Pharmacological and surgical treatment of nonreproductive ......of PCOS.2-5,7,19,20 Most guidelines...

19
Clinical Endocrinology. 2018;89:535–553. wileyonlinelibrary.com/journal/cen | 535 © 2018 John Wiley & Sons Ltd Received: 29 April 2018 | Revised: 25 May 2018 | Accepted: 28 May 2018 DOI: 10.1111/cen.13753 REVIEW ARTICLE Pharmacological and surgical treatment of nonreproductive outcomes in polycystic ovary syndrome: An overview of systematic reviews Chau T. Tay 1,2 | Anju E. Joham 1,2 | Danielle S. Hiam 3 | Moustafa A. Gadalla 4,5 | Jyotsna Pundir 6,7 | Shakila Thangaratinam 7 | Helena J. Teede 1,2 | Lisa J. Moran 1,4 1 Monash Centre for Health Research and Implementation, School of Public Health and Preventive Medicine, Monash University, Melbourne, Vic., Australia 2 Department of Diabetes and Vascular Medicine, Monash Health, Melbourne, Vic., Australia 3 Institute of Health, Exercise and Sport, Victoria University, Melbourne, Vic., Australia 4 Robinson Research Institute, Discipline of Obstetrics and Gynaecology, University of Adelaide, Adelaide, SA, Australia 5 Department of Obstetrics and Gynaecology, Women’s Health Hospital, Assiut University, Assiut, Egypt 6 Centre of Reproductive Medicine, St Bartholomew’s Hospital, London, UK 7 Barts Research Centre for Women’s Health (BARC), Barts and the London School of Medicine and Dentistry, Queen Mary University of London, London, UK Correspondence Chau T. Tay, Monash Centre for Health Research and Implementation, School of Public Health and Preventive Medicine, Monash University, Melbourne, Vic., Australia. Email: [email protected] Funding information National Health and Medical Research Council; National Heart Foundation of Australia; CRE in PCOS entry level scholarship Summary Background: Polycystic ovary syndrome (PCOS) affects up to 13% women and is associated with significant complications. The quality of evidence supporting the recommendations on treatment of nonreproductive outcomes in PCOS is unknown. Objective: To summarize and appraise the methodological quality of systematic reviews and meta-analyses evaluating pharmacological and surgical treatments for nonreproductive outcomes in PCOS. Methods: A literature search from MEDLINE, EMBASE, CINAHL PLUS and PROSPERO was performed from inception until 15th of September 2017. Article selection, data extraction and quality appraisal of included reviews were performed in duplicate. A narrative synthesis of the findings was conducted. Results: This overview included 31 reviews. The quality was low for 7 (23%), moder- ate for sixteen (52%) and high for 8 reviews (26%). Two reviews assessed psychologi- cal outcomes. Metformin improved anthropometric (7 of 10 reviews), metabolic (4 of 14 reviews) and endocrine outcomes (3 of twelve reviews). Thiazolidinediones im- proved metabolic (2 of 5 reviews) and endocrine outcomes (one of 5 reviews) but worsened weight gain (5 of 5 reviews). Combined oral contraceptive pill (COCP) im- proved clinical hyperandrogenism (2 of 2 reviews). Statins improved lipid profile (3 of 3 reviews) and testosterone level (2 of 3 reviews). There was no conclusive evidence from included systematic reviews regarding the use of other interventions. Conclusions: There is reliable evidence regarding the use of metformin for anthropo- metric outcomes and COCPs for hyperandrogenism in women with PCOS but not for other interventions. There is significant gap in knowledge regarding the management of psychological outcomes in women with PCOS which needs further evaluation. KEYWORDS meta-analysis, overview, polycystic ovary syndrome, systematic review, treatment 1 | INTRODUCTION Polycystic ovary syndrome (PCOS) is a common endocrinopathy af- fecting up to 13% of reproductive-aged women. 1 PCOS is diagnosed based on the presence of 2 of the following 3 reproductive features: menstrual or ovulatory dysfunction, clinical or biochemical hyperan- drogenism and/or polycystic ovarian morphology on ultrasonogra- phy with exclusion of other causes of hyperandrogenism. 2-5 Whilst

Transcript of Pharmacological and surgical treatment of nonreproductive ......of PCOS.2-5,7,19,20 Most guidelines...

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Clinical Endocrinology. 2018;89:535–553. wileyonlinelibrary.com/journal/cen  | 535© 2018 John Wiley & Sons Ltd

Received:29April2018  |  Revised:25May2018  |  Accepted:28May2018DOI: 10.1111/cen.13753

R E V I E W A R T I C L E

Pharmacological and surgical treatment of nonreproductive outcomes in polycystic ovary syndrome: An overview of systematic reviews

Chau T. Tay1,2  | Anju E. Joham1,2  | Danielle S. Hiam3 | Moustafa A. Gadalla4,5 |  Jyotsna Pundir6,7 | Shakila Thangaratinam7 | Helena J. Teede1,2  | Lisa J. Moran1,4

1MonashCentreforHealthResearchandImplementation,SchoolofPublicHealthandPreventiveMedicine,MonashUniversity,Melbourne,Vic.,Australia2DepartmentofDiabetesandVascularMedicine,MonashHealth,Melbourne, Vic.,Australia3InstituteofHealth,ExerciseandSport,VictoriaUniversity,Melbourne, Vic.,Australia4RobinsonResearchInstitute,DisciplineofObstetricsandGynaecology,UniversityofAdelaide,Adelaide,SA,Australia5DepartmentofObstetricsandGynaecology,Women’sHealthHospital,AssiutUniversity,Assiut,Egypt6CentreofReproductiveMedicine, StBartholomew’sHospital,London,UK7BartsResearchCentreforWomen’sHealth(BARC),BartsandtheLondonSchoolofMedicineandDentistry,QueenMaryUniversityofLondon,London,UK

CorrespondenceChauT.Tay,MonashCentreforHealthResearchandImplementation,SchoolofPublicHealthandPreventiveMedicine,MonashUniversity,Melbourne,Vic.,Australia.Email:[email protected]

Funding informationNationalHealthandMedicalResearchCouncil;NationalHeartFoundationofAustralia;CREinPCOSentrylevelscholarship

SummaryBackground: Polycystic ovary syndrome (PCOS) affects up to13%womenand isassociatedwith significant complications. The quality of evidence supporting therecommendationsontreatmentofnonreproductiveoutcomesinPCOSisunknown.Objective: To summarize and appraise the methodological quality of systematicreviewsandmeta-analysesevaluatingpharmacologicalandsurgicaltreatmentsfornonreproductiveoutcomesinPCOS.Methods: A literature search from MEDLINE, EMBASE, CINAHL PLUS andPROSPEROwas performed from inception until 15th of September 2017. Articleselection,dataextractionandqualityappraisalofincludedreviewswereperformedinduplicate.Anarrativesynthesisofthefindingswasconducted.Results:Thisoverviewincluded31reviews.Thequalitywaslowfor7(23%),moder-ateforsixteen(52%)andhighfor8reviews(26%).Tworeviewsassessedpsychologi-caloutcomes.Metforminimprovedanthropometric(7of10reviews),metabolic(4of14reviews)andendocrineoutcomes (3of twelve reviews).Thiazolidinediones im-provedmetabolic (2of5 reviews)andendocrineoutcomes (oneof5 reviews)butworsenedweightgain(5of5reviews).Combinedoralcontraceptivepill(COCP)im-provedclinicalhyperandrogenism(2of2reviews).Statinsimprovedlipidprofile(3of3reviews)andtestosteronelevel(2of3reviews).Therewasnoconclusiveevidencefromincludedsystematicreviewsregardingtheuseofotherinterventions.Conclusions:Thereisreliableevidenceregardingtheuseofmetforminforanthropo-metricoutcomesandCOCPsforhyperandrogenisminwomenwithPCOSbutnotforotherinterventions.ThereissignificantgapinknowledgeregardingthemanagementofpsychologicaloutcomesinwomenwithPCOSwhichneedsfurtherevaluation.

