid and talc.
CLINICAL PHARMACOLOGY
Cyclophosphamide is biotransformed principally in the liver to active alkylating metabolites by a mixed function microsomal oxidase system. These metabolites interfere with the growth of susceptible rapidly proliferating malignant cells. The mechanism of action is thought to involve cross-linking of tumor cell DNA.
Cyclophosphamide is well absorbed after oral administration with a bioavailability greater than 75%. The unchanged drug has an elimination half-life of 3 to 12 hours. It is eliminated primarily in the form of metabolites, but from 5 to 25% of the dose is excreted in urine as unchanged drug. Several cytotoxic and noncytotoxic metabolites have been identified in urine and in plasma. Concentrations of metabolites reach a maximum in plasma 2 to 3 hours after an intravenous dose. Plasma protein binding of unchanged drug is low but some metabolites are bound to an extent greater than 60%. It has not been demonstrated that any single metabolite is responsible for either the therapeutic or toxic effects of cyclophosphamide. Although elevated levels of metabolites of cyclophosphamide have been observed in patients with renal failure, increased clinical toxicity in such patients has not been demonstrated.
INDICATIONS AND USAGE
Malignant Diseases
Cyclophosphamide, although effective alone in susceptible malignancies, is more frequently used concurrently or sequentially with other antineoplastic drugs. The following malignancies are often susceptible to cyclophosphamide treatment:
- Malignant lymphomas (Stages III and IV of the Ann Arbor staging system), Hodgkin’s disease, lymphocytic lymphoma (nodular or diffuse), mixed-cell type lymphoma, histiocytic lymphoma, Burkitt’s lymphoma.
- Multiple myeloma.
- Leukemias: Chronic lymphocytic leukemia, chronic granulocytic leukemia (it is usually ineffective in acute blastic crisis), acute myelogenous and monocytic leukemia, acute lymphoblastic (stem-cell) leukemia in children (cyclophosphamide given during remission is effective in prolonging its duration).
- Mycosis fungoides (advanced disease).
- Neuroblastoma (disseminated disease).
- Adenocarcinoma of the ovary.
- Retinoblastoma.
- Carcinoma of the breast.
Nonmalignant Disease
Biopsy Proven “Minimal Change” Nephrotic Syndrome in Children:
Cyclophosphamide is useful in carefully selected cases of biopsy proven “minimal change” nephrotic syndrome in children but should not be used as primary therapy. In children whose disease fails to respond adequately to appropriate adrenocorticosteroid therapy or in whom the adrenocorticosteroid therapy produces or threatens to produce intolerable side effects, cyclophosphamide may induce a remission. Cyclophosphamide is not indicated for the nephrotic syndrome in adults or for any other renal disease.
CONTRAINDICATIONS
Continued use of cyclophosphamide is contraindicated in patients with severely depressed bone marrow function. Cyclophosphamide is contraindicated in patients who have demonstrated a previous hypersensitivity to it. See WARNINGS and PRECAUTIONS.
WARNINGS
Carcinogenesis, Mutagenesis, and Impairment of Fertility
Second malignancies have developed in some patients treated with cyclophosphamide used alone or in association with other antineoplastic drugs and/or modalities. Most frequently, they have been urinary bladder, myeloproliferative, or lymphoproliferative malignancies. Second malignancies most frequently were detected in patients treated for primary myeloproliferative or lymphoproliferative malignancies or nonmalignant disease in which immune processes are believed to be involved pathologically.
In some cases, the second malignancy developed several years after cyclophosphamide treatment had been discontinued. In a single breast cancer trial utilizing two to four times the standard dose of cyclophosphamide in conjunction with doxorubicin a small number of cases of secondary acute myeloid leukemia occurred within two years of treatment initiation. Urinary bladder malignancies generally have occurred in patients who previously had hemorrhagic cystitis. In patients treated with cyclophosphamide-containing regimens for a variety of solid tumors, isolated case reports of secondary malignancies have been published. One case of carcinoma of the renal pelvis was reported in a patient receiving long-term cyclophosphamide therapy for cerebral vasculitis. The possibility of cyclophosphamide-induced malignancy should be considered in any benefit-to-risk assessment for use of the drug.
