PHARMACOKINETICS SECTION.


Pharmacokinetics. In systemic absorption studies in 52 patients, topical application of 0.05 mL of 0.5% podofilox solution to external genitalia did not result in detectable serum levels. Applications of 0.1 to 1.5 mL resulted in peak serum levels of to 17 ng/mL one to two hours after application. The elimination half-life ranged from 1.0 to 4.5 hours. The drug was not found to accumulate after multiple treatments.

PRECAUTIONS SECTION.


PRECAUTIONS. General. Data are not available on the safe and effective use of this product for treatment of warts occurring in the perianal area or on mucous membranes of the genital area (including the urethra, rectum and vagina). The recommended method of application, frequency of application, and duration of usage should not be exceeded (see DOSAGE AND ADMINISTRATION).. Information for Patients. The patient should be provided with Patient Information leaflet when Podofilox Topical Solution prescription is filled.. Carcinogenesis, Mutagenesis and Impairment of Fertility. Reports of lifetime carcinogenicity studies in mice are not available. Published animal studies, in general, have not shown the drug substance, podofilox, to be carcinogenic.1,2,3,4,5 There are published reports that, in mouse studies, crude podophyllin resin (containing podofilox) applied topically to the cervix produced changes resembling carcinoma in situ.6 These changes were reversible at five weeks after cessation of treatment. In one reported experiment, epidermal carcinoma of the vagina and cervix was found in out of 18 mice after 120 applications of podophyllin7 (the drug was applied twice weekly over 15-month period).Podofilox was not mutagenic in the Ames plate reverse mutation assay at concentrations up to mg/plate, with and without metabolic activation. No cell transformation related to potential oncogenicity was observed in BALB/3T3 cells after exposure to podofilox at concentrations up to 0.008 ug/mL without metabolic activation and 12 ug/mL podofilox with metabolic activation. Results from the mouse micronucleus in vivo assay using podofilox 0.5% solution in concentrations up to 25 mg/kg, indicate that podofilox should be considered potential clastogen (a chemical that induces disruption and breakage of chromosomes).Daily topical application of Podofilox Topical Solution 0.5% at doses up to the equivalent of 0.2 mg/kg (5 times the recommended maximum human dose) to rats throughout gametogenesis, mating, gestation, parturition and lactation for two generations demonstrated no impairment of fertility.. Pregnancy. Teratogenic Effects:. Pregnancy Category C:. Podofilox was not teratogenic in the rabbit following topical application of up to 0.21 mg/kg (5 times the maximum human dose) once daily for 13 days. The scientific literature contains references that podofilox is embryotoxic in rats when administered systemically in dose approximately 250 times the recommended maximum human dose.8,9 Teratogenicity and embryotoxicity have not been studied with intravaginal application. Many antimitotic drug products are known to be embryotoxic. There are no adequate and well-controlled studies in pregnant women. Podofilox should be used during pregnancy only if the potential benefit justifies the potential risk to the fetus.. Nursing Mothers. It is not known whether this drug is excreted in human milk. Because of the potential for serious adverse reactions in nursing infants from podofilox, 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. Safety and effectiveness in pediatric patients have not been established.

PACKAGE LABEL.PRINCIPAL DISPLAY PANEL.


PRINCIPAL DISPLAY PANEL 3.5 mL Carton. Rx OnlyNDC 0574-0611-05PodofiloxTopical Solution0.5%For topical use only3.5 mLThe following image is placeholder representing the product identifier that is either affixed or imprinted on the drug package label during the packaging operation.. 4U3RC-podofilox-topical-solution.jpg. serialization-template.jpg.

PEDIATRIC USE SECTION.


Pediatric Use. Safety and effectiveness in pediatric patients have not been established.

ADVERSE REACTIONS SECTION.


ADVERSE REACTIONS. In clinical trials, the following local adverse reactions were reported at some point during treatment.Adverse ExperienceMalesFemalesBurning64%78%Pain50%72%Inflammation71%63%Erosion67%67%Itching50%65%Reports of burning and pain were more frequent and of greater severity in women than in men.Adverse effects reported in less than 5% of the patients included pain with intercourse, insomnia, tingling, bleeding, tenderness, chafing, malodor, dizziness, scarring, vesicle formation, crusting edema, dryness/peeling, foreskin irretraction, hematuria, vomiting and ulceration.

