Practical management of acne for clinicians: An international consensus from the Global Alliance to Improve Outcomes in Acne Diane M. Thiboutot, MD, Chair,a Brigitte Dr(cid:1)eno, MD, PhD, Co-Chair,b,c,d Abdullah Abanmi, MD,e Andrew F. Alexis, MD, MPH,f Elena Araviiskaia, MD, PhD,g Maria Isabel Barona Cabal, MD,h Vincenzo Bettoli, MD,i Flordeliz Casintahan, MD,j Steven Chow, MD,k Adilson da Costa, MD, MSc, PhD,l Tam El Ouazzani, MD,m Chee-Leok Goh, MD,n Harald P. M. Gollnick, MD,o Minerva Gomez, MD,p Nobukazu Hayashi, MD, PhD,q Maria Isabel Herane, MD,r Juan Honeyman, MD,s Sewon Kang, MD,t Lajos Kemeny, MD, PhD,u Raj Kubba, MD,v Julien Lambert, MD, PhD,w Alison M. Layton, MB ChB,x James J. Leyden, MD,y Jose Luis Lo(cid:1)pez-Estebaranz, MD, PhD,z Nopadon Noppakun, MD,aa,bb Falk Ochsendorf, MD,cc Cristina Oprica, MD, PhD,dd Beatriz Orozco, MD,ee Montserrat Perez, MD,ff Jaime Piquero-Martin, MD, MSc,gg Jo-Ann See, MD,hh Dae Hun Suh, MD, PhD,ii Jerry Tan, MD,jj Vicente Torres Lozada, MD,kk Patricia Troielli, MD,ll and Leihong Flora Xiang, MD, PhDmm Hershey,Pennsylvania;Nantes,France;Riyadh,SaudiArabia;NewYork,NewYork;St.Petersburg,Russia; Cali and Medellin, Colombia; Ferrara, Italy; Manila, Philippines; Kuala Lumpur, Malaysia; Sao Paulo, Brazil; Casablanca, Morocco; Singapore; Magdeburg, Germany; Monterrey, M(cid:1)exico; Tokyo, Japan; Santiago, Chile; Baltimore, Maryland; Szeged, Hungary; New Delhi, India; Edegem, Belgium; Harrogate, United Kingdom; Philadelphia, Pennsylvania; Madrid and Barcelona, Spain; Bangkok, Thailand; Frankfurt, Germany; Stockholm, Sweden; Caracas, Venezuela; Sydney, Australia; Seoul, South Korea; Windsor, Canada; Mexico City, M(cid:1)exico; Buenos Aires, Argentina; and Shanghai, China Scientific advances are continually improving the knowledge of acne and contributing to the refinement of treatment options; it is important for clinicians to regularly update their practice patterns to reflect current standards. The Global Alliance to Improve Outcomes in Acne is an international group of dermatologists with an interest in acne research and education that has been meeting regularly since 2001. As a group, we have continuously evaluated the literature on acne. This supplement focuses on Publication of this article was supported by an unrestricted Baltimoret; MTA-SZTE Dermatological Research Group, Depart- educational grant provided by Galderma International SAS, ment of Dermatology and Allergology, University of Szegedu; Paris,France. KubbaClinic/DelhiDermatologyGroup,NewDelhiv;Department From the Clinical and Transitional Science Research Education, of Dermatology, University Hospital of Antwerp University of Penn State Hershey Dermatologya; Department of Dermato Antwerp, Edegemw; Harrogate and District National Health Cancerology, CHU Nantes - Place Alexis Ricordeaub; Unit of Science Foundation Trustx; Perelman School of Medicine, GeneandCellTherapy,CHUNantes-PlaceAlexisRicordeauc; University of Pennsylvania, Philadelphiay; Dermatology Depart- FacultyofMedicineNantesFrance,CHUNantes-PlaceAlexis ment, Hospital Universitario Fundacio(cid:1)n Alcorco(cid:1)n, Madridz; Ricordeaud; Dr Sulaiman Al Habib Hospital, Riyadhe; Depart- Department of Clinical Immunology, Allergology, and Derma- mentofDermatology,MountSinaiSt.Luke’sandMountSinai tology, Chulalongkorn University, Bangkokaa; Department of West, New Yorkf; Department of Dermatology and Venereal Dermatology, Bumrungrad International Hospital, Bangkokbb; Diseases, First State Medical University of St. Petersburgg; Klinik fu€r Dermatologie, Venerologie, und Allergologie, Univer- CentroM(cid:1)edicoImbanaco,Calih;DermatologyUnit,Department sity Hospital, Frankfurtcc; Department of Laboratory Medicine, ofClinicalandExperimentalMedicine,AziendaOspedalieraS. Karolinska Institutet, Division of Clinical Microbiology, Anna-UniversityofFerrarai;DepartmentofDermatology,Jose Karolinska University Hospital Huddinge, Stockholmdd; Medica R. Reyes Memorial Medical Center, Manilaj; Pantai Hospital, Dermatologa,ClinicaLasAmericas,Medellinee;ClinicaDermato- KualaLumpurk;StateofSaoPauloWorkers’WelfareInstitutel; logica de Moragas Barcelonaff; Instituto de Biomedicina Uni- Dermatologie e Allergologie, Casablancam; National Skin versidad Central de Venezuela, Caracasgg; Central Sydney Centre, Singaporen; Department of Dermatology and Venere- Dermatologyhh; Department of Dermatology, Seoul National ology, Otto-von-Guericke-University, Magdeburgo; Derma- University College of Medicineii; Schulich School of Medicine tology Department, University Hospital, Universidad andDentistry,UniversityofWesternOntario,Windsorjj;Derma- AutonomadeNuevoLeon,Monterreyp;DepartmentofDerma- tology Department, Hospital Juarez, Mexico Citykk; Faculty of tology,ToranomonHospital,Tokyoq;privatepractice,Santiagor; Medicine, University of Buenos Airesll; and Department of University of Chile and Catholic University of Chile, Santiagos; Dermatology, Huashan Hospital, Shanghai Medical College, DepartmentofDermatology,JohnsHopkinsSchoolofMedicine, FudanUniversity.mm S1 