Cyclophosphamide can cause fetal harm when administered to a pregnant woman and such abnormalities have been reported following cyclophosphamide therapy in pregnant women. Abnormalities were found in two infants and a six-month-old fetus born to women treated with cyclophosphamide. Ectrodactylia was found in two of the three cases. Normal infants have also been born to women treated with cyclophosphamide during pregnancy, including the first trimester. If this drug is used during pregnancy, or if the patient becomes pregnant while taking (receiving) this drug, the patient should be apprised of the potential hazard to the fetus. Women of childbearing potential should be advised to avoid becoming pregnant.
Cyclophosphamide interferes with oogenesis and spermatogenesis. It may cause sterility in both sexes. Development of sterility appears to depend on the dose of cyclophosphamide, duration of therapy, and the state of gonadal function at the time of treatment. Cyclophosphamide-induced sterility may be irreversible in some patients.
Amenorrhea associated with decreased estrogen and increased gonadotropin secretion develops in a significant proportion of women treated with cyclophosphamide. Affected patients generally resume regular menses within a few months after cessation of therapy. Girls treated with cyclophosphamide during prepubescence generally develop secondary sexual characteristics normally and have regular menses. Ovarian fibrosis with apparently complete loss of germ cells after prolonged cyclophosphamide treatment in late prepubescence has been reported. Girls treated with cyclophosphamide during prepubescence subsequently have conceived.
Men treated with cyclophosphamide may develop oligospermia or azoospermia associated with increased gonadotropin but normal testosterone secretion. Sexual potency and libido are unimpaired in these patients. Boys treated with cyclophosphamide during prepubescence develop secondary sexual characteristics normally, but may have oligospermia or azoospermia and increased gonadotropin secretion. Some degree of testicular atrophy may occur. Cyclophosphamide-induced azoospermia is reversible in some patients, though the reversibility may not occur for several years after cessation of therapy. Men temporarily rendered sterile by cyclophosphamide have subsequently fathered normal children.
Urinary System
Hemorrhagic cystitis may develop in patients treated with cyclophosphamide. Rarely, this condition can be severe and even fatal. Fibrosis of the urinary bladder, sometimes extensive, also may develop with or without accompanying cystitis. Atypical urinary bladder epithelial cells may appear in the urine. These adverse effects appear to depend on the dose of cyclophosphamide and the duration of therapy. Such bladder injury is thought to be due to cyclophosphamide metabolites excreted in the urine. Forced fluid intake helps to assure an ample output of urine, necessitates frequent voiding, and reduces the time the drug remains in the bladder. This helps to prevent cystitis. Hematuria usually resolves in a few days after cyclophosphamide treatment is stopped, but it may persist. Medical and/or surgical supportive treatment may be required, rarely, to treat protracted cases of severe hemorrhagic cystitis. It is usually necessary to discontinue cyclophosphamide therapy in instances of severe hemorrhagic cystitis.
Cardiac Toxicity
Although a few instances of cardiac dysfunction have been reported following use of recommended doses of cyclophosphamide, no causal relationship has been established. Acute cardiac toxicity has been reported with doses as low as 2.4 g/m2 to as high as 26 g/m2, usually as a portion of an intensive antineoplastic multi-drug regimen or in conjunction with transplantation procedures. In a few instances with high doses of cyclophosphamide, severe, and sometimes fatal, congestive heart failure has occurred after the first cyclophosphamide dose. Histopathologic examination has primarily shown hemorrhagic myocarditis. Hemopericardium has occurred secondary to hemorrhagic myocarditis and myocardial necrosis. Pericarditis has been reported independent of any hemopericardium.
No residual cardiac abnormalities, as evidenced by electrocardiogram or echocardiogram appear to be present in patients surviving episodes of apparent cardiac toxicity associated with high doses of cyclophosphamide.
Cyclophosphamide has been reported to potentiate doxorubicin-induced cardiotoxicity.
Infections
Treatment with cyclophosphamide may cause significant suppression of immune responses. Serious, sometimes fatal, infections may develop in severely immunosuppressed patients. Cyclophosphamide treatment may not be indicated, or should be interrupted, or the dose reduced, in patients who have or who develop viral, bacterial, fungal, protozoan, or helminthic infections.
PRECAUTIONS
General
Special attention to the possible development of toxicity should be exercised in patients being treated with cyclophosphamide if any of the following conditions are present.