K E Y W O R D S

meta-analysis,overview,polycysticovarysyndrome,systematicreview,treatment

1  | INTRODUC TION

Polycysticovarysyndrome(PCOS)isacommonendocrinopathyaf-fectingupto13%ofreproductive-agedwomen.1PCOSisdiagnosed

basedonthepresenceof2ofthefollowing3reproductivefeatures:menstrualorovulatorydysfunction,clinicalorbiochemicalhyperan-drogenismand/orpolycysticovarianmorphologyonultrasonogra-phywithexclusionofothercausesofhyperandrogenism.2-5Whilst

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theaetiology isnotfullyunderstood, insulinresistanceandhyper-androgenismarethe2keyhormonaldisturbancesthatunderpinthecondition.2,6,7

Polycystic ovary syndromehas a broad rangeof clinicalmani-festationsthatvaryacrossphenotypes,ethnicitiesand lifestages.Youngwomentypicallypresentwithdermatologicalcomplaints(hir-sutism or acne) or reproductive problems (oligo-/amenorrhoea orinfertility).4,8Metabolic features of PCOS include a predispositiontodevelopobesity,metabolicsyndrome,type2diabetes,hyperten-sionandnonalcoholicfatty liverdisease.9-12Psychologically,PCOSincreasestheriskofanxiety,depressionandlowqualityoflife.13-15 Thereare increasedpregnancycomplications includinggestationaldiabetes mellitus, gestational hypertension, preterm labour andpreeclampsiaandalso increased riskofendometrialneoplasia.16,17 ThesenonreproductivefeaturesinPCOScontributetoasignificanthealthandeconomicburden.18

The management of PCOS should encompass treating fertil-ity and nonreproductive outcomes such as reducing clinical symp-toms of hyperandrogenism, improvingmetabolic health, improvingpsychological well-being and preventing long-term health risks.6 Evidence-basedguidelinespublishedbytheAustralianPCOSAllianceandotherprofessionalspecialtysocietypositionstatementsrecom-mend lifestyle interventionsasfirst-linetreatmentforwomenwithPCOS.A5%-10%reductioninbodyweightiseffectiveinimprovinganthropometric, reproductive,metabolicandpsychological aspectsof PCOS.2-5,7,19,20Most guidelines discussed 3main pharmacologi-caltherapycategories,namelyinsulinsensitizers(eg,metforminand thiazolidinediones), anti-androgens (eg, spironolactone, flutamide and cyproterone acetate) and combined oral contraceptive pills(COCP).2-5,7,21,22 Bariatric surgery is also recommended for consider-ationinobesewomenwithPCOSgiventhatitisaneffectivemeansofweightreductionwhichmayimprovetheclinicalfeaturesofPCOS.2-5,7,23

However,thequalityofevidencesupportingtheserecommen-dationsforPCOS-relatednonreproductiveoutcomesisnotknown.Whiletherehasbeenan increasingnumberofsystematicreviewspublishedsummarizingtheevidenceofdifferentpharmacologicalorsurgicaltherapiesonthenonreproductiveoutcomesinPCOS,con-clusionsaredifficulttointerpretduetodiversemethodologiesandqualityofboththesystematicreviewsandtheirincludedstudies.

Theaimofthisstudywastoconductanoverviewofsystematicreviews evaluating pharmacological or surgical therapy for nonre-productiveoutcomes inwomenwithPCOS to summarize and ap-praisetheresultsandmethodologicalquality.

2  | METHODS

2.1 | Protocol and registration

This review was designed and reported in accordance with thePreferred Reporting Items for Systematic Reviews and Meta-Analyses(PRISMA)guidelines.24Anaprioristudyprotocolwasreg-isteredwithPROSPERO(CRD42016052649).Ethicsapplicationwasnotrequired.

2.2 | Literature search

TheelectronicdatabasesMEDLINEin-processandothernonindexedcitations(OvidMEDLINE(R)In-Process&OtherNon-IndexedCitations,OvidMEDLINE(R)DailyandOvidMEDLINE(R)1946toPresent),OvidEMBASE(EBMReviews—CochraneDatabaseofSystematicReviews2005to15September2017,EBMReviews—ACPJournalClub1991toSeptember2017,EBMReviews—DatabaseofAbstractsofReviewsofEffects1stQuarter2016,EBMreviews—CochraneCentralRegisterof Controlled Trials September 2017, EBM Reviews—CochraneMethodology Register 3rd quarter 2012, EBM Reviews—HealthTechnology Assessment 4th Quarter 2016, EBM Reviews—NHSEconomicEvaluationDatabase1stQuarter2016)andCINAHLPLUSweresearchedtoidentifyrelevantpublishedarticles.Additionalongo-ingreviewswereidentifiedfromsearchingtheinternationalprospec-tiveregisterofsystematicreviewsPROSPERO(http://www.crd.york.ac.uk/PROSPERO/).Theliteraturesearchwaslastupdatedonthe15th ofSeptember2017.The search termsused included “PCOS,” “poly-cysticovarysyndrome,”“Stein-Leventhal,”“systematic,”“review,”and“meta-analysis”withthecompletesearchstrategyforeachdatabaseprovided inAppendixS1 (found in theSupporting Information).Thesearchstrategywaslimitedtohumanstudiesonly.

2.3 | Eligibility criteria and study collection

Articleswereincludediftheymetthefollowinginclusioncriteria:originalsystematicreviewormeta-analysis;PCOSwastheprimaryfocusofthereviewwitharticlesinwhichPCOSwasasecondaryconditionassessedaspartofabroadertopicexcluded;clearsearchstrategywithatleastkeywordsortermsincluded,documentationofsearchreturnsandperformedqualityappraisaloftheincludedstudies; published in English; and published from year 2009 on-wardsgiventhiswaswhenthePRISMAstatementwaspublishedtoguidereportingofsystematicreviewsandmeta-analyses.24

The outcomes of interestwere anthropometric (weight, bodymass index (BMI), waist-hip ratio, waist circumference or bodycomposition), endocrine (total or free testosterone, sex hormonebinding globulin (SHBG), free androgen index (FAI), dehydroepi-androsteronesulphate(DHEAS),dehydroepiandrosterone(DHEA),androstenedioneorclinicalhyperandrogenism),metabolic(glucoseintolerance, surrogate markers of insulin resistance, lipid profileor blood pressure) and psychological (quality of life, anxiety ordepression).