CARCINOGENESIS & MUTAGENESIS & IMPAIRMENT OF FERTILITY SECTION.


Carcinogenesis, Mutagenesis and Impairment of Fertility. Reports of lifetime carcinogenicity studies in mice are not available. Published animal studies, in general, have not shown the drug substance, podofilox, to be carcinogenic.1,2,3,4,5 There are published reports that, in mouse studies, crude podophyllin resin (containing podofilox) applied topically to the cervix produced changes resembling carcinoma in situ.6 These changes were reversible at five weeks after cessation of treatment. In one reported experiment, epidermal carcinoma of the vagina and cervix was found in out of 18 mice after 120 applications of podophyllin7 (the drug was applied twice weekly over 15-month period).Podofilox was not mutagenic in the Ames plate reverse mutation assay at concentrations up to mg/plate, with and without metabolic activation. No cell transformation related to potential oncogenicity was observed in BALB/3T3 cells after exposure to podofilox at concentrations up to 0.008 ug/mL without metabolic activation and 12 ug/mL podofilox with metabolic activation. Results from the mouse micronucleus in vivo assay using podofilox 0.5% solution in concentrations up to 25 mg/kg, indicate that podofilox should be considered potential clastogen (a chemical that induces disruption and breakage of chromosomes).Daily topical application of Podofilox Topical Solution 0.5% at doses up to the equivalent of 0.2 mg/kg (5 times the recommended maximum human dose) to rats throughout gametogenesis, mating, gestation, parturition and lactation for two generations demonstrated no impairment of fertility.

CLINICAL PHARMACOLOGY SECTION.


CLINICAL PHARMACOLOGY. Mechanism of Action. Treatment of genital warts with podofilox results in necrosis of visible wart tissue. The exact mechanism of action is unknown.. Pharmacokinetics. In systemic absorption studies in 52 patients, topical application of 0.05 mL of 0.5% podofilox solution to external genitalia did not result in detectable serum levels. Applications of 0.1 to 1.5 mL resulted in peak serum levels of to 17 ng/mL one to two hours after application. The elimination half-life ranged from 1.0 to 4.5 hours. The drug was not found to accumulate after multiple treatments.

CLINICAL STUDIES SECTION.


CLINICAL STUDIES. In clinical studies with podofilox solution, the test product and its vehicle were applied in double-blind fashion to comparable patient groups. Patients were treated for two to four weeks, and reevaluated at two-week follow-up examination. Although the number of patients and warts evaluated at each time period varied, the results among investigators were relatively consistent.The following table represents the responses noted in terms of frequency of response by lesions treated and the overall response by patients. Data are presented for the 2-week follow-up only for those patients evaluated at that time point.Response in Treated PatientsInitially ClearedCleared and clearing mean no visible wart tissue remained at the treated sitesRecurred after ClearingCleared at 2-Week Follow-up% Warts(n=524)79%(412/524)35%(146/412)60%(269/449)% Patients(n=70)50%(35/70)60%(21/35)25%(14/57).

CONTRAINDICATIONS SECTION.


CONTRAINDICATIONS. Podofilox Topical Solution 0.5% is contraindicated for patients who develop hypersensitivity or intolerance to any component of the formulation.

DESCRIPTION SECTION.


DESCRIPTION. Podofilox Topical Solution is an antimitotic drug which can be chemically synthesized or purified from the plant families Coniferae and Berberidaceae (e.g. species of Juniperus and Podophyllum). Podofilox Topical Solution 0.5% is formulated for topical administration. Each milliliter of solution contains mg of podofilox, in vehicle containing lactic acid and sodium lactate in alcohol 95%, USP.Podofilox has molecular weight of 414.4 daltons, and is soluble in alcohol and sparingly soluble in water. Its chemical name is 5,8,8a,9-Tetrahydro-9-hydroxy-5-(3,4,5-trimethoxylphenyl)furo[3,4:6,7] naphtho[2,3,d]-1, 3-dioxol-6(5aH)-one. Podofilox has the following structural formula:. Chemical Structure.

DOSAGE & ADMINISTRATION SECTION.


