dry lips, desquamation, dryness of skin, cracked lips, burning skin, pruritus, flakiness of skin, and stinging on skin; each adverse reaction occurred in less than 1% of patients receiving acyclovir cream and placebo. three patients on acyclovir cream and one patient on placebo discontinued treatment due to an adverse event. an additional study, enrolling 22 healthy adults, was conducted to evaluate the dermal tolerance of acyclovir cream compared with vehicle using single occluded and semi-occluded patch testing methodology. both acyclovir cream and placebo showed a high and cumulative irritation potential. another study, enrolling 251 healthy adults, was conducted to evaluate the contact sensitization potential of acyclovir cream using repeat insult patch testing methodology. of 202 evaluable subjects, possible cutaneous sensitization reactions were observed in the same 4 (2%) subjects with both acyclovir cream and placebo, and these reactions to both acyclovir cream and placebo were confirmed in 3 subjects upon rechallenge. the sensitizing ingredient(s) has not been identified. the safety profile in patients 12 to 17 years of age was similar to that observed in adults. 6.2 postmarketing experience in addition to adverse events reported from clinical trials, the following events have been identified during postapproval use of acyclovir cream. because they are reported voluntarily from a population of unknown size, estimates of frequency cannot be made. these events have been chosen for inclusion due to a combination of their seriousness, frequency of reporting, or potential causal connection to acyclovir cream. general: angioedema, anaphylaxis. skin: contact dermatitis, eczema.

d pregnancies is 2% to 4% and 15% to 20%, respectively. 8.2 lactation risk summary acyclovir is minimally absorbed systemically following topical route of administration, and breastfeeding is not expected to result in exposure of the child to acyclovir cream [see clinical pharmacology (12.3) ] . there are no data on the effects of acyclovir on the breastfed infant or on milk production. the developmental and health benefits of breastfeeding should be considered along with the mother’s clinical need for acyclovir cream and any potential adverse effects on the breastfed child from acyclovir cream or from the underlying maternal condition. 8.4 pediatric use an open-label, uncontrolled trial with acyclovir cream was conducted in 113 patients aged 12 to 17 years with recurrent herpes labialis. in this trial, therapy was applied using the same dosing regimen as in adults and subjects were followed for adverse events. the safety profile was similar to that observed in adults. safety and effectiveness in pediatric patients less than 12 years of age have not been established. 8.5 geriatric use clinical studies of acyclovir cream did not include sufficient numbers of subjects aged 65 and over to determine whether they respond differently from younger subjects. other reported clinical experience has not identified differences in responses between the elderly and younger patients. systemic absorption of acyclovir after topical administration is minimal [see clinical pharmacology (12.3) ] .

15% to 20%, respectively.