2.4 | Study selection and data extraction

Identified articles from the literature searchwere screened in atwo-step process. First, the titles and abstracts were screenedforsuitability.Second,allarticlesthatmeettheinclusioncriteriafromthefirststepwereretrievedfordetailedfull-textassessmenttodetermineeligibility.Studyselectionwasperformed indepen-dentlyinduplicateby3investigators(C.T.T,D.S.HandL.J.M)withanydiscrepanciesresolvedbyconsensus.

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Datacollectedfromtheeligiblearticlesincludedauthorship,pub-licationyear,countryofauthors’origin,typesofstudyeligibleforthesystematicreview,dateofliteraturesearch,languagerestriction,ad-herencetoasystematicreviewguideline,presenceofmeta-analysis,the authors’ interpretation of quality assessment of the includedstudies,numberofincludedstudiesandparticipantsinvolvedandtheParticipant,Intervention,Comparison,OutcomesandStudies(PICOS)frameworkofthestudy. If theauthorsdidnot interpretthequalityoftheincludedstudiesnorsummarizetheoverallqualityoftheen-tirestudy,thesectiononqualityassessmentwasbedocumentedas“unclear.”Dataextractionwasconductedindependentlyinduplicate(C.T.T,L.J.MandM.A.G)withanydiscrepanciesresolvedbyconsensusanddiscussionwithathirdinvestigator(D.S.H).

2.5 | Quality assessment (AMSTAR)

The Assessing the Methodological Quality of Systematic Reviews(AMSTAR)toolwasemployedtoappraisethequalityoftheincludedsystematic reviews.25,26 AMSTAR evaluates the methodological as-pectsof systematic reviewsusing11 items: (i) theprovisionofanaprioridesign,(ii)duplicationofstudyselectionanddataextraction,(iii)conductionofacomprehensiveliteraturesearch,(iv)inclusionofgreyliteratureinthereview,(v)availabilityofalistoftheincludedandex-cludedstudies, (vi)descriptionof thecharacteristicsof the includedstudies, (vii) clear documentation of the scientific quality of the in-cluded studies, (viii) considerationof the scientificqualityof the in-cludedstudiesinformulatingconclusions,(ix)appropriateanalysisofresultsdependingonheterogeneity,(x)assessmentofpublicationbiasand(xi)considerationofconflictofinterestofboththesystematicre-viewandtheincludedstudies.26Eachitemwasgiven1pointifitwasdeterminedas“yes”and0point if itwasdeterminedas“no”or“notapplicable.”The reviewswerecategorizedas lowquality if the totalAMSTARscorewas≤3,moderatequality ifthetotalAMSTARscorewasbetween4to7,andhighqualityifthetotalAMSTARscorewas≥8.

Qualityassessmentofalleligiblesystematic reviewswascon-ductedindependentlyinduplicate(C.T.T,L.J.MandM.A.G)withanydisagreements resolvedby consensusanddiscussionwitha thirdinvestigator(D.S.H).

2.6 | Data synthesis

Anarrativesynthesisoffindingsfromtheincludedreviewswasper-formed.Resultswerepresentedaccordingtothedifferenttypesofintervention.Statisticallysignificantoutcomesofinterestwerepre-sentedifameta-analysiswasperformedbythereview.

3  | RESULTS

3.1 | Literature search

The electronic database search retrieved 978 articles, and an addi-tional60wereidentifiedfromPROSPERO.Afterremovingthedupli-cates,831articlesremainedforscreening.Atotalof564articleswere

excluded after reviewing the title and abstract leaving 267 articlesavailableforfull-textevaluation.Atotalof140articleswereeligibleforanalysisofwhich33wererelatedtotreatmentofnonreproductiveoutcomes.Ofthese,2articleswereapriorversionofasystematicre-view,andtherefore,weonlyincludedthemostrecentpublications.27,28 Finally,31systematicreviewswereincludedinthisstudy.ThePRISMAflowdiagramis illustrated inFigure1.The listofexcludedarticles isavailableinAppendixS2(foundintheSupportingInformation).

3.2 | Study characteristics

ThestudycharacteristicsandPICOframeworkoftheincludedsys-tematicreviewsaresummarizedinTable1.ThecountryoforiginoftheauthorsincludedChina(n=11),29-39Australia(n=6),40-45UnitedKingdom (n=5),43,45-48 the United States of America (n=4),49-52 India (n=3),44,52,53 Canada (n=3),50,54,55 Brazil (n=2),41,56 Iran (n=2),40,54Columbia(n=1),46Greece(n=1),57Italy(n=1),57Spain(n=1),58Scotland(n=1),59Luton(n=1),48Netherlands(n=1)41 and Saudi Arabia (n=1).46 Thirteen reviews explicitly included rand-omizedcontroltrials(RCTs)only29-32,34,36,38,42,43,46,53,57,59;5reviewsincluded RCTs and phase-1 data of cross-over trials39,41,44,45,52; 2 reviews included RCTs and prospective trials50,56; 2 reviews in-cluded RCTs and observational studies49,58; 1 review included RCTs, comparative studies and case series with >5 patients55; 2 reviews includedallclinical trials40,54;3 reviews includedall studytypes35,48,51;and3reviewsdidnotstateaninclusioncriteriaforthestudytype.33,37,47Fifteenreviewsdidnotsetalanguagerestrictionin their literature search30,31,39-41,43-46,49,50,52,56-58; 11 reviews re-strictedtheirsearchtoEnglishpublicationsonly32,34-38,42,51,53,55,59; 1reviewrestricteditslanguagetoEnglishandPersian54; 1 review re-stricteditslanguagetoEnglishandChinese33;and3reviewsdidnotstateifanylanguagerestrictionwasapplied.29,47,48Twelvereviewsreportedfollowingaguidelineongoodpracticeinconductingsys-tematic reviews30,31,35,39,41,44-47,53,57,58; 25 reviews included meta-analyses29-38,41-47,49-53,55-57; and18 reviewsdidnotprovideaclearstatementastotheoverallqualityassessmentoftheincludedarti-cles.31,33,34,36,37,41-44,47,51-58Thenumberofstudiesincludedineachsystematic review ranged from1 to35, and the total participantsrangedfrom16to3992.Eighteen(58%)ofthesystematicreviewshadlessthan10studiesincludedintotal.29-32,36,38-42,44,46-48,52,56,57,59

3.3 | Methodological quality of systematic reviews

TheAMSTARscoresoftheincludedsystematicreviewsareprovidedinAppendixS3(foundintheSupportingInformation).Majorityoftheincludedsystematicreviewswereoflow(n=7;23%)42,47,48,54,55,58,59 to moderate quality (n=16; 52%)29-34,36,37,39,40,43,49-51,53,56 withonly8gradedhighquality (n=8;26%).35,39,41,44-46,52,57Commonlyunreported itemswereconsiderationof conflictof interestof theincludedstudies(n=28;90%),presenceofanaprioristudydesign(n=23; 74%), a list of the excluded articles (n=23; 74%), inclu-sionofgrey literature (n=22;71%),duplicationofstudyselectionor data extraction (n=21; 68%), formulation of study conclusion

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basedonthescientificqualityoftheincludedstudies(n=18;58%)andconductionofacomprehensiveliteraturesearch(n=18;58%).Assessmentofpublicationbiaswasnotappropriatelyperformedin9 reviews (29%),documentationof thescientificqualityof the in-cluded studieswasunsatisfactory in6 reviews (19%), andhetero-geneitywasnot taken intoaccountby2 reviews (6%).All reviewsreportedthestudycharacteristicsoftheincludedstudies.