DOSAGE AND ADMINISTRATION. In order to ensure that the patient is fully aware of the correct method of therapy and to identify which specific warts should be treated, the technique for initial application of the medication should be demonstrated by the prescriber.Apply twice daily morning and evening (every 12 hours), for consecutive days, then withhold use for consecutive days. This one week cycle of treatment may be repeated up to four times until there is no visible wart tissue. If there is incomplete response after four treatment weeks, alternative treatment should be considered. Safety and effectiveness of more than four treatment weeks have not been established. Podofilox Topical Solution 0.5% is applied to the warts with an applicator supplied with the drug. The drug-dampened applicator should be touched to the wart to be treated, applying the minimum amount of solution necessary to cover the lesion. Treatment should be limited to less than 10 cm2 of wart tissue and to no more than 0.5 mL of the solution per day. There is no evidence to suggest that more frequent application will increase efficacy, but additional applications would be expected to increase the rate of local adverse reactions and systemic absorption.Care should be taken to allow the solution to dry before allowing the return of opposing skin surfaces to their normal positions. After each treatment, the used applicator should be carefully disposed of and the patient should wash his or her hands.

GENERAL PRECAUTIONS SECTION.


General. Data are not available on the safe and effective use of this product for treatment of warts occurring in the perianal area or on mucous membranes of the genital area (including the urethra, rectum and vagina). The recommended method of application, frequency of application, and duration of usage should not be exceeded (see DOSAGE AND ADMINISTRATION).

HOW SUPPLIED SECTION.


HOW SUPPLIED. 3.5 mL Podofilox Topical Solution 0.5% is supplied as clear liquid in amber glass bottles with child-resistant screw caps. NDC 0574-0611-05. Store at 20 and 25C (68 to 77F) [see USP Controlled Room Temperature]. Avoid excessive heat. Do not freeze.

INDICATIONS & USAGE SECTION.


INDICATIONS AND USAGE. Podofilox Topical Solution 0.5% is indicated for the topical treatment of external genital warts (Condyloma acuminatum). This product is not indicated in the treatment of perianal or mucous membrane warts (see PRECAUTIONS).. Diagnosis. Although genital warts have characteristic appearance, histopathologic confirmation should be obtained if there is any doubt of the diagnosis. Differentiating warts from squamous cell carcinoma (so-called Bowenoid papulosis) is of particular concern. Squamous cell carcinoma may also be associated with human papillomavirus but should not be treated with Podofilox Topical Solution 0.5%.

INFORMATION FOR PATIENTS SECTION.


Information for Patients. The patient should be provided with Patient Information leaflet when Podofilox Topical Solution prescription is filled.

MECHANISM OF ACTION SECTION.


Mechanism of Action. Treatment of genital warts with podofilox results in necrosis of visible wart tissue. The exact mechanism of action is unknown.

NURSING MOTHERS SECTION.


Nursing Mothers. It is not known whether this drug is excreted in human milk. Because of the potential for serious adverse reactions in nursing infants from podofilox, decision should be made whether to discontinue nursing or to discontinue the drug, taking into account the importance of the drug to the mother.

OVERDOSAGE SECTION.


OVERDOSE. Topically applied podofilox may be absorbed systemically (see CLINICAL PHARMACOLOGY section). Toxicity reported following systemic administration of podofilox in investigational use for cancer treatment included: nausea, vomiting, fever, diarrhea, bone marrow depression, and oral ulcers. Following to 10 daily intravenous doses of 0.5 to mg/kg/day, significant hematological toxicity occurred but was reversible. Other toxicities occurred at lower doses. Toxicity reported following systemic administration of podophyllum resin included: nausea, vomiting, fever, diarrhea, peripheral neuropathy, altered mental status, lethargy, coma, tachypnea, respiratory failure, leukocytosis, pancytosis, hematuria, renal failure, and seizures. Treatment of topical overdosage should include washing the skin free of any remaining drug and symptomatic and supportive therapy.

PREGNANCY SECTION.


Pregnancy. Teratogenic Effects:. Pregnancy Category C:. Podofilox was not teratogenic in the rabbit following topical application of up to 0.21 mg/kg (5 times the maximum human dose) once daily for 13 days. The scientific literature contains references that podofilox is embryotoxic in rats when administered systemically in dose approximately 250 times the recommended maximum human dose.8,9 Teratogenicity and embryotoxicity have not been studied with intravaginal application. Many antimitotic drug products are known to be embryotoxic. There are no adequate and well-controlled studies in pregnant women. Podofilox should be used during pregnancy only if the potential benefit justifies the potential risk to the fetus.