of acyclovir following topical application of cream has not been evaluated in patients <18 years of age. 12.4 microbiology mechanism of action: acyclovir is a synthetic purine deoxynucleoside analogue with cell culture and in vivo inhibitory activity against hsv types 1 (hsv-1) and 2 (hsv-2) dna polymerases. it inhibits hsv-1 and hsv-2 replication in cell culture and in vivo. the inhibitory activity of acyclovir is selective due to its affinity for the enzyme thymidine kinase (tk) encoded by hsv. this viral enzyme converts acyclovir into acyclovir monophosphate, a deoxynucleotide analogue. the monophosphate is further converted into diphosphate by cellular guanylate kinase and into triphosphate by a number of cellular enzymes. in biochemical assays, acyclovir triphosphate inhibits replication of α-herpes viral dna. this inhibition is accomplished in 3 ways: 1) competitive inhibition of viral dna polymerase, 2) incorporation into and termination of the growing viral dna chain, and 3) inactivation of the viral dna polymerase. antiviral activity the quantitative relationship between the susceptibility of herpes viruses to antivirals in cell culture and the clinical response to therapy has not been established in humans, and virus sensitivity testing has not been standardized. sensitivity testing results, expressed as the concentration of drug required to inhibit by 50% the growth of virus in cell culture (ec 50 value), vary greatly depending upon a number of factors. using plaque-reduction assays on vero cells, the ec 50 values of acyclovir against herpes simplex virus isolates range from 0.09 to 59.9 μm (0.02 to 13.5 μg/ml) for hsv-1 and from 0.04 to 44.0 μm (0.01 to 9.9 μg/ml) for hsv-2. resistance in cell culture acyclovir-resistant hsv-1 and hsv-2 strains were isolated in cell culture. acyclovir-resistant hsv resulted from mutations in the viral thymidine kinase (tk; pul23) and dna polymerase (pol; pul30) genes. frameshifts were commonly isolated and result in premature truncation of the hsv tk product with consequent decreased susceptibility to acyclovir. mutations in the viral tk gene may lead to complete loss of tk activity (tk negative), reduced levels of tk activity (tk partial), or alteration in the ability of viral tk to phosphorylate the drug without an equivalent loss in the ability to phosphorylate thymidine (tk altered). in cell culture the following resistance-associated substitutions in tk of hsv-1 and hsv-2 were observed (table 1). table 1: summary of acyclovir (acv) resistance-associated amino acid substitutions in cell culture hsv-1 tk p5a, h7q, l50v, g56v, g59a, g61a, k62n, t63a, e83k, p84s, d116n, p131s, r163h, a167v, p173l, q185r, r216s, r220h, t245m, r281stop, t287m, m322k hsv-2 tk l69p, c172r, t288m hsv-1 pol d368a, y557s, e597d, v621s, l702h, n815s, v817m, g841c hsv-2 pol - in hsv-infected patients clinical hsv-1 and hsv-2 isolates obtained from patients who failed treatment for their α-herpesvirus infections were evaluated for genotypic changes in the tk and pol genes and for phenotypic resistance to acyclovir (table 2). hsv isolates with frameshift mutations and resistance-associated substitutions in tk and pol were identified. the listing of substitutions in hsv tk and pol leading to decreased susceptibility to acyclovir is not all inclusive and additional changes will likely be identified in hsv variants isolated from patients who fail acyclovir-containing regimens. the possibility of viral resistance to acyclovir should be considered in patients who fail to respond or experience recurrent viral shedding during therapy. table 2: summary of acv resistance-associated amino acid substitutions observed in treated patients hsv-1 tk g6c, r32h, r41h, r51w, y53c/d/h, y53stop, d55n, g56d/s, p57h, h58/n/r/y, g59r, g61a, k62n, t63i, q67stop, s74stop, y80n, e83k, p84l, y87h, w88r, r89q/w, e95stop, t103p, q104h, q104stop, h105p, d116n, m121l/r, s123r, q125h, m128l, g129d, i143v, a156v, d162a/h/n, r163g/h, l170p, y172c, p173l, a174p, a175v, r176q/w, r176stop, l178r, s181n, v187m, a189v, v192a, g200c/d/s, t201p, v204g, a207p, l208f/h, r216c/h, r220c/h, r221h, r222c/h, l227f, t245m/p, l249p, q250stop, c251g, r256w, e257k, q261r, t287m, l288stop, l291p/r, l297s, l315s, l327r, c336y, q342stop, t354p, l364p, a365t hsv-2 tk r34c, g39e, r51w, y53n, g59p, g61w, s66p, a72s, d78n, p85s, a94v, n100h, i101s, q105p, t131p, d137stop, f140l, l158p, s169p, r177w, s182n, m183i, v192m, g201d, r217h, r221c/h, q222stop, r223h, y239stop, r271v, p272s, d273r, t287m, c337y hsv-1 pol k532t, q570r, l583v, a605v, a657t, d672n, v715g, a719t/v, s724n, f733c, e771q, s775n, l778m, e798k, v813m, n815s, g841s, i890m, g901v, v958l h1228d hsv-2 pol e250q, d307n, k533e, a606v, c625r, r628c, e678g, a724v, s725g, s729n, i731f, q732r, m789k/t, v818a, n820s, y823c, q829r, t843a, m910t, d912n/v, a915v, f923l, t934a, r964h note: additional substitutions to acyclovir resistance may exist. cross-resistance cross-resistance has been observed among hsv isolates carrying frameshift mutations and resistance-associated substitutions, which confer reduced susceptibility to penciclovir (pcv), famciclovir (fcv), and foscarnet (fos) [table 3]. table 3: summary of amino acid substitutions conferring cross-resistance to pcv, fcv or fos cross-resistant to pcv/fcv hsv-1 tk g6c, r32h, r51w, y53c/h, h58n, g61a, s74stop, e83k, p84l, t103p, q104stop, d116n, m121r, i143v, r163h, l170p, y172c, a174p, r176q/w, q185r, a189v, g200d, l208h, r216c, r220h, r222c/h, t245m, q250stop, r256w, r281stop, t287m, l315s, m322k, c336y cross-resistant to pcv/fcv hsv-1 pol a657t, d672n, v715g, a719v, s724n, e798k, n815s, g841s cross-resistant to pcv/fcv hsv-2 tk g39e, r51w, y53n, r177w, r221h, t288m cross-resistant to pcv/fcv hsv-2 pol k533e, a606v, c625r, r628c, s729n, q732r, m789k/t, v818a, n820s, f923l, t934a cross-resistant to fos hsv-1 pol d368a, a605v, d672n, l702h, v715g, a719t/v, s724n, l778m, e798k, v813m, n815s, v817m, g841c/s, i890m cross-resistant to fos hsv-2 pol k533e, a606v, c625r, r628c, a724v, s725g, s729n, i731f, q732r, m789k/t, v818a, y823c, d912v, f923l, t934a, r964h