- Leukopenia
- Thrombocytopenia
- Tumor cell infiltration of bone marrow
- Previous X-ray therapy
- Previous therapy with other cytotoxic agents
- Impaired hepatic function
- Impaired renal function
Laboratory Tests
During treatment, the patient’s hematologic profile (particularly neutrophils and platelets) should be monitored regularly to determine the degree of hematopoietic suppression. Urine should also be examined regularly for red cells which may precede hemorrhagic cystitis.
Drug Interactions
The rate of metabolism and the leukopenic activity of cyclophosphamide reportedly are increased by chronic administration of high doses of phenobarbital.
The physician should be alert for possible combined drug actions, desirable or undesirable, involving cyclophosphamide even though cyclophosphamide has been used successfully concurrently with other drugs, including other cytotoxic drugs.
Cyclophosphamide treatment, which causes a marked and persistent inhibition of cholinesterase activity, potentiates the effect of succinylcholine chloride.
If a patient has been treated with cyclophosphamide within 10 days of general anesthesia, the anesthesiologist should be alerted.
Adrenalectomy
Since cyclophosphamide has been reported to be more toxic in adrenalectomized dogs, adjustment of the doses of both replacement steroids and cyclophosphamide may be necessary for the adrenalectomized patient.
Carcinogenesis, Mutagenesis, and Impairment of Fertility
See WARNINGS for information on carcinogenesis, mutagenesis, and impairment of fertility.
Nursing Mothers
Cyclophosphamide is excreted in breast milk. Because of the potential for serious adverse reactions and the potential for tumorigenicity shown for cyclophosphamide in humans, a decision should be made whether to discontinue nursing or to discontinue the drug, taking into account the importance of the drug to the mother.
Pediatric Use
The safety profile of cyclophosphamide in pediatric patients is similar to that of the adult population (see ADVERSE REACTIONS).
Geriatric Use
Insufficient data from clinical studies of cyclophosphamide for malignant lymphoma, multiple myeloma, leukemia, mycosis fungoides, neuroblastoma, retinoblastoma, and breast carcinoma are available for patients 65 years of age and older to determine whether they respond differently than younger patients. In two clinical trials in which cyclophosphamide was compared with paclitaxel, each in combination with cisplatin, for the treatment of advanced ovarian carcinoma, 154 (28%) of 552 patients who received cyclophosphamide plus cisplatin were 65 years or older. Subset analyses (<65 versus >65 years) from these trials, published reports of clinical trials of cyclophosphamide-containing regimens in breast cancer and non-Hodgkin’s lymphoma, and postmarketing experience suggest that elderly patients may be more susceptible to cyclophosphamide toxicities. In general, dose selection for an elderly patient should be cautious, usually starting at the low end of the dosing range and adjusting as necessary based on patient response (see DOSAGE AND ADMINISTRATION: Treatment of Malignant Diseases).
ADVERSE REACTIONS
Information on adverse reactions associated with the use of cyclophosphamide is arranged according to body system affected or type of reaction. The adverse reactions are listed in order of decreasing incidence. The most serious adverse reactions are described in the WARNINGS section.
Digestive System
Nausea and vomiting commonly occur with cyclophosphamide therapy. Anorexia and, less frequently, abdominal discomfort or pain and diarrhea may occur. There are isolated reports of hemorrhagic colitis, oral mucosal ulceration and jaundice occurring during therapy. These adverse drug effects generally remit when cyclophosphamide treatment is stopped.
Skin and Its Structures
Alopecia occurs commonly in patients treated with cyclophosphamide. The hair can be expected to grow back after treatment with the drug or even during continued drug treatment, though it may be different in texture or color. Skin rash occurs occasionally in patients receiving the drug. Pigmentation of the skin and changes in nails can occur. Very rare reports of Stevens-Johnson syndrome and toxic epidermal necrolysis have been received during postmarketing surveillance; due to the nature of spontaneous adverse event reporting, a definitive causal relationship to cyclophosphamide has not been established.
Hematopoietic System
Leukopenia occurs in patients treated with cyclophosphamide, is related to the dose of drug, and can be used as a dosage guide. Leukopenia of less than 2000 cells/mm3 develops commonly in patients treated with an initial loading dose of the drug, and less frequently in patients maintained on smaller doses. The degree of neutropenia is particularly important because it correlates with a reduction in resistance to infections. Fever without documented infection has been reported in neutropenic patients.