REFERENCES SECTION.


REFERENCES. 1.Berenblum I. The effect of podophyllotoxin on the skin of the mouse, with reference to carcinogenic, cocarcinogenic, and anticarcinogenic action. Cancer Inst 11:839-841, 1951.2.Kaminetzky HA, Swerdlow M. Podophyllin and the mouse cervix: assessment of carcinogenic potential. Am Obst Gyn 95:486-490, 1965.3.McGrew EA, Kaminetzky HA. The genesis of experimental cervical epithelial dysplasia. Am Clin Path 35:538-545, 1961.4.Roe FJC, Salaman MH. Further studies on incomplete carcinogenesis: triethylene melamine (T.E.M.) 1,2 benxanthracene and beta-propiolactone as initiators of skin tumor formation in the mouse. Brit Cancer, 9:177-203, 1955.5.Taper HS. Induction of the deficient acid DNAase activity in mouse interfollicular epidermis by croton oil as possible tumor promoting mechanism. Zeitschrift fur Krebsforschung and Klinisch Onkologie (Cancer Research and Clinical Oncology, Berlin). 90:197-210, 1977.6.Kaminetzky HA, McGrew EA, Phillips RL. Experimental cervical epithelial dysplasia. Obst Gyn 14:1-10, 1959.7.Kaminetzky HA, McGrew EA: Podophyllin and mouse cervix: Effect of long term application. Arch Path 73:481-485, 1962.8.Didcock K, Jackson D, Robson JM. The action of some nucleotoxic substances on pregnancy. Brit Pharmacol 11:437-441, 1956.9.Thiersch JB. Effect of podophyllin (P) and podophylotoxine (PT) on the rat litter in utero. Soc Exptl Biol Med Proc. 113:124-127, 1963.. 1.Berenblum I. The effect of podophyllotoxin on the skin of the mouse, with reference to carcinogenic, cocarcinogenic, and anticarcinogenic action. Cancer Inst 11:839-841, 1951.. 2.Kaminetzky HA, Swerdlow M. Podophyllin and the mouse cervix: assessment of carcinogenic potential. Am Obst Gyn 95:486-490, 1965.. 3.McGrew EA, Kaminetzky HA. The genesis of experimental cervical epithelial dysplasia. Am Clin Path 35:538-545, 1961.. 4.Roe FJC, Salaman MH. Further studies on incomplete carcinogenesis: triethylene melamine (T.E.M.) 1,2 benxanthracene and beta-propiolactone as initiators of skin tumor formation in the mouse. Brit Cancer, 9:177-203, 1955.. 5.Taper HS. Induction of the deficient acid DNAase activity in mouse interfollicular epidermis by croton oil as possible tumor promoting mechanism. Zeitschrift fur Krebsforschung and Klinisch Onkologie (Cancer Research and Clinical Oncology, Berlin). 90:197-210, 1977.. 6.Kaminetzky HA, McGrew EA, Phillips RL. Experimental cervical epithelial dysplasia. Obst Gyn 14:1-10, 1959.. 7.Kaminetzky HA, McGrew EA: Podophyllin and mouse cervix: Effect of long term application. Arch Path 73:481-485, 1962.. 8.Didcock K, Jackson D, Robson JM. The action of some nucleotoxic substances on pregnancy. Brit Pharmacol 11:437-441, 1956.. 9.Thiersch JB. Effect of podophyllin (P) and podophylotoxine (PT) on the rat litter in utero. Soc Exptl Biol Med Proc. 113:124-127, 1963.

SPL PATIENT PACKAGE INSERT SECTION.