S2 Thiboutotetal JAMACADDERMATOL FEBRUARY2018 providing relevant clinical guidance to health care practitioners managing patients with acne, with an emphasis on areas where the evidence base may be sparse or need interpretation for daily practice. (J Am Acad Dermatol 2018;78:S1-23.) Keywords:acnevulgaris;adultacne;scar;post-inflammatoryhyperpigmentation. INTRODUCTION undergraduate training; however, all medical Acneisachronicinflammatoryskindiseasethatis schools teach dermato-venereology. Scientific ad- estimated to affect approximately 85% of the vances arecontinuallyimprovingtheknowledge of population at some point in their lives.1 Generally acneandcontributingtotherefinementoftreatment straightforward to recognize clinically, acne has a options; it is important for clinicians to regularly variable presentation with a constellation of lesion update their practice patterns to reflect current types including open and closed comedones, standards. The Global Alliance to Improve papules, pustules, nodules, and cysts.1,2 The face is Outcomes in Acne is an international group of involvedinmostcases,andthetrunkisaffectedinup dermatologists with an interest in acne research to 61% of patients.3-6 Acne lesions can progress to andeducationthathasbeenmeetingregularlysince scars, postinflammatory hyperpigmention (PIH), or 2001. As a group, we have continuously evaluated both, which can be bothersome to patients.3,7,8 theliteratureonacne.Wecreatedconsensusrecom- The pathogenesis is multifactorial, involving the mendations about acne management based on our hormonal influence of androgens along with experience and available research, which were excess sebum production, disturbed keratinization, publishedin2previoussupplementstotheJournal inflammation, and stimulation of the innate of the American Academy of Dermatology.9,10 immune system by several pathways including Outside of the Global Alliance, we have also each hypercolonizationbyPropionibacteriumacnes.9-11 been involved in creating evidence-based national Although acne is a very common disease, little and international guidelines for acne management, time is spenton it in medical curricula, even within including those published by the European dermatology modules.12 In fact, dermatology Dermatology Forum (EDF); the Colegio Ibero- education as a whole is lacking in medicine in Latinoamericano de Dermatolog(cid:1)ıa; the Indian some countries; 33 US medical schools have no Society Dermatology, Venereology, and Leprosy; undergraduate dermatology programs, and more and the American Academy of Dermatology than half of American medical schools teach (AAD).3,14,15 In our experience, evidence-based \10 hours of dermatology.12,13 In Europe, which is guidelinesandclinicalconsensusrecommendations home to 25,000 dermato-venereologists, teaching can be quite different. Evidence-based guidelines hours vary between 18 to 60 hours during medical rate the quality of evidence supporting available Conflicts of interest: All authors have served as advisory board investigator for Galderma, a consultant for Glaxo SmithKline, membersforGaldermaandreceivedhonoraria.Inaddition,Dr and an investigator and speaker for Meda. Dr Leyden has Thiboutothasreceivedfeesandresearchfundingforservingas received honoraria serving as an advisory board member for a consultant and investigator for Allergan, Mimetica, Novan, AllerganandaconsultantforBioPharmX,Unliver,Cutanea,and and Sebacia and as a consultant for Dermira, Galderma, Foamix.Dr Seehasreceivedhonorariaservingasan advisory Photosonix, and Xenon. Dr Dreno has received honoraria board member for Allergan and Meda. Dr Tan has received servingasanadvisoryboardmemberforMeda.DrAlexishas honorariaandgrantsservingasanadvisoryboardmemberfor received consulting fees from Roche, honoraria serving as an Allergan, Bayer, Cipher, Valeant, and Roche; a speaker for advisoryboardmemberforAllerganandFoamixandreceived Cipher,Valeant,andPierreFabre;aninvestigatorforDermira, grantspaidtohisinstitutionforservingasaninvestigatorfor Galderma,andXenon;andaconsultantforGalderma,Xenon, BioPharmix,Allergan,andNovan.DrAraviiskaiahasservedas andBoots/Walgreens.DrTorreshasreceivedhonorariaservinh an advisoryboard member for L’Oreal and Vicy and received as an advisory board member for Galderma. Dr Troielli has honoraria for speaking for La Roche Posay, Astellas Pharma, receivedhonorariaservingasaspeakerforLaRochePosayand Pierre Fabre, Uriage, Jadran JGL, Glenmark, Meda, and Bayer aspeakerandinvestigatorforGalderma. Healthcare.DrCostahasreceivedhonorariaandgrantsserving AcceptedforpublicationSeptember20,2017. as an advisory board member for Hypermarcas, L’Oreal, and Reprint requests: Diane M. Thiboutot, MD, Department of AvonandasaninvestigatorforGaldermaandHypermarcas.Dr Dermatology, Penn State University College of Medicine, 500 Hayashireceivedfeesandhonorariaservingasaspeakerand University Drive, Hershey, PA 17033. E-mail: dthiboutot@ consultantforMaruhoandGlaxoSmithKlineandasaspeaker pennstatehealth.psu.edu. forPolaPharma.DrHeranehasreceivedhonorariaservingas 