3.4 | Types of intervention

The typesof treatments assessedweremetformin, thiazolidinedi-one,oralcontraceptivepills(OCP),anti-androgens,statins,orlistat,bariatric surgery and antidepressants. Nonconventional therapiessuchasvitaminD,inositol,N-acetyl-cysteineandantioxidantswerealsoincludedinthisreview.

3.4.1 | Insulin sensitizer: metformin

Sixteen reviews evaluated the efficacy of metformin(Table2).29,30,32,34-36,38,41,43,45,46,49,53,56,57,59 Five were rated highquality,10wereratedmoderatequality,and1wasratedlowquality.

A total of 174 trials and10525 adolescent and adult participantswere involved.

Anthropometricoutcomeswereassessedby10reviews.Sevenreviews (n=3 comparing metformin vs thiazolidinediones,29,30,34 n=2 comparing metformin vs placebo,45,53 n=1 comparing met-forminvsCOCPs46andn=1comparingcombinationtherapywithmetformin and clomiphene citrate vs clomiphene citrate alone)59 reportedresultsfavouringmetforminintermsofBMIand/orwaist-hipratio.Therewasnosignificantdifferenceinanthropometricout-comeswhenmetforminwascompared toacarbose38ororlistat,56 orwhencombinationtherapywithmetforminandstatinwascom-pared to metformin alone.36 Endocrine outcomes were assessedby 12 reviews. Three reviews (n=2 comparingmetformin vs pla-cebo45,53 and n=1 comparing metformin and clomiphene citratevsclomiphenecitratealone59) reportedreductions intestosteronewhenusingmetformin.Therewasno significantdifference in en-docrine outcomes whenmetformin was compared to acarbose,38 OCP,46vitaminD,32,57thiazolidinediones,29,30,34orlistat,56inositol43 or combination therapy with statin.36 Metabolic outcomes wereassessed by 14 reviews with 4 reviews reporting beneficial out-comes favouringmetformin for theprevalenceof type2diabetes

F IGURE  1 Studyselectionprocess

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mellitusorprediabetes(n=1comparingmetforminvsOCP),46totalcholesterol and low-density lipoprotein (LDL) (n=1 comparingmetformin vsOCP),46 blood pressure (n=2 comparingmetforminvs placebo),45,53 triglycerides (n=1 comparing metformin vs pla-cebo,53n=1comparingmetforminvsthiazolidinediones),34glucose(n=1comparingmetforminvsplacebo),45 insulin (n=1comparingmetforminvsplacebo)45andglucose/insulinratio(n=1comparingmetformin vs placebo).53No significantmetabolic outcomesweredetected when comparing metformin to vitamin D,32,57 orlistat,56 inositol,43 acarbose38 orwith the additionofmetformin to folliclestimulatinghormone (FSH)-containinggonadotrophinovulation in-ductionorclomiphenecitrate.59Psychologicaloutcomeswerenotassessedbyanyoftheabovereviews.

3.4.2 | Insulin sensitizer: thiazolidinediones

Fivereviews29-31,34,45evaluatedtheefficacyofthiazolidinedionesinwhichonewashighqualityand4weremoderatequality(Table2).Atotalof74trialsand5282participantswithPCOSwereinvolved.All5reviewsassessedtheanthropometric,endocrineandmetabolicout-comesofthiazolidinediones(n=3comparedwithmetformin,29,30,34 n=2comparedwithplacebo).31,45BMIwassignificantlyincreasedwith thiazolidinediones in all 5 reviews while endocrine benefits(reducedfreetestosterone)werereportedinonereviewwhencom-paredtometformin.34Formetabolicoutcomes,onereviewshowedimprovedfastingglucoseandinsulinincomparisonwithplacebo,31 one review showed improved fasting insulin and homoeostaticmodelassessmentofinsulinresistance(HOMA-IR)whencomparedto metformin,30 and one review showed worsened triglycerideswhencomparedtometformin.34Psychologicaloutcomeswerenotassessedbyanyoftheabovereviews.

3.4.3 | Insulin sensitizer: inositol

Three reviews43,45,48 evaluated the efficacy of inositol (Table2).The reviewswereof low (n=1),moderate (n=1)andhigh (n=1)quality.Atotalof62trialswith5072womenwithPCOSwerein-volved. In all 3 reviews, inositol was compared against placebo.Anthropometric outcomes were reported by 2 reviews with onereview reporting reduced BMI and waist-hip ratio.48 Endocrineoutcomeswereassessedbyall3reviewswith2ofthesereportingbenefits(testosterone,DHEASorandrostenedione).43,48Metabolicoutcomeswerealsoassessedbyall3reviewswith2reviewsreport-ingreducedinsulin,43,48onereviewreportingreducedglucoseandHOMA-IR,43 and one review reporting improved blood pressure,triglycerides and high-density lipoprotein (HDL).48 Psychologicaloutcomeswerenotassessedbyanyoftheabovereviews.

3.4.4 | Hormonal therapy: combined oral contraceptive pill

The efficacy of COCPs was assessed by 4 reviews46,49,50,58 (Table3) of low to high quality (n=1 high, n=2moderate, and

n=1 low). Results from88 trials involving3722 adolescent andadult women with PCOS were analysed. Anthropometric out-comes were reported by one review with COCP being associ-atedwitha lesserreductionofBMIcomparedwithmetformin.46 Endocrineoutcomeswereassessedby2reviewswithonereport-ing greater acne reduction when compared to metformin46 and one review reporting general improvement in clinical hyperan-drogenismwhenusingCOCPasmonotherapyor in combinationwithmetformin.58 Two reviews assessedmetabolic outcomesofwhichonereviewreportedthatCOCPusewaslesseffectivethanmetformininreducingtheprevalenceofdysglycaemia,totalcho-lesterolandLDL,46andonereviewreportedthatCOCPusewasassociatedwith increasedHDL and triglycerides comparedwithbaseline.50Psychologicaloutcomeswerenotassessedbyanyoftheabovereviews.

3.4.5 | Hormonal therapy: anti- androgens

Onehigh-qualityreviewevaluatedthesideeffectsofanti-androgensandtheirefficacyonmetabolicoutcomes(Table3).49Nosignificanteffectsonmetabolicoutcomeswerereported.

3.4.6 | Weight loss therapy: orlistat

Orlistatwasevaluatedbyonemoderatequalityreviewincompari-sonwithplacebo,metforminorotheranti-obesitydrugs56(Table4)where9trialsand602adolescentandadultwomenwithPCOSwereinvolved.Meta-analysisofthestudiescomparingorlistattoplacebowasnotpossiblebutthesystematicreviewreportedimprovementsin anthropometric (BMI, weight, waist circumference or waist-hipratio), endocrine (testosterone) andmetabolicoutcomes (triglycer-ides,HDL,LDL,HOMA-IRandinsulin).Meta-analysisofthestudiescomparingorlistattometforminshowednosignificantdifferences.56 Psychologicaloutcomeswerenotassessedbytheabovereview.