Thrombocytopenia or anemia develops occasionally in patients treated with cyclophosphamide. These hematologic effects usually can be reversed by reducing the drug dose or by interrupting treatment. Recovery from leukopenia usually begins in 7 to 10 days after cessation of therapy.
Urinary System
See WARNINGS for information on cystitis and urinary bladder fibrosis.
Hemorrhagic ureteritis and renal tubular necrosis have been reported to occur in patients treated with cyclophosphamide. Such lesions usually resolve following cessation of therapy.
Respiratory System
Interstitial pneumonitis has been reported as part of the postmarketing experience. Interstitial pulmonary fibrosis has been reported in patients receiving high doses of cyclophosphamide over a prolonged period.
Other
Anaphylactic reactions have been reported; death has also been reported in association with this event. Possible cross-sensitivity with other alkylating agents has been reported. SIADH (syndrome of inappropriate ADH secretion) has been reported with the use of cyclophosphamide. Malaise and asthenia have been reported as part of the postmarketing experience.
OVERDOSAGE
No specific antidote for cyclophosphamide is known. Overdosage should be managed with supportive measures, including appropriate treatment for any concurrent infection, myelosuppression, or cardiac toxicity should it occur.
DOSAGE AND ADMINISTRATION
Treatment of Malignant Diseases
Adults and Children
When used as the only oncolytic drug therapy, the initial course of cyclophosphamide for patients with no hematologic deficiency usually consists of 40 to 50 mg/kg given intravenously in divided doses over a period of 2 to 5 days. Other intravenous regimens include 10 to 15 mg/kg given every 7 to 10 days or 3 to 5 mg/kg twice weekly.
Oral cyclophosphamide dosing is usually in the range of 1 to 5 mg/kg/day for both initial and maintenance dosing.
Many other regimens of intravenous and oral cyclophosphamide have been reported. Dosages must be adjusted in accord with evidence of antitumor activity and/or leukopenia. The total leukocyte count is a good, objective guide for regulating dosage. Transient decreases in the total white blood cell count to 2000 cells/mm3 (following short courses) or more persistent reduction to 3000 cells/mm3 (with continuing therapy) are tolerated without serious risk of infection if there is no marked granulocytopenia.
When cyclophosphamide is included in combined cytotoxic regimens, it may be necessary to reduce the dose of cyclophosphamide as well as that of the other drugs.
Cyclophosphamide and its metabolites are dialyzable although there are probably quantitative differences depending upon the dialysis system being used. Patients with compromised renal function may show some measurable changes in pharmacokinetic parameters of cyclophosphamide metabolism, but there is no consistent evidence indicating a need for cyclophosphamide dosage modification in patients with renal function impairment.
Treatment of Nonmalignant Diseases
Biopsy Proven "Minimal Change" Nephrotic Syndrome in Children
An oral dose of 2.5 to 3 mg/kg daily for a period of 60 to 90 days is recommended. In males, the incidence of oligospermia and azoospermia increases if the duration of cyclophosphamide treatment exceeds 60 days. Treatment beyond 90 days increases the probability of sterility. Adrenocorticosteroid therapy may be tapered and discontinued during the course of cyclophosphamide therapy. See PRECAUTIONS concerning hematologic monitoring.
Intravenous administration
Parenteral drug products should be inspected visually for particulate matter and discoloration prior to administration, whenever solution and container permit.
Cyclophosphamide does not contain any antimicrobial preservative and thus care must be taken to assure the sterility of prepared solutions. USE ASEPTIC TECHNIQUE.
Cyclophosphamide for Injection, USP
Cyclophosphamide may be prepared for intravenous administration using 0.9% Sterile Sodium Chloride Injection, USP or Sterile Water for Injection, USP with the following methods. Add the diluent to the vial and gently swirl to dissolve the drug completely. Use the quantity of diluent shown below to reconstitute the product:
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| Contains Mannitol |
Quantity of | Approximate Cyclophosphamide Concentration |
| 500 mg | 534.5 mg | 375 mg | 25 mL | |
| 1 g | 1069.0 mg | 750 mg | 50 mL | 2% (20 mg per mL) |
| 2 g | 2138.0 mg | 1500 mg | 100 mL |
For Direct Intravenous Injection
Cyclophosphamide reconstituted to 2% concentration in 0.9% Sterile Sodium Chloride Injection, USP can be injected directly.