0190-9622/$36.00 an advisory board member for Galderma. Dr Layton has (cid:1)2017PublishedbyElsevieronbehalfoftheAmericanAcademy received grants, fees, research funding, and honoraria for ofDermatology,Inc. serving as an advisory board member, speaker, and https://doi.org/10.1016/j.jaad.2017.09.078 JAMACADDERMATOL Thiboutot etal S3 VOLUME78,NUMBER2 An online questionnaire was developed by a Abbreviationsused: selected subgroup of the Global Alliance Steering AAD: AmericanAcademyofDermatology Committee and then distributed to panel members. A/BPO: adapalene/benzoylperoxide Participantswereaskedtorateagreementwitheach EDF: EuropeanDermatologyForum FASET: FacialAcneSeverityEvaluationTool statement on a 5-point Likert scale (strongly agree, FDA: FoodandDrugAdministration agree, disagree, strongly disagree, unable to IGA: InvestigatorGlobalAssessment answer). Those who selected disagree, strongly OC: oralcontraceptive OG: olumacostatglasaretil disagree, or unable to answer were prompted to PIH: postinflammatoryhyperpigmention provideawrittenexplanationofwhattheydisagreed with.Responsesfromthefirstsurveywereclassified as round 1, analyzed, and a summary of all areas treatment options, but do not strongly advise the ofconsensusandindividualstatementsofdisagree- clinician about creating a practical treatment mentwasprepared.Theresults,alongwithmodified approach.Clinicalconsensusrecommendationsuse survey questions (round 2), were sent to respon- expert opinion and experience and focus more on dents.Again,resultswerecollectedandanalyzedto the philosophy of treatment, the individual patient, arrive at the final results, which are presented here. as well as clinical experience of what options work Thefinalstatementsanddocumentwereeditedand wellinparticularsituations. reviewed by the panel. Consensus was defined as Inthissupplement,weaimedtoidentifythecore agreement among $75% of the dermatologists principlesofaneffectiveacnemanagementstrategy who participated in the panel. The statements and using the Delphi method to reach consensus. The votingresultsarepresentedasSupplementalTableI goal was to help guide clinicians to understand (availaleathttp://www.jaad.org). efficient acne therapeutic strategies that could be readily implemented in the office. We particularly CONSENSUS RECOMMENDATIONS focusedonareaswheretheexistingevidencebaseis Assessing acne severity: impact of new topical less robust and expert opinion could have a role in medications refiningpracticepatterns. There is no standardized acne grading or classi- fication system; however, acne is often categorized byanoverallgestaltasmild,moderate,andseverein DELPHI METHODOLOGY guidelines and recommendations as well as by A live meeting of the Steering Committee of the clinicians treating patients.2,3,14 These categories Global Alliance group was held to identify areas are useful to help guide selection of therapy but of acne management that could be useful to arechosenonthebasisofthesubjectiveopinionof clinicians but that were not well defined in the physician. As a more objective measure of existing evidence-based guidelines. Topics dis- severity, lesion counts or estimates may be used to cussed included acne grading, recent data with help define acne severity.3,17 For example, acne topical therapies, combination regimens for acne, research trials typically associate a range of lesion and special topics of interest (acne in women, counts to objectively classify acne severity, along postinflammatoryhyperpigmentation,andscarring). with an Investigator Global Assessment (IGA).3,17,18 ItwasagreedthattheDelphimethodologycouldbe Butoneproblemindefiningobjectiveassessmentsis usedtohelpcreateastrategicapproachtoacne. that lesion counts alone do not accurately convey A Delphi panel and questionnaire method was subjective aspects of acne, such as variations in usedtoprovideasystematicframeworkforarriving lesion size and visibility (Fig 1).18 Furthermore, at consensus. This methodology incorporates clinical studies in the past did not differentiate expertise into a collective judgment via a panel of between small nodules [0.5-1 cm and those experts who respond to a set of questionnaires.16 [1 cm, which is of clinical importance regarding The panel comprised 36 internationally recognized selectionoftreatmentsandresponserate.Therefore, dermatologists from 27 countries (Argentina, comparison of evidenced-based clinical studies in Australia, Belgium, Brazil, Canada, Chile, China, moderate-to-severeacneisoftennotpossible.3 Colombia, France, Germany, India, Italy, Japan, Anotherproblemincategorizingacneseverityhas Mexico, Malaysia, Morocco, Philippines, Russia, emerged with the development of new, highly Saudi Arabia, Singapore, South Korea, Spain, efficacioustopicalacnemedications:howtodenote Sweden, Thailand, United States, United Kingdom, acne severity in patients who might be good Venezuela).AllweremembersoftheGlobalAlliance candidates for strong topical medications versus internationalandregionalgroups. those who are best suited by early institution