3.4.7 | Weight loss therapy: bariatric surgery

TheeffectofbariatricsurgeryinwomenwithPCOSwasevaluatedin 2 low-quality reviews47,55 (Table4). They involved 19 trials and2394participantswithandwithoutPCOS.Bothreviewscomparedthesamegroupofwomenbeforeandafterbariatricsurgery.Bothreviewsassessedanthropometricandendocrineoutcomesandre-portedreductionsinBMI,percentageofexcessweightlossandhir-sutism.47,55Metabolicoutcomeswereassessedbyonereviewandshowedreductionsinbloodpressure,improvementindyslipidaemia,normalizationofglucose levels, improvementofglycaemiccontrolandresolutionoftype2diabetesmellitus.47Psychologicaloutcomeswereassessedbyonereviewandreportedbenefitsindepression.47

3.4.8 | Other therapy: statins

Three reviews evaluated the efficacy of statins36,42,44 (AppendixS3, found in the Supporting Information) with rating of one low,

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TABLE 1 Studycharacteristics

Aut

hor (

y)Co

untr

yIn

clud

ed s

tudy

type

Dat

e of

last

lit

erat

ure

sear

chLa

ngua

ge

Syst

emat

ic

revi

ew

guid

elin

e fo

llow

ed

Met

a-

anal

ysis

pe

rfor

med

Num

ber o

f in

clud

ed

pape

rs

Tota

l num

ber

of in

clud

ed

part

icip

ants

Popu

latio

n an

d PC

OS

diag

nost

ic c

riter

ia

AlKhalifahetal

(2016)

46Canada,Saudi

Arabia,Columbia,

UnitedKingdom

RCTs

15-Jan

All

Yes

Yes

417

0Adolescents(11-19y)

ESHRE/ASRM

Aminietal(2015)54

Iran

Experimentalor

quasiexperimental

trials

13-Nov

English,

Persian

No

No

1183

4Ir

ania

n ESHRE/ASRM

Azadi-Yazdietal

(2017)

40Iran,Australia

Clinicaltrials

17-Jan

All

No

No

618

3Diagnosticcriterianotstated

Bordewijketal

(2017)

41Netherlands,

Australia,Brazil

RCTsandphase1of

cross-overtrials

16-Sep

All

Yes

Yes

526

4Anovulatorywomen

undergoingovulationinduction

withFSHESHRE/ASRM

Butterworthetal

(2016)

47UnitedKingdom

Notstated

15-Mar

Notstated

Yes

Yes

626

4ESHRE/ASRM

Domecqetal

(2013)

49UnitedStates

RCTsandcomparative

observationalstudies

11-Apr

All

No

Yes

2213

35Diagnosticcriterianotstated

Duetal(2012)31

China

RCTs

12-Jun

All

Yes

Yes

828

6ESHRE/ASRM

Duetal(2012)29

China

RCTs

12-Feb

Notstated

No

Yes

626

7ESHRE/ASRM

Duetal(2012)30

China

RCTs

11-Nov

All

Yes

Yes

627

8ESHRE/ASRM

Fangetal(2017)32

China

RCTs

15-Dec

English

No

Yes

950

2ESHRE/ASRM

Galazisetal

(2011)

48UnitedKingdom,

Luton

Allstudytypes

10-Jul

Notstated

No

No

847

9Diagnosticcriterianotstated

Gaoetal(2012)42

Australia

RCTs

11-Sep

English

No

Yes

425

4Diagnosticcriterianotstated

Gilletal(2014)59

Scotland

RCTs

13-May

English

No

No

412

9Clomipheneresistantwomen

Diagnosticcriterianotstated

Graffetal(2016)56

Brazil

RCTsandprospective

studies

15-May

All

No

Yes

960

2Withoutpre-existingdiabetes,

13-44y

ESHRE/ASRM

Halperinetal

(2011)

50Canada,United

States

RCTsandprospective

cohorts

10-Apr

All

No

Yes

3579

8Withoutpre-existingdiabetes,

13-44y

ESHRE/ASRM

Heetal(2015)51

UnitedStates

Allstudytypes

15-Jan

English

No

Yes

30 (7regarding

intervention)

3182

(2

83

includedfor

intervention)

ESHRE/ASRM

Jiaetal(2015)33

China

Notstated

14-Sep

English,

Chinese

No

Yes

1723

97ESHRE/ASRM

Page 7: Pharmacological and surgical treatment of nonreproductive ......of PCOS.2-5,7,19,20 Most guidelines discussed 3 main pharmacologi-cal therapy categories, namely insulin sensitizers

     |  541TAY eT Al.

Aut

hor (

y)Co

untr

yIn

clud

ed s

tudy

type

Dat

e of

last

lit

erat

ure

sear

chLa

ngua

ge

Syst

emat

ic

revi

ew

guid

elin

e fo

llow

ed

Met

a-

anal

ysis

pe

rfor

med

Num

ber o

f in

clud

ed

pape

rs

Tota

l num

ber

of in

clud

ed

part

icip

ants

Popu

latio

n an

d PC

OS

diag

nost

ic c

riter

ia

Lietal(2011)34

China

Parallel-group

designedRCTs

10-May

English

No

Yes

1045

9Diagnosticcriterianotstated

Mendozaetal

(2014)

58Spain,Italy

RCTs,nonrandomized

studiesand

noncontrolled

studies

13-Oct

All

Yes

No

2715

89Diagnosticcriterianotstated

Mengetal(2016)35

China

Allstudytypes

15-Dec

English

Yes

Yes

34 (7regarding

interven-

tion)

3117

(1

41

includedfor

intervention)

ESHRE/ASRM

Pateletal(2017)53

Indi

aRCTs

16-May-

English

Yes

Yes

1459

316-45y(excludepregnancyor

clomipheneresistant)

Diagnosticcriterianotstated

Pergialiotisetal

(2017)

57Greece

RCTs

16-Sep

All

Yes

Yes

964

7Diagnosticcriterianotstated

Pundiretal(2017)43

UnitedKingdom,

Australia

RCTs

16-Aug-

All

No

Yes

1060

1Diagnosticcriterianotstated

Ravaletal(2011)44

India,Australia

RCTsandphase1of

cross-overtrials

11-Jul

All

Yes

Yes

424

4ESHRE/ASRM

Skublenyetal

(2016)

55Canada

RCTs,comparison

studies,andcase

series>5patients

Notstated

English

No

Yes

1321

30WomenwithorwithoutPCOS

Diagnosticcriterianotstated

Sunetal(2015)36

China

RCTs(excludingtrails

comparingstatins

withOCPorother

statins)

14-Oct

English

No

Yes

928

2Diagnosticcriterianotstated

Tangetal(2012)45

UnitedKingdom,

Australia

RCTsandphase1of

cross-overtrials

11-Oct

All

Yes

Yes

4439

92Oligo-oranovulatory

ESHRE/ASRM

Thakkeretal

(2015)

52India,UnitedStates

RCTsandphase1of

cross-overtrials

13-Sep

All

No

Yes

891

0ESHRE/ASRM

Xueetal(2017)37

China

Notstated

16-Apr

English

No

Yes

1685

5ESHRE/ASRM

Zhangetal(2014)38

China

RCTs

13-Sep

English

No

Yes

626

3ESHRE/ASRM

Zhuangetal

(2013)

39China

RCTsandphase1of

cross-overtrials

12-Jun

All

Yes

No

116

ESHRE/ASRM

RCT,randomizedcontroltrials;ESHRE,EuropeanSocietyofHumanReproductionandEmbryology;ASRM,AmericanSocietyforReproductive

Medicine;OCP,oralcontraceptivepill.