nce was observed between subjects receiving acyclovir cream or placebo in the prevention of progression of cold sore lesions. 14.2 pediatric subjects an open-label, uncontrolled trial with acyclovir cream was conducted in 113 patients aged 12 to 17 years with recurrent herpes labialis. in this trial, therapy was applied using the same dosing regimen as in adults and subjects were followed for adverse events. the safety profile was similar to that observed in adults.

at the earliest sign or symptom of recurrence. instruct patients to wash hands prior to application and ensure the face and/or lips are clean and dry. advise patients to apply acyclovir cream topically 5 times per day for 4 days. instruct patients to topically apply a quantity of acyclovir cream sufficient to cover the affected area, including the outer margin. advise patients to avoid unnecessary rubbing of the affected area to avoid aggravating or transferring the infection. instruct patients to wash their hands with soap and water after using acyclovir cream. keep out of reach of children. possible side effects common skin-related side effects that occurred when acyclovir cream was applied include application site reactions. acyclovir cream has the potential for irritation and contact sensitization. manufactured in canada by: bausch health companies inc. laval, quebec h7l 4a8, canada manufactured for: teva pharmaceuticals usa, inc. parsippany, nj 07054 revised february 2021 9673501

you: • become sick very easily (have a weak immune system). • are pregnant or plan to become pregnant. it is not known if acyclovir cream will harm your unborn baby. • are breastfeeding or plan to breastfeed. it is not known if acyclovir cream passes into your breast milk. talk to your healthcare provider about the best way to feed your baby if you use acyclovir cream. tell your healthcare provider about all the medicines you take, including prescription and over-the-counter medicines, vitamins, and herbal supplements. how should i use acyclovir cream? • use acyclovir cream exactly as your healthcare provider tells you to use it. • use acyclovir cream as soon as you have the first symptoms of a cold sore such as itching, redness, burning or tingling, or when the cold sore appears. • wash your hands with soap and water before and after applying acyclovir cream. • the affected area should be clean and dry before applying acyclovir cream. • apply acyclovir cream to the affected area 5 times each day for 4 days, including the outer edge. • you should not apply other skin products to the affected area during treatment with acyclovir cream. • avoid unnecessary rubbing of the cold sore because this may cause the cold sore to spread to other areas around your mouth or make your cold sore worse. what are the possible side effects of acyclovir cream? the most common side effects of acyclovir cream are skin reactions at the treatment site and may include: dry or cracked lips, peeling, flaking or dryness of the skin, a burning or stinging feeling, and itching. these are not all the possible side effects of acyclovir cream. call your doctor for medical advice about side effects. you may report side effects to fda at 1-800-fda-1088. how should i store acyclovir cream? • store acyclovir cream at room temperature between 68° to 77°f (20° to 25°c). keep acyclovir cream and all medicines out of reach of children. general information about the safe and effective use of acyclovir cream. medicines are sometimes prescribed for purposes other than those listed in a patient information leaflet. do not use acyclovir cream for a condition for which it was not prescribed. do not give acyclovir cream to other people, even if they have the same symptoms you have. it may harm them. you can ask your pharmacist or healthcare provider for information about acyclovir cream that is written for health professionals. what are the ingredients in acyclovir cream? active ingredient: acyclovir inactive ingredients: cetostearyl alcohol, mineral oil, poloxamer 407, propylene glycol, sodium lauryl sulfate, water, and white petrolatum manufactured in canada by: bausch health companies inc. laval, quebec h7l 4a8, canada manufactured for: teva pharmaceuticals usa, inc. parsippany, nj 07054 for more information, call 1-800-321-4576. this patient information has been approved by the u.s. food and drug administration. revised: 02/2021 9673501