of S4 Thiboutotetal JAMACADDERMATOL FEBRUARY2018 Fig1. Illustrationofdifferencesinlesionsofacnevulgaristhatcouldaffectoverallassessment ofacneseveritybutnotlesioncounts.PhotoscourtesyofDermQuest.com.Copyright(cid:1)2006 GaldermaS.A.Allrightsreserved. Table I. Investigator Global Assessment scale recommended by theUS Food and Drug Administration17 Grade Clinicaldescription 0 Clearskin with noinflammatory ornoninflammatory lesions 1 Almost clear;rare noninflammatory lesions with more thanone smallinflammatory lesion 2 Mildseverity;greater than grade1;some noninflammatory lesions with nomore than afew inflammatory lesions (papules/pustules only, nonodular lesions) 3 Moderate severity;greaterthan grade 2;upto many noninflammatory lesions andmay havesome inflammatory lesions, but nomore than onesmallnodular lesion 4 Severe;greater thangrade 3;up to manynoninflammatory and inflammatory lesions, butnomore than afew nodular lesions Scalenotintendedtocovercandidatesfororalisotretinointherapy. oralisotretinoin.19,20Manypracticingdermatologists scale). In 2016, Stein Gold et al reported that the perceive the term severe to refer primarily to fixed combination adapalene 0.3%/benzoyl nodular/conglobate acne, which is appropriately peroxide 2.5% (A/BPO 0.3%) was the ‘‘first topical treated withoral isotretinoin.2Now,however,there fixedecombination agent therapy developed for might be a need for a more refined system of severe inflammatory acne.’’20 A/BPO 0.3% was classifying moderately severe, severe, and very evaluatedina50%-50%populationofsubjects with severe that aligns with additional potential first-line moderateandsevereacne(definedasmoderate[IGA treatment options. The 2016 European S3 Acne score of 3] or severe [IGA score of 4] with 20-100 Guideline has used the following 4-point inflammatory lesions, 30-150 noninflammatory classification system that might help to approach lesions, and #2 nodules on the face).20 A/BPO these issues in a practical fashion3: 1) comedonal 0.3% was efficacious across the population and acne, 2) mild-moderate papulopustular acne; well tolerated (Fig 3); further, in the severe popula- 3) severe papulopustular acne, moderate nodular tion A/BPO 0.3% showed significantly greater effi- acne; and 4) severe nodular acne, conglobate acne. cacyinachievingsuccess(clearoralmostclearora Similarly, the IGA scale recommended by the US 3-grade improvement) and reductions in lesion Food and Drug Administration (FDA) considers counts versus vehicle (P = .029 for success and qualityoflesionsandquantity(TableI).17Thisscale P \ .001 for lesion counts).20 Stein Gold et al alsoincludesagradeofsevereacnethatisseparate concludedthatA/BPO0.3%couldhaveanimportant fromnodular/conglobateacne.Weproposethatthe systemic antibiotic-sparing role for patients with designation very severe be reserved for cystic and moderateandsevereinflammatoryacne,particularly conglobateacne,whichareillustratedinFig2. because it targets the microcomedone.20 These in- Single-agent topical therapy for severe vestigators also suggested A/BPO 0.3% could be inflammatory acne. Recently, there have been used alone or in combination with other therapies several studies of topical combination therapy that before moving to oral isotretinoin or while gaining included patients that would be categorized as accesstooralisotretinointherapy.20 severe inflammatory acne (grade 3 on the Phase2studieswithnovelagentshavealsobeen European Union scale or grade 4 on the US FDA published recently for moderate-to-severe acne. A JAMACADDERMATOL Thiboutot etal S5 VOLUME78,NUMBER2 Fig 2. Illustrative photos of severe inflammatory acne vulgaris, largely without nodules (A). B, Very severe acne with cysts. Photos courtesy of DermQuest.com. Copyright (cid:1) 2006 GaldermaS.A.Allrightsreserved. S6 Thiboutotetal JAMACADDERMATOL FEBRUARY2018 Fig3. Patientwithsevereacnevulgaristreatedwithadapalene/benzoylperoxideatbaseline andweek12. Fig 4. Action of retinoids on microcomedones (acne vulgaris precursor lesions) and visible lesions. Note the lag time after cessation of retinoid therapy before visible lesions begin to reappear.ReprintedwithpermissionfromThielitzetal.30 newtopicalagent,olumacostatglasaretil(OG)7.5% score.22 Two phase 3 studies were completed with (aninhibitorofacetylcoenzyme-Acarboxylasewith theminocyclinefoam,withonereportingstatistically putative action as a topical sebum inhibitor), has significantlysuperiorresultstovehiclebuttheother shown promise for treating moderate-to-severe failingtodemonstrateasignificantdifferenceinIGA acne.21 A phase 2 study of 108 patients treated (1of2co-primaryendpoints).Anadditionalphase3 with OG twice daily for 12 weeks showed that study is planned.23 However, it should be noted OGwassignificantlysuperiortovehicleinreducing that monotherapy with a topical antibiotic is inflammatorylesions((cid:1)63.9%vs(cid:1)45.9%,P=.0006) advised against in current guidelines and recom- and noninflammatory lesions ((cid:1)48.1% vs (cid:1)28.8%, mendations because of the potential for anti- P = .0025); in addition, more