Patient Information. PODOFILOX TOPICAL SOLUTION 0.5% AND GENITAL WARTS1.APPLY PODOFILOX TOPICAL SOLUTION ONLY ON THE WARTS POINTED OUT BY YOUR DOCTOR.2.STOP TREATMENT AND CALL YOUR DOCTOR IF YOU HAVE BLEEDING, SWELLING, OR EXCESSIVE PAIN, BURNING, OR ITCHING.3.DO NOT USE MORE THAN TWO TIMES DAY.4.DO NOT USE FOR MORE THAN THREE DAYS IN ROW.5.DO NOT HAVE SEXUAL INTERCOURSE ON THE DAYS YOU ARE APPLYING PODOFILOX TOPICAL SOLUTION.6.WASH HANDS AFTER EVERY USE.INTRODUCTIONPodofilox Topical Solution slowly kills external genital warts. The warts will change from fleshy skin color to dry, crusted, dead look, then disappear. Three out of four patients feel some burning or pain after they apply Podofilox Topical Solution. Other side effects may include redness, soreness, tenderness, and small sores. These usually go away within week after Podofilox Topical Solution is stopped. If pain or other side effects bother you too much, stop applying Podofilox Topical Solution and contact your doctor.HOW TO USE PODOFILOX TOPICAL SOLUTIONFollow these and your doctors instructions carefully. Apply Podofilox Topical Solution only on the warts pointed out by your doctor. Do not use it on any other warts on or inside your body, or for any other skin growth.1.Open the bottle and put it on flat surface. Hold the bottle and dip the applicator tip into the liquid. Touch the applicator tip against the inside edge of the bottle so the applicator is wet with no liquid dripping. Make sure to close the bottle tightly after use.APPLY PODOFILOX TOPICAL SOLUTION ONLY WHERE YOUR DOCTOR HAS INSTRUCTED YOU2.Apply Podofilox Topical Solution to the wart. Do not get it on normal skin. If wart is in skin fold, spread the skin apart so you can reach the wart. hand mirror can help sometimes. Let Podofilox Topical Solution dry before letting the skin folds return to their normal position. Wash your hands well with soap and water after you use Podofilox Topical Solution.3.Apply Podofilox Topical Solution once in the morning and once in the evening for three days in row. Then stop applying Podofilox Topical Solution and wait four days. Using Podofilox Topical Solution like this is called treatment week.There is no need to wash Podofilox Topical Solution off the wart area.DO NOT APPLY PODOFILOX TOPICAL SOLUTION MORE THAN TWICE EACH DAY OR FOR MORE THAN THREE DAYS IN ROW. USING PODOFILOX TOPICAL SOLUTION MORE OFTEN WILL NOT MAKE IT WORK BETTER BUT MAY INCREASE SIDE EFFECTS4.If the warts do not go away, repeat the Podofilox Topical Solution treatment for another week. You can use Podofilox Topical Solution up to four treatment weeks (REMEMBER: treatment week is twice day for three days, then four days with no treatment). Your doctor may ask you to come back for check-up visit during treatment. If the warts have not gone away after four treatment weeks, stop applying Podofilox Topical Solution and contact your doctor.IF THE AREA YOU ARE PUTTING PODOFILOX TOPICAL SOLUTION ON IS BLEEDING OR SWOLLEN, OR IF THERE IS EXCESSIVE PAIN, BURNING OR ITCHING, STOP APPLYING PODOFILOX TOPICAL SOLUTION AND CONTACT YOUR DOCTOR5.Genital warts can come back. If your warts come back, contact your doctor.SPECIAL CAUTIONSoGenital warts are contagious. You can give them to or get them from your sexual partner. Make sure your sexual partner has been checked for genital warts. Condoms can help protect both you and your partner. Do not have sexual intercourse for the three days you are applying Podofilox Topical Solution.oWomen should make sure to use birth control so they will not get pregnant while on Podofilox Topical Solution. The effects on the unborn baby are not known. Women can use Podofilox Topical Solution during their menstrual period.oPodofilox Topical Solution is prescribed only for your external genital warts. Do not let anyone else use it.REMEMBER:oDo not use the applicator more than once. Throw it away so it can not infect anyone else.oAlways wash your hands after using Podofilox Topical Solution.oDo not get it in your eyes. If you do, immediately flush your eyes with water and contact your doctor.oKeep the bottle tightly closed and store in an upright position.oBe sure to keep this and all medications out of the reach of children.CONTACT YOUR DOCTOR IF YOU HAVE QUESTIONS ABOUT PODOFILOX TOPICAL SOLUTIONManufactured ByPerrigo(R)Minneapolis, MN 554272124160(05-12). 1.APPLY PODOFILOX TOPICAL SOLUTION ONLY ON THE WARTS POINTED OUT BY YOUR DOCTOR.. 2.STOP TREATMENT AND CALL YOUR DOCTOR IF YOU HAVE BLEEDING, SWELLING, OR EXCESSIVE PAIN, BURNING, OR ITCHING.. 3.DO NOT USE MORE THAN TWO TIMES DAY.. 4.DO NOT USE FOR MORE THAN THREE DAYS IN ROW.. 5.DO NOT HAVE SEXUAL INTERCOURSE ON THE DAYS YOU ARE APPLYING PODOFILOX TOPICAL SOLUTION.. 6.WASH HANDS AFTER EVERY USE.. 1.Open the bottle and put it on flat surface. Hold the bottle and dip the applicator tip into the liquid. Touch the applicator tip against the inside edge of the bottle so the applicator is wet with no liquid dripping. Make sure to close the bottle tightly after use.. 2.Apply Podofilox Topical Solution to the wart. Do not get it on normal skin. If wart is in skin fold, spread the skin apart so you can reach the wart. hand mirror can help sometimes. Let Podofilox Topical Solution dry before letting the skin folds return to their normal position. Wash your hands well with soap and water after you use Podofilox Topical Solution.. 3.Apply Podofilox Topical Solution once in the morning and once in the evening for three days in row. Then stop applying Podofilox Topical Solution and wait four days. Using Podofilox Topical Solution like this is called treatment week.There is no need to wash Podofilox Topical Solution off the wart area.. 4.If the warts do not go away, repeat the Podofilox Topical Solution treatment for another week. You can use Podofilox Topical Solution up to four treatment weeks (REMEMBER: treatment week is twice day for three days, then four days with no treatment). Your doctor may ask you to come back for check-up visit during treatment. If the warts have not gone away after four treatment weeks, stop applying Podofilox Topical Solution and contact your doctor.. 5.Genital warts can come back. If your warts come back, contact your doctor.. oGenital warts are contagious. You can give them to or get them from your sexual partner. Make sure your sexual partner has been checked for genital warts. Condoms can help protect both you and your partner. Do not have sexual intercourse for the three days you are applying Podofilox Topical Solution.. oWomen should make sure to use birth control so they will not get pregnant while on Podofilox Topical Solution. The effects on the unborn baby are not known. Women can use Podofilox Topical Solution during their menstrual period.. oPodofilox Topical Solution is prescribed only for your external genital warts. Do not let anyone else use it.. oDo not use the applicator more than once. Throw it away so it can not infect anyone else.. oAlways wash your hands after using Podofilox Topical Solution.. oDo not get it in your eyes. If you do, immediately flush your eyes with water and contact your doctor.. oKeep the bottle tightly closed and store in an upright position.. oBe sure to keep this and all medications out of the reach of children.