Page 8: Pharmacological and surgical treatment of nonreproductive ......of PCOS.2-5,7,19,20 Most guidelines discussed 3 main pharmacologi-cal therapy categories, namely insulin sensitizers

542  |     TAY eT Al.

TABLE 2 Resultsofsystematicreviewsregardinginsulinsensitizers

Revi

ews

AM

STA

RQ

ualit

y of

in

clud

ed s

tudi

esO

utco

mes

ass

esse

dCo

mpa

rison

Sign

ifica

nt re

sults

Metformin

AlKhalifahetal

(2016)

46High

Verylowtolow

Anthropometric

BMI

MetforminvsOCP

Anthropometric

BMI(WMD−4.02,95%CI−5.23to−2.81)

Reproductive

Hirsutism,acne,

testosterone

Reproductive

Acnescores(W

MD0.3,95%0.05to0.55)

a

Metabolic

Dysglycaemia,

cholesterol,TG,

HDL,LDL

Metabolic

Dysglycaemia(riskratio0.41,95%CI0.19to

0.86)

Cholesterol(W

MD−43.23,95%CI−64.15to

−22.32)

LDL(WMD−35.5,95%CI−57.45to−13.33)

Psychologic

–N

A

Bordewijketal

(2017)

41High

Unclear

Anthropometric

–Metformin+

ovulation

inductionvs

ovulation

induction

Reproductive

Metabolic

Insulin,glucose

Psychologic

Mengetal

(2016)

35High

RCTs:lowto

moderateriskof

bias;observa-

tionalstudies:

highriskofbias

Anthropometric

–Metforminvsno

treatment

NA

Reproductive

Metabolic

Psychologic

Pergialiotisetal

(2017)

57High

Unclear

Anthropometric

–Metformin±vitD

vsvitaminD

NA

Reproductive

DHEAS,SHBG

Metabolic

Glucose,insulin

Psychologic

Tangetal

(2012)

45High

Verylowtolow

Anthropometric

BMI,waist-hipratio

Metforminvs

plac

ebo

Anthropometric

Waist-hipratio(MD−0.01,95%CI−0.01to

0.00)

Reproductive

Testosterone,SHBG

Reproductive

Totaltestosterone(MD−0.60,95%CI−0.73to

−0.48)

Metabolic

BP,glucose,insulin,

cholesterol,TG

Metabolic

SystolicBP(MD−3.59,95%CI−5.13to−2.04)

Glucose(MD−0.15,95%CI0.25to−0.06)

Insulin(MD−3.51,95%CI−6.50to0.53)

Psychologic

Domecqetal

(2013)

49Moderate

RCTs:lowto

moderateriskof

bias;observa-

tionalstudies:

highriskofbias

Anthropometric

–Metformin(no

comparators)

NA

Reproductive

Metabolic

Psychologic

(Con

tinue

s)

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     |  543TAY eT Al.

Revi

ews

AM

STA

RQ

ualit

y of

in

clud

ed s

tudi

esO

utco

mes

ass

esse

dCo

mpa

rison

Sign

ifica

nt re

sults

Duetal(2012)29

Moderate

High

Anthropometric

BMI

Metforminvs

thiazolidinediones

Anthropometric

BMI(SMD−0.4,95%CI0.16to0.65)

Reproductive

Testosterone

Metabolic

Glucose,HOMA-IR

Psychologic

Duetal(2012)30

Moderate

Verylowtolow

Anthropometric

BMI

Metforminvs

pioglitazone

Anthropometric

BMI(SMD−0.25,95%CI0.01to0.49)

Reproductive

Testosterone,hirsutism

Metabolic

Insulin(SMD0.37,95%CI−0.61to−0.13)a

HOMA-IR(SMD0.32,95%CI−0.57to−0.06)a

Metabolic

Glucose,insulin,

HOMA-IR

Psychologic

Fangetal

(2017)

32Moderate

Lowtomoderate

riskofbias

Anthropometric

–Metforminvs

vitaminD

NA

Reproductive

Metabolic

Cholesterol,TG,HDL,

LDL,insulin,glucose,

QUICKI,HOMA-IR

Psychologic

Graffetal

(2016)

56Moderate

Unclear

Anthropometric

BMI,weight,waist

circumference

Metforminvs

orlistat

NA

Reproductive

Testosterone

Metabolic

Insulin,HOMA-IR,

cholesterol,TG,HDL,

LDL

Psychologic

Lietal(2011)34

Moderate

Unclear

Anthropometric

BMI

Metforminvs

thiazolidinediones

Anthropometric

BMIat3-mo(SMD−2.47,95%CI−3.33to−1.62)

BMIat6-mo(SMD−0.70,95%CI−0.76to

−0.65)

Reproductive

Hirsutism,androsten-

edione,testosterone,

DHEA

Reproductive

Freetestosterone(SMD0.36,95%CI−0.03to

−0.69)

a

Metabolic

Glucose,insulin,

HOMA-IR,HDL,LDL,

TG

Metabolic

TGat6-mo(SMD−1.13,95%CI−1.68to−0.57)

Psychologic

TABLE 2 (Continued)

(Con

tinue

s)

Page 10: Pharmacological and surgical treatment of nonreproductive ......of PCOS.2-5,7,19,20 Most guidelines discussed 3 main pharmacologi-cal therapy categories, namely insulin sensitizers

544  |     TAY eT Al.

Revi

ews

AM

STA

RQ

ualit

y of

in

clud

ed s

tudi

esO

utco

mes

ass

esse

dCo

mpa

rison

Sign

ifica

nt re

sults

Pateletal

(2017)

53Moderate

Unclear

Anthropometric

BMI,waist-hipratio

Metforminvs

plac

ebo

Anthropometric

BMI(MD−1.18,95%CI−2.0to−0.36)

WHR(MD−0.02,95%CI−0.03to0.00)

Reproductive

Hirsutism,testosterone,

freetestosterone,

FAI,SHBG,DHEAS

Reproductive

Testosterone(MD−14.32,95%CI−26.80to

−1.85)

Metabolic

Bloodpressure,

cholesterol,TG,HDL,

LDL,

glucose,insulin,

glucose/insulinratio,

HOMA-IR,

QUICKI

Metabolic

SystolicBP(MD−4.92,95%CI−7.51to−2.33)

DiastolicBP(MD−1.51,95%CI−2.23to−0.79)

TG(MD−10.74,95%CI−17.93to−3.56)

Glucose/insulinratio(MD2.28,95%CI1.16to

3.41)

Psychologic

Pundiretal

(2017)

43Moderate

Unclear

Anthropometric

–Metforminvs

inositol

NA

Reproductive

Androstenedione,

testosterone,DHEAS,

SHBG

Metabolic

Insulin,glucose,

glucose/insulinratio,

HOMA-IR

Psychologic

Sunetal(2015)36

Moderate

Unclear

Anthropometric

BMI

Metformin+statin

vsmetformin

Metabolic

Totalcholesterol(SMD−1.28,95%CI−1.59to

−0.97)

LDL(SMD−0.74,95%CI−1.03to−0.44)

TG(SMD−1.37,95%CI−2.46to−0.28)

Reproductive

Testosterone,andros-

tenedione,DHEAS,

SHBG,FAI

Metabolic

Cholesterol,LDL,HDL,

TG,glucose,insulin,

HOMA-IR

Psychologic

Zhangetal

(2014)

38Moderate

Poor

Anthropometric

BMI

Metforminvs

acarbose

NA

Reproductive

Hirsutism,testosterone

Metabolic

TG,HDL

Psychologic

TABLE 2 (Continued)

(Con

tinue

s)

Page 11: Pharmacological and surgical treatment of nonreproductive ......of PCOS.2-5,7,19,20 Most guidelines discussed 3 main pharmacologi-cal therapy categories, namely insulin sensitizers

     |  545TAY eT Al.