Cyclophosphamide reconstituted to 2% concentration in Sterile Water for Injection, USP is hypotonic and should not be injected directly.
For Intravenous Infusion
Cyclophosphamide should first be reconstituted in 0.9% Sterile Sodium Chloride Injection, USP or Sterile Water for Injection, USP to a 2% concentration (20 mg per mL) and then further diluted for infusion to a minimum concentration of 0.2% (2 mg per mL) with any of the following diluents:
- Dextrose Injection, USP (5% dextrose)
- Dextrose and Sodium Chloride Injection, USP (5% dextrose and 0.9% Sterile Sodium Chloride Injection, USP)
- Sodium Chloride Injection, USP (0.45% Sterile Sodium Chloride Injection, USP)
Storage
Unopened vials of cyclophosphamide are stable until the date indicated on the package when stored at or below 25°C (77°F).
If not used immediately, for microbiological integrity, cyclophosphamide solutions should be stored as follows:
|
||
| Diluent | Storage | |
| Room Temperature | Refrigerated | |
| Reconstituted Solution (Without Further Dilution) | ||
| 0.9% Sterile Sodium Chloride Injection, USP | up to 24 hrs | up to 6 days |
| Reconstituted solution in Sterile Water for Injection, USP must be further diluted and stored as described below | ||
| Further Diluted Solutions * | ||
|
Sodium Chloride Injection, USP (0.45% Sterile Sodium Chloride Injection, USP) | up to 24 hrs | up to 6 days |
|
Dextrose Injection, USP (5% dextrose) | up to 24 hrs | up to 36 hrs |
|
Dextrose and Sodium Chloride Injection, USP (5% Dextrose and 0.9% Sterile Sodium Chloride Injection, USP) | up to 24 hrs | up to 36 hrs |
Cyclophosphamide (prepared for intravenous administration) is chemically and physically stable for the period of time as shown in the above table.
HOW SUPPLIED
Cyclophosphamide for Injection, USP
Cyclophosphamide for Injection, USP (lyophilized) is a sterile white cake containing cyclophosphamide monohydrate and mannitol and is supplied in vials for single dose use.
Cyclophosphamide for Injection, USP
| NDC 10019-988-01 | 500 mg vial, carton of 1 |
| NDC 10019-989-01 | 1.0 g vial, carton of 1 |
| NDC 10019-990-01 | 2.0 g vial, carton of 1 |
Store vials at or below 25°C (77°F). During transport or storage of cyclophosphamide vials, temperature influences can lead to melting of the active ingredient, cyclophosphamide. Vials containing melted substance can be visually differentiated. Melted cyclophosphamide is a clear or yellowish viscous liquid usually found as a connected phase or in droplets in the affected vials. Do not use cyclophosphamide vials if there are signs of melting.
Cyclophosphamide Tablets, USP
Cyclophosphamide Tablets, 25 mg and Cyclophosphamide Tablets, 50 mg, are white tablets with blue flecks containing 25 mg and 50 mg cyclophosphamide (anhydrous), respectively.
| NDC 10019-984-09 | 50 mg, bottles of 100 |
| NDC 10019-982-09 | 25 mg, bottles of 100 |
Store tablets at or below 25°C (77°F); tablets will withstand brief exposure to temperatures up to 30°C (86°F) but should be protected from temperatures above 30°C (86°F).
Caution should be exercised when handling and preparing the cyclophosphamide for injection, USP (lyophilized), or bottles containing cyclophosphamide tablets. The handling and preparation of cyclophosphamide should always be in accordance with current guidelines1-4 on safe handling of cytotoxic agents. To minimize the risk of dermal exposure, always wear gloves when handling vials containing cyclophosphamide sterile powder for injection, or bottles containing cyclophosphamide tablets. The coating of the cyclophosphamide tablets prevents direct contact of persons handling the tablets with the active substance. However, to prevent inadvertent exposure to the active substance, the cyclophosphamide tablets should not be divided or crushed. Personnel should avoid exposure to broken tablets. If contact with broken tablets occurs, wash immediately and thoroughly. More information is available in the references listed below.
REFERENCES
- NIOSH Alert: Preventing occupational exposures to antineoplastic and other hazardous drugs in healthcare settings. 2004. U.S. Department of Health and Human Services, Public Health Service, Centers for Disease Control and Prevention, National Institute for Occupational Safety and Health, DHHS (NIOSH) Publication No. 2004-165.