SPL UNCLASSIFIED SECTION.


Diagnosis. Although genital warts have characteristic appearance, histopathologic confirmation should be obtained if there is any doubt of the diagnosis. Differentiating warts from squamous cell carcinoma (so-called Bowenoid papulosis) is of particular concern. Squamous cell carcinoma may also be associated with human papillomavirus but should not be treated with Podofilox Topical Solution 0.5%.

TERATOGENIC EFFECTS SECTION.


Teratogenic Effects:. Pregnancy Category C:. Podofilox was not teratogenic in the rabbit following topical application of up to 0.21 mg/kg (5 times the maximum human dose) once daily for 13 days. The scientific literature contains references that podofilox is embryotoxic in rats when administered systemically in dose approximately 250 times the recommended maximum human dose.8,9 Teratogenicity and embryotoxicity have not been studied with intravaginal application. Many antimitotic drug products are known to be embryotoxic. There are no adequate and well-controlled studies in pregnant women. Podofilox should be used during pregnancy only if the potential benefit justifies the potential risk to the fetus.

WARNINGS SECTION.


WARNINGS. Correct diagnosis of the lesions to be treated is essential. See the Diagnosis subsection of the INDICATIONS AND USAGE statement.Podofilox Topical Solution 0.5% is intended for cutaneous use only. Avoid contact with the eye. If eye contact occurs, patient should immediately flush the eye with copious quantities of water and seek medical advice.