patients had microbial resistance.2,3,14 For additional details, see improvement of at least 2 grades in IGA (24.5% vs Zouboulisetal.24 7.3%,P=.007).OGwaswelltolerated,withmild-to- Goldetalreportedapost-hocsubgroupanalysis moderateapplication-siteadverseevents.21Atopical ofaphase3studyofclindamycin1.2%/BPO3.75%in foam formulation of minocycline 4% was evaluated moderate-to-severe acne (n = 498) that specifically in subjects with a mean of 33.5 inflammatory compared results in participants with severe acne lesions at baseline. In a phase 2 study, minocycline (n = 86) with those in participants with moderate foam was superior to vehicle in reducing acne (n = 412).25,26 An improvement in global both inflammatory and noninflammatory lesions severity of at least 2 grades was achieved in 55.1% ((cid:1)71.7% vs (cid:1)50.6%, P = .0001; (cid:1)72.7% vs (cid:1)56.5%, ofpatientswithsevereacnecomparedwith31.3%of P=.0197,respectively),aswellasinimprovingIGA those with moderate acne. The proportion of JAMACADDERMATOL Thiboutot etal S7 VOLUME78,NUMBER2 Table II. Strategiesto minimize thelikelihood oftolerabilityproblems associated with induction oftopical retinoidtherapy d Take adetailed patienthistory B Have there beentolerability problems inthe past? d Educatepatient B Mildirritationcanbepartofthetreatmentprocess,butusuallysubsideswithin1-2weeksandcanbemanagedwith appropriate steps B A small dose of retinoid (demonstrate fingertip or pea-sized dose) should be applied in a thin layer to the entire affectedarea B Patientshould usea gentlecleansing regimenand avoidovercleansing d Selectmosttolerable retinoid formulation forclimate andseason B Creamsandlotionsmightbebestfordryorsensitiveskinandgelsorfoamformoreoilyskin(althoughneweraqueous gelsmight also besuitableforsensitiveskin) d Titrateretinoiddose atinitiation B Apply retinoid every other day for first 2-4 weeks (based on clinical trial evidence that this is when irritation is most likely tooccur) B Applygentle,noncomedogenicmoisturizer B Usea short contact methodfor first 2-4 weeks(apply retinoidto fullface for30-60 minutesthen washoff) AdaptedwithpermissionfromLeydenetal.32 participants rated clear or almost clear at study noncomparative study, Gold et al had shown that endpoint was 30.6% in the severe group and 35.7% the combination of A/BPO 0.1% plus doxycycline inthemoderategroup.Theauthorscommentedthat 100mgwassignificantlymoreeffectivethanvehicle ‘‘topicaltherapymayindeed bemorevaluablethan plus doxycycline 100 mg in potential candidates for oftenassumedinpatientswithsevereacnevulgaris.’’ oralisotretinoin.27InasimilarEuropeanstudy,Dreno Gold etal alsonote that in their study persons with etalstudiedA/BPO0.1%pluslymecycline300mgin severe acne were more likely to be female and patientswithmoderate-to-severeacne,andreported youngercomparedwiththemoderategroup,which statistically significantly superior improvements in mighthaveaffectedtheresults.25 acnewiththecombinedregimenversuslymecycline Combination regimens for severe alone.28Zaengleinetalreportedresultsfromaphase acne. Combination regimens with newer agents 4, open-label study of a population with a large mightalsoprovidealternativestooralisotretinoinor proportion(77%)ofpatientswithacnesevereenough serve as an intermediate treatment step before iso- to warrant isotretinoin as judged by independent tretinoin.In a comparative study, Tan et al reported reviewofdigitalphotographs.29Inthisstudy,atriple thatA/BPO0.1%plusdoxycycline200mg/daywasa combination regimen of oral minocycline, BPO 6%, noninferior alternative to oral isotretinoin.19 The and clindamycin phosphate 1.2%/tretinoin 0.025% combination regimen compared with isotretinoin gel significantly improved acne, reducing lesion hadasignificantlyearlieronsetofactioninreducing counts and improving IGA scores.29 By the end of acne lesions at week 2. Overall, isotretinoin was studyatweektwelve,84%ofthosepatientswhowere superiortoA/BPO0.1%plusdoxycyclineinreducing potential candidates for isotretinoin at baseline had nodules (95.6% vs 88.7%), inflammatory lesions experienced enough improvement that isotretinoin (95.2%vs79.6%),andtotal lesions(92.9%vs78.2%; wasnolongeranecessarytreatmentapproach.29 allP\.001)atweek20.However,treatment-related, medicallyrelevantadverseeventswerelessfrequent Delphi results: strategic approach to acne inthecombinationtreatmentarmversusisotretinoin therapy arm (33 events in 18% of subjects vs 73 events in Consensus recommendation 1: retinoids 33.8%,respectively).Theinvestigatorsconcluded‘‘D- have an essential role in treatment of acne.3,14 A/BPO showed a favourable composite efficacy/ For most patients with inflammatory acne, safety profile compared to ISO [isotretinoin].’’ comedonal acne, or both, a topical retinoid Further,theyindicatedA/BPO0.1%plusdoxycycline plus BPO is first-line therapy.2 Together, these is an acceptable alternative to isotretinoin for agents target multiple aspects of acne pathophysi- treatment of acne in patients who are unable or ology, working to normalize keratinization, reduce unwilling to have isotretinoin prescribed.19 In a inflammation,andkillP.acnes.9,10Further,retinoids S8 Thiboutotetal JAMACADDERMATOL FEBRUARY2018 have a unique class action reducing formation of Consensus recommendation 2: the role of acne precursor lesions (microcomedones) and antibioticsinacnetherapyhaschanged.Neither limiting development of new lesions (Fig 4).10,30 topicalnorsystemicantibioticsshouldbeusedas Using cyanoacrylate strips, Thielitz et al demon- monotherapyforacnetreatment.2,45,46 Antibiotic strated that microcomedones rebound almost resistance is a worldwide problem and should be an immediatelyaftertreatmentisdiscontinued,whereas essential consideration when selecting therapy for reductions in visible lesions continue for several acne.45-47Resistantmicrobialorganismsareincreasing weeks because of normal skin turnover.30 This throughout the world’s populations, and worldwide finding is why the AAD guidelines state topical health authorities have called upon the medical retinoids ‘‘allow for maintenance of clearance.’’14 community to limit antibiotic use in situations where Thielitzetalalsoshowedtheefficacyofazelaicacid othermanagementapproachesmaybeused.48-50Use in maintenance therapy was equivalent to that of ofantibioticsinacneaffectsalargenumberofpeople, adapaleneasmentionedintheS3EDFguideline.3,31 considering that resistance can occur in both treated Generally,retinoidsaresimilarin efficacy, andthe individuals and their close household contacts.51 In efficacyimproveswithhigherconcentrations.32Dose- addition, antibiotics are often prescribed for a much dependent effects were first shown with tretinoin in longer duration in acne than for typical infections animal models and ultra-structural studies.30,33 After (eg,monthsratherthandays).52Thus,antibioticusein 2 weeks of treatment, tretinoin 0.1% reduced micro- acne exerts considerable selective pressure on comedones by 80% and tretinoin 0.025% achieved a microbes, including pathogenic and nonpathogenic 35%reduction.30,34Studieshaveshownthatadapalene organisms. However, somestudies could notconfirm has a dose-dependent effect on down-regulating the resistance problem following topical antibiotic expression of molecules important in the innate im- treatment.53Therearecurrentlymultiplenonantibiotic mune response, including toll-like receptor 2, B- therapies for acne with proven efficacy, and it is defensin4,andinterleukin-8,andincreasesexpression reasonableforclinicianstodevelopantibiotic-sparing ofCD1d.35,36Thishelpstoexplainthegreaterclinical approaches for this disease.45 Subantimicrobial-dose effectinpatientswithmoresevereacnereportedwith doxycycline is used in the treatment of acne due to A/BPO0.3%bySteinGoldetal.20Similarly,thepivotal anti-inflammatorypropertiesbutthistreatmenthasnot trialsofadapalenegel0.3%foundefficacysuperiorto been studied in detail regarding the possible adapalene0.1%acrossallmeasures,andbothdosages implicationsforantibioticresistance.54 were similarly tolerated.37,38 In the phase 3 study of BPO is the preferred topical antimicrobial agent adapalene gel 0.3%, the greatest improvements were due to the current climate of antimicrobial achieved in patients who had higher lesion counts at stewardship.2,3,14,45,47 BPO is a potent bactericidal baseline.37Thus,therearenowmoretreatmentoptions agent, with strong oxidative activity. In a review forpatientswithsevereinflammatoryacne.20Forthese article discussing management of acne in the era of patients,higherconcentrationretinoidtherapymaybe antimicrobial resistance, Tzellos et al state ‘‘overall, used as an option before adding systemic therapy. A BPO combined with topical or oral antibiotics once-daily topical agent can readily be added to the ortopicalretinoidsisthemostefficaciousevidence- patient’sexistingskincarehabitsandmaybepreferred basedtreatmentoptiontopreventthedevelopment by some patients who do not wish to use an oral of antibiotic resistance in patients with acne and to therapy.Asimpleregimenisalsobeneficialforpatient confer significant clinical improvement on patients adherence.39,40 who have already developed antibiotic-resistant Although there is a solid rationale and strong acne.’’55,56 However, there is an urgent need for an recommendations for use of topical retinoids in both antimicrobialagentwithbettertolerabilitythanBPO theEDFandAADguidelines,3,14astudyofprescribing inmonotherapyandfixedcombinationtherapies. practices during 2012-2014 reported that dermatolo- Systemic antibiotics are useful for moderate-to- gistsprescribedretinoidsforjust58.8%ofalmost75,000 moderatelysevereacne,buteffortsshouldbemade acnepatientsandnondermatologistsprescribedthem to limit the duration of therapy to 3-4 months.2,45-47 foronly32.4%ofcases.41Clinicianperceptionsofthe In our clinical experience, the top 3 factors to irritationpotentialoftopicalretinoidscanlimittheiruse consider when determining duration of antibiotic in practice.2,42 However, when present, most topical therapyincludetheseverityofacne,thepotentialfor retinoidsideeffectsresolvewithin2-3weeksandcan