- OSHA Technical Manual, TED 1-0.15A, Section VI: Chapter 2. Controlling Occupational Exposure to Hazardous Drugs. OSHA, 1999.
http://www.osha.gov/dts/osta/otm/otm_vi/otm_vi_2.html - American Society of Health-System Pharmacists. ASHP guidelines on handling hazardous drugs. Am J Health-Syst Pharm. 2006; 63:1172-1193.
- Polovich, M., White, J. M., & Kelleher, L.O. (eds.) 2005. Chemotherapy and biotherapy guidelines and recommendations for practice (2nd. ed.) Pittsburgh, PA: Oncology Nursing Society.
Baxter Logo
Vials Manufactured by:
Baxter Healthcare Corporation
Deerfield, Illinois 60015 USA
Tablets Manufactured for:
Baxter Healthcare Corporation
Deerfield, Illinois 60015 USA
Revised April 2012
Baxter is a trademark of Baxter International Inc.
USA C66
HA-30-01-218
PRINCIPAL DISPLAY PANEL - PACKAGING LABELING
Container Label
NDC 10019-988-01
Cyclophosphamide
for Injection, USP
500 mg
Lyophilized
CYTOTOXIC AGENT
Rx only
Single use vial for intravenous use.
Discard unused solution.
Baxter Logo
Manufactured by Baxter Healthcare Corporation
Deerfield, IL 60015 USA
Each vial contains 500 mg cyclophosphamide
and 375 mg mannitol.
Usual Dosage: See insert for complete
Dosage and Administration instructions.
Caution: After reconstitution, only Sodium
Chloride Injection 0.45%; Dextrose
Injection, USP 5%; and Dextrose and
Sodium Chloride Injection, USP 5%/0.9%
can be used for diluting this product prior
to intravenous infusion.
Store Vial at or below 25°C (77°F)
460-629-01
(01)00310019955506
USA HA-65-01-180 C 61
Carton Label
NDC 10019-988-01
Cyclophosphamide
for Injection, USP
500 mg
Lyophilized
CYTOTOXIC AGENT
After Reconstitution: For direct intravenous
injection or must be further diluted before
intravenous infusion
Single Use Vial.
Discard unused solution.
Rx only
Baxter Logo
Manufactured by:
Baxter Healthcare Corporation
Deerfield, IL 60015 USA
Made in Germany
Each vial contains
500 mg cyclophosphamide and 375 mg
mannitol.
Lyophilized
CYTOTOXIC AGENT
Store Vial at or below 25°C (77°F)
Usual dosage: See prescribing information
for complete Dosage and Administration
instructions.
Caution: After reconstitution, only Sodium
Chloride Injection 0.45%; Dextrose Injection,
USP 5%; and Dextrose and Sodium Chloride
Injection, USP 5%/0.9% can be used for
diluting this product prior to intravenous
infusion.
Single use vial for intravenous use.
Discard unused solution.
460-630-01
NDC 10019-988-01
Cyclophosphamide
for Injection, USP
500 mg
Lyophilized
CYTOTOXIC AGENT
After Reconstitution: For direct intravenous
injection or must be further diluted before
intravenous infusion
Single Use Vial.
Discard unused solution.
Rx only
Baxter Logo
Maufactured by:
Baxter Healthcare Corporation
Deerfield, IL 60015 USA
Made in Germany
NDC 10019-988-01
Cyclophosphamide
for Injection, USP
500 mg
Lyophilized
CYTOTOXIC AGENT
After Reconstitution: For direct intravenous
injection or must be further diluted before
intravenous infusion
Single Use Vial.
Discard unused solution.
Rx only
N3
1001995501
8
NDC 10019-988-01
Cyclophosphamide
for Injection, USP
500 mg
Lyophilized
Single Use Vial.
Discard unused solution.
HA-80-01-372
USA
C
66
LOT/EXP:
2638B5126
| CYCLOPHOSPHAMIDE
cyclophosphamide injection, powder, lyophilized, for solution |
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| Labeler - Baxter Healthcare Corporation (005083209) |
| Establishment | |||
| Name | Address | ID/FEI | Business Operations |
| Baxter Oncology GmbH | 344276063 | MANUFACTURE | |