Revi

ews

AM

STA

RQ

ualit

y of

in

clud

ed s

tudi

esO

utco

mes

ass

esse

dCo

mpa

rison

Sign

ifica

nt re

sults

Gilletal(2014)59

Low

3high,1low

Anthropometric

BMI

Metformin+

clomiphenevs

clomiphene

Anthropometric

2trials:BMIwasdecreased

Reproductive

SHBG,testosterone

Reproductive

2trials:testosteronewasdecreased

Metabolic

Insulin

Psychologic

Thiazolidinediones

Tangetal

(2012)

45High

Verylowtolow

Anthropometric

BMI,waist,hipratio

Rosiglitazonevs

plac

ebo

Anthropometric

BMI(MD+0.68,95%CI0.40to0.96)

Reproductive

Testosterone,SHBG

Pioglitazonevs

plac

ebo

NA

Metabolic

BP,glucose,insulin,

cholesterol,TG

Psychologic

Duetal(2012)31

Moderate

Unclear

Anthropometric

BMI

Thiazolidinediones

vsplacebo

Anthropometric

BMI(SMD+0.39,95%CI0.13to0.66)

Reproductive

Hirsutism,testosterone

Metabolic

Insulin(SMD−0.81,95%CI−1.5to−0.12)

Glucose(SMD−0.55,95%CI−1.06to−0.05)

Metabolic

Glucose,insulin

Psychologic

Duetal(2012)30

Moderate

Verylowtolow

Anthropometric

BMI

Pioglitazonevs

metformin

Anthropometric

BMI(SMD0.25,95%CI0.01to0.49)

a

Reproductive

Hirsutism,testosterone

Metabolic

Insulin(SMD−0.37,95%CI−0.61to−0.13)

HOMA-IR(SMD−0.32,95%CI−0.57to−0.06)

Metabolic

Glucose,insulin,

HOMA-IR

Psychologic

Duetal(2012)29

Moderate

High

Anthropometric

BMI

Thiazolidinediones

vsmetformin

Anthropometric

BMI(SMD0.4,95%CI0.16to0.65)

a

Reproductive

Testosterone

Metabolic

Glucose,HOMA-IR

Psychologic

TABLE 2 (Continued)

(Con

tinue

s)

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546  |     TAY eT Al.

Revi

ews

AM

STA

RQ

ualit

y of

in

clud

ed s

tudi

esO

utco

mes

ass

esse

dCo

mpa

rison

Sign

ifica

nt re

sults

Lietal(2011)34

Moderate

Unclear

Anthropometric

BMI

Thiazolidinediones

vsmetformin

Anthropometric

BMIat3-mo(SMD2.47,95%CI−3.33to−1.62)a

BMIat6-mo(SMD0.70,95%CI−0.76to−0.65)a

Reproductive

Hirsutism,androsten-

edione,testosterone,

DHEA

Reproductive

Freetestosterone(SMD−0.36,95%CI−0.03to

−0.69)

Metabolic

Glucose,insulin,

HOMA-IR,cholesterol,

TG,HDL,LDL

Reproductive

TGat6-mo(SMD1.13,95%CI−1.68to−0.57)a

Psychologic

Inositol

Tangetal

(2012)

45High

Verylowtolow

Anthropometric

BMI,waist,hipratio

D-chiro-inositolvs

plac

ebo

NA

Reproductive

Testosterone,SHBG

Metabolic

BP,glucose,insulin,

cholesterol,TG

Psychologic

Pundiretal

(2017)

43Moderate

Unclear

Anthropometric

–Inositol(myo-or

di-chiroisomers)

vsplacebo

Reproductive

Androstenedione(SMD−1.6,95%CI−2.3to

−0.6)

Totaltestosterone(SMD−3.3,95%CI−5.1to

−1.5)

DHEAS(SMD−3.2,95%CI−5.7to−0.6)

Reproductive

Androstenedione,

testosterone,DHEAS,

SHBG

Metabolic

Insulin(SMD−2.1,95%CI−3.2to−0.9)

Glucose(SMD−1.0,95%CI−1.7to−0.2)

HOMA-IR(SMD−1.8,95%CI−2.6to−1.0)

InsulinAUC(SMD−1.6,95%CI−2.8to−0.4)

Glucose/insulinratio(SMD2.9,95%CI2.2to

3.6)

Metabolic

Insulin,glucose,

glucose/insulinratio,

HOMA-IR

Psychologic

Galazisetal

(2011)

48Low

4low,4high

Anthropometric

Notspecified

D-chiro-inositolvs

plac

ebo

Anthropometric

2trials:improvedBMI,waist-hipratio

Reproductive

Reproductivesteroids

Reproductive

3trials:reducedtestosterone

Metabolic

BP,cholesterol,insulin

sensitivity

Metabolic

3trials:reducedinsulin,BP,TG

Psychologic

–1trial:increasedHDL

NA,notavailable;MD,meandifference;WMD,weightedmeandifference;SMD,standardizedmeandifference;CI,confidenceinterval;BMI,bodymassindex;SHBG,sexhormonebindingglobulin;FAI,

freeandrogenindex;DHEA,dehydroepiandrosterone;DHEAS,dehydroepiandrosteronesulphate;BP,bloodpressure;HDL,high-densitylipoprotein;LDL,low-densitylipoprotein;TG,triglycerides;

HOMA-IR,homoeostaticmodelassessmentofinsulinresistance;QUIKI,quantitativeinsulinsensitivitycheckindex;AUC,areaunderthecurve;OCP,oralcontraceptivepill.

a Resultslessbeneficialthancomparator.

TABLE 2 (Continued)

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     |  547TAY eT Al.