bacterial resistance, and the response to treatment. bemanagedbyuseofmoisturizers.2TableIIpresents Factors that make it difficult to limit the duration of strategiesthatcanbeemployedtominimizethelikeli- systemic antibiotic therapy include acne recurrence hoodofirritation.2,32,43,44 andpatientpreference. JAMACADDERMATOL Thiboutot etal S9 VOLUME78,NUMBER2 period of 4-6 months has been recommended to Reducingantibioticuseinacne:Real-worldstrategies reducerelapseandimproveremissionrates.Tanetal Topicaltherapy2,10,14 performed asystematic literature search to evaluate d First-lineacnetherapy=topicalretinoidsandBPO evidence supporting cumulative dosing for d Topical antibiotics should not be used as isotretinoin.61 Tan reported that the cumulative monotherapy dose is based on data from studies that were not B Rapiddevelopmentofresistance designed to evaluate the role of cumulative dose in d BPO6atopicalretinoidshouldbeaddediftopical relapse rates.61,63 Further, a retrospective chart antibioticisprescribed reviewof1453patientstreatedwithoralisotretinoin B Speedsresponseandachievessuperiorclearing showed that 22.4% required a second course of d AllstrainsofPacnesaresensitivetoBPO isotretinoin (follow-up $12 months, range 12 d Topicalretinoids(withorwithoutBPO)orazelaicacid months-5years)andthatdailyandcumulativedoses aretreatmentofchoiceformaintenance did not influence relapse as long as treatment was Systemictherapy continued for $2 months after complete resolution d Assessingrisk-benefitanalysisforsystemicantibiotics of acne.63 The authors suggest proceeding with shouldbalanceindividualneedversuspublicinterest treatment until full clearance, independent of the inpreservingantibioticeffectiveness cumulativedose.63Weagreethisisareasonableand B Antibiotics should be avoided when effective effective strategy for patients with severe acne. For alternativesareavailable those with moderate acne, full clearance can be d Oral antibiotics are indicated when inflammatory acne is not responding well to topical treatments achieved with lower cumulative doses. A rule of andacneinvolvingtrunkormultiplebodilyareas thumb may be to treat until full clearance plus an B Response to therapy should be evaluated at 6- additionalmonth. 8weeks Inadditiontotheneedfortreatmenttoremission B Targetdurationoftherapylessthan3-4months (dosagewillvarybyindividual),thereisalsoagoalof B AtopicalretinoidandBPOorazelaicacidcanbe maintaining remission. For maintaining remission, usedatdiscontinuationofantibiotic specific dosing has not been established by d Avoidsystemicantibioticmonotherapy high-quality clinical trials. Factors that have been d Subantimicrobialdoseantibiotics,whichhaveanti- implicated as higher risk for relapse include severe inflammatory actions, can be useful to minimize seborrhea, young age, family history of acne, potentialforresistance prepubertalacne,andtruncalacne.63-66 Similarly, although it has been suggested that highercumulative doses of oral isotretinoin may be Consensus recommendation 3: oral isotreti- needed for severe truncal acne, in our clinical noin should be first-line therapy for very se- experience severe truncal acne can usually be vere (cystic and conglobate) acne.2 Isotretinoin treated with the same dose as that for severe facial isahighlyefficaciousacnetreatment,proventoclear acne.Therearenoclearstatisticaldatasupportinga acne lesions, including nodules and cysts, and differentdose. achieve a prolonged remission period.57,58 It usually Consensus recommendation 5: acne flare has been recommended at a dose of 0.5-1.0 mg/kg with oral isotretinoin can be minimized by administeredoveraperiodof;4-6monthstoreacha initiating therapy at a low dose. Acne flare cumulative dose of 120-150 mg/kgda target that occurs in a small proportion of patients (up to 15%) has been recommended to reduce relapse and at the initiation of oral isotretinoin therapy.67 improveremissionrates.59,60However,moremodern The group reached consensus that starting with thinking is reflected in core principle 4.61 Systemic a low dose (0.5 mg/kg in the United States and corticosteroidsmaybeusedatinitiationoftherapyto #0.2mg/kginsomecountriesasreportedbyBorghi help speed lesion clearing. Many experts and etal)67reducesthelikelihoodofflare,althoughseveral researchers in the field think that isotretinoin use panelists felt that sometimes the propensity for should not be restricted to cases with demonstrated inflammatoryflareisindependentofdose. failuretoconventionaltherapy.62 Consensus recommendation 6:mostpatients Consensus recommendation 4: oral isotreti- with acne should receive maintenance therapy noin therapy should proceed until full clear- with a topical retinoid with or without BPO. ance of acne. Additional studies are needed to Topical antibiotics should not be used as acne define a total cumulative dose that maintains maintenance therapy. Topical retinoid mono- remission. After the introduction of oral isotreti- therapy may be sufficient in some cases, with noin, a threshold dose of 120-150 mg/kg over a BPO or an oral antibiotic added as needed.68-72 S10 Thiboutotet al JAMACADDERMATOL FEBRUARY2018 Thielitz et al were able to demonstrate that Consensusrecommendation9:aminorityof maintenance therapy with a topical retinoid women $25 years of age have acne lesions achieved sustained reductions in microcomedones, localized only to the lower face. Topical which in turn translated to fewer active acne retinoids with or without BPO are important lesions.71 Clinical trials with adapalene, A/BPO, components in therapy of adult acne. Thereis and tazarotene have shown significant superiority a clinical impression that women with acne have a over their respective vehicles when used as subtypeofacnethatisdifficulttotreatandprimarily maintenance therapy after successful acute phase driven by hormonal abnormalities. However, a therapy.69,70,72-74 Thielitz et al showed that good large-scale international study showed that 89% of results could be achieved with retinoid therapy womenhaveafacialdistributionofacnelesionsthat appliedeveryotherday,whichmightbeappealing is similar to adolescent acne (Fig 5).77 Further, for patients.71 Azelaic acid may be a maintenance analysis of clinical registration data for adapalene option for women with acne.31 and A/BPO have both shown good efficacy in the Consensus recommendation 7: azelaic acid adult female population.78,79 Adding skin care cream 20% or gel 15% is a useful acne regimens, such as moisturizers and pH-balanced treatment in pregnant women and patients cleansers, has been shown to improve both with acne and PIH. The group reached efficacy and tolerability for women.80 Long-term consensus that azelaic acid should be recommen- maintenance is particularly important in the adult ded as a second-line therapy3,14; however, femalepopulationbecausefrequentrecurrencesare dissenting panelists commented that it has a rela- common.Inaddition,dryandsensitiveskinismore tively high potential to cause irritation and aggra- common in this group, supporting use of strategies vate already inflamed skin. Further, it was noted to minimize irritation from topical treatments thatazelaicacidisnotavailableinallregionsofthe (application every other day initiation; short- world and is a risk category B drug in pregnancy. contact therapies; use of moisturizers and gentle, Although there was a consensus that azelaic acid is nonsoapcleansers).81,82 useful in patients with acne and PIH, data support- Oral therapies, including limited-duration ing its use in this setting are sparse.75 Kircik et al antibiotics, isotretinoin, and hormonal treatments, reported that azelaic acid gel 15% twice daily canbeusefulforadultfemaleacne.81,82Adiscussion improved both mild-moderate acne and PIH in 20 on the use of oral contraceptives and hormonal adults with Fitzpatrick skin type Vand VI. At study therapyisprovidedlaterinthissupplement. conclusion (week 16), PIH was cleared in 31% of Consensus recommendation 10: early and subjects and slight or mild improvement was noted effective treatment is important to minimize in 69% of subjects.75 potential risk for acne scarring. Acne lesions Consensus recommendation 8: at present, canevolveintomorepermanentscars,whichcanbe devices, including laser, intense pulsed light, either atrophic or hypertrophic. It is challenging to and photodynamic therapy should not be identify which patients will scar, but early considered first-line treatment for inflamma- administration of effective therapy can reduce one tory acne. Although laser and light devices have modifiableriskfactorforscarring:prolongeduncon- some benefit in the setting of acne, well-designed trolledacne.8,83-85Thereareanumberofriskfactors studiesevaluatingtheireffectivenessversusstandard thathavebeenlinkedtothedevelopmentofatrophic medical therapies are lacking.76 In addition, acnescars,includingsevereacne(althoughscarscan standardized regimenshavenot been agreedupon; occur even with mild acne), family history, extent multiple treatments are generally necessary (and and duration of inflammation, and (perhaps most costly), and the results are temporary.14 A recent important) the time to effective treatment of Cochrane database systematic review of light acne.8,83,84 Additional risk factors might include therapies in acne found ‘‘high-quality evidence on manipulation of lesions, onset of acne at a young the use of light therapies for people with acne is age,frequentrelapses,localizationtothetrunk,and lacking.’’76 In the AAD guidelines, Zaenglein et al ethnicity.8 Histologic data suggest that an early report that photodynamic therapy with a strong inflammatory response in the skin appears photosensitizer has the best supporting evidence tobeassociatedwithlessscarringthenmilderforms and shows great promise, but that more studies are of acne that demonstrate delayed inflammatory neededtooptimizethetreatmentregimen,including response.86 A tool to assess risk of acne scarring the optimal sensitizer, incubation time, and light was recently developed after a review of the source.14 literature and clinical trials and a modified Delphi