TABLE 3 Resultsofsystematicreviewsregardinghormonaltherapies

Revi

ews

AM

STA

RQ

ualit

y of

in

clud

ed s

tudi

esO

utco

mes

ass

esse

dCo

mpa

rison

Sign

ifica

nt re

sults

Oralcontraceptivepills

AlKhalifahetal

(2016)

46High

Verylowtolow

Anthropometric

BMI

OCPvs

metformin

Anthropometric

BMI(WMD4.02,95%CI−5.23

 to−2.81)

a

Reproductive

Hirsutism,acne,testosterone

Reproductive

Acnescores(W

MD−0.3,95%

 0.05to0.55)

Metabolic

Dysglycaemia,cholesterol,TG,HDL,

LDL

Metabolic

Dysglycaemia(riskratio0.41,

 95%CI0.19to0.86)

a

Cholesterol(W

MD43.23,

 95%CI−64.15to−22.32)

a

LDL(WMD35.5,95%CI−57.45

 to−13.33)a

Psychologic

Domecqetal(2013)49

Moderate

RCTs:lowto

moderaterisk

ofbias;

observational

studies:high

riskofbias

Anthropometric

Weight,BM

IOCP(no

com

para-

tor)

NA

Reproductive

Metabolic

Fastingglucose,postprandialglucose,

glucosetolerancetest,random

glucose,areaunderthecurveof

glucose,glucose/insulinratio,

HOMA-IR,QUICKI

Psychologic

Halperinetal(2011)50

Moderate

17high,9

moderate,16

low

Anthropometric

–Pre-vs

post-OCP

Metabolic

HDL(SMD0.46,95%CI0.14to

0.78)

TG(SMD0.55,95%CI0.17to

0.93)

Reproductive

Metabolic

Insulin,glucose,cholesterol,TG,HDL,

LDL,hyperinsulinemiceuglycaemic

clamp(m-value),glucose/insulinratio,

HOMA-IR

Psychologic

Mendozaetal

(2014)

58Low

Unclear

Anthropometric

BMI,weight

OCP±

metformin/

anti-

androgen

(no

clea

r co

mpa

ra-

tor)

Reproductive

Relievedhyperandrogenismafter

6 m

o

Reproductive

Hirsutism,acne,seborrhoea,testoster-

one,DHEAS,SHBG,FAI,

androstenedione

Metabolic

Combinationwithmetformin

moreeffectiveinreducingIR

Metabolic

BP,cholesterol,TG,HDL,LDL,glucose,

insulin,HOMA-IR

Psychologic

(Con

tinue

s)

Page 14: Pharmacological and surgical treatment of nonreproductive ......of PCOS.2-5,7,19,20 Most guidelines discussed 3 main pharmacologi-cal therapy categories, namely insulin sensitizers

548  |     TAY eT Al.

onemoderateandonehighquality.Resultswerederived from17trials and 780 participantswith PCOS. Statinswere evaluated ei-therasastandalone therapycomparedtoplaceboorascombina-tiontherapywithmetformincomparedtometformin.All3reviewsreported improvements inmetabolic outcomes (n=3 for the lipidprofile36,42,44 and n=1 for insulin),42 and 2 reviews reported im-provementinendocrineoutcomes(testosterone).42,44Theeffectsofstatinsonanthropometricoutcomeswerenotsignificant(n=2).36,44 Psychologicaloutcomeswerenotassessedbyanyofthereviews.

3.4.9 | Other therapy: vitamin D

Seven reviews evaluated vitamin D32,33,37,40,51,54,57 (Appendix S3,foundintheSupportingInformation)eitherasmonotherapyvspla-ceboormetformin,ascombinationtherapywithmetforminvsmet-forminorcomparingtheeffectsofbeforeandaftervitaminD.Onlyonereviewhadahighratingwhilethemajorityofthereviews(n=5)wereofmoderatequality,andonereviewwasoflowquality.Atotalof75trialsand5701participantswomenwithPCOSwereinvolved.

Five reviewsassessedendocrineoutcomeswith2 reviewsre-portingbenefitsDHEAS(n=1comparingvitaminDvsplaceboandvitaminDwithmetformin vsmetformin)57 or testosterone (n=1comparingvitaminDvsplacebo).40Metabolicoutcomeswereas-sessedby6reviewswith4reviewsreportedbenefitsasreductionsinHOMA-IR(n=1comparingvitaminDvsplaceboorcombinationtherapyvsmetformin),57totalcholesterol(n=1comparingvitaminDvsplacebo)57or triglycerides (n=2comparingbeforeandaftervitaminD).37,51One review reported significant improvements inblood pressure for vitamin D vs placebo.54 Anthropometric out-comeswereassessedbyonereviewwhichdidnotshowanysignif-icantresults.54Psychologicaloutcomeswerenotassessedbyanyofthereviews.

3.4.10 | Other therapy: N- acetyl- cysteine

Two reviews52,54 evaluated the efficacy of N-acetyl-cysteine ofwhichone reviewwasof highquality andone reviewwasof lowquality(AppendixS3,foundintheSupportingInformation).Atotalof19trialswith1744participantswithPCOSwereinvolved.Bothreviewsassessedanthropometric,endocrineandmetaboliceffectsof N-acetyl-cysteine in comparison with placebo or metformin.One review reported improvements in anthropometric anthropol-ogy (reducedBMI,weight andwaist-hip ratio) andmetabolic out-comes (improved lipidprofile, reduced fastingglucose, insulinandHOMA-IR).54Psychologicaloutcomeswerenotassessedbyanyofthereviews.

3.4.11 | Other therapy: antidepressants

One high-quality review39 aimed to investigate the efficacy ofantidepressants in PCOS (Appendix S3, found in the SupportingInformation)andidentifiedonestudyinvolving16womenwithPCOScomparingfluoxetine(antidepressant)andsibutramine(anti-obesityRe

view

sA

MST

AR

Qua

lity

of

incl

uded

stu

dies

Out

com

es a

sses

sed

Com

paris

onSi

gnifi

cant

resu

lts

Anti-androgens

Domecqetal(2013)49

Moderate

RCTs:lowto

moderaterisk

ofbias;

observational

studies:high

riskofbias

Anthropometric

–Anti-

androgen

(no

com

para-

tor)

NA

Reproductive

Metabolic

Fastingglucose,postprandialglucose,

glucosetolerancetest,random

glucose,areaunderthecurveof

glucose,glucose/insulinratio,

HOMA-IR,QUICKI

Psychologic

NA,notavailable;WMD,weightedmeandifference;SMD,standardizedmeandifference;CI,confidenceinterval;BMI,bodymassindex;SHBG,sexhormonebindingglobulin;FAI,freeandrogenindex;

DHEAS,dehydroepiandrosteronesulphate;BP,bloodpressure;HDL,high-densitylipoprotein;LDL,low-densitylipoprotein;TG,triglycerides;IR,insulinresistance;HOMA-IR,homoeostaticmodelassess-

mentofinsulinresistance;QUIKI,quantitativeinsulinsensitivitycheckindex;OCP,oralcontraceptivepill.

a Resultslessbeneficialthancomparator.

TABLE 3 (Continued)

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     |  549TAY eT Al.

TABLE 4 Resultsofsystematicreviewsregardingweightlosstherapies

Revi

ews

AM

STA

RQ

ualit

y of

in

clud

ed s

tudi

esO

utco

mes

ass

esse

dCo

mpa

rison

Sign

ifica

nt re

sults

Bariatricsurgery

Butterworthetal

(2016)

47Low

Unclear

Anthropometric

Percentageofexcess

weightloss

Pre-vspostbariatric

surgery

Anthropometric

1trial:improvedpercentageof

excessweightloss

Reproductive

Hirsutism

Reproductive

2trials:improvedhirsutism

Metabolic

T2DM,bloodpressure,

cholesterol,TG,HDL,

LDL,glucose

Metabolic

3trials:improvedglycaemicprofile

(resolutionofT2DM,improvement

ofglycaemiccontrol,ornormaliza-

tionofglucoselevels)

2trials:improvedbloodpressure

Psychologic

Depression

Psychologic

1trial:improveddyslipidaemia

1trial:improveddepression

Skublenyetal(2016)55

Low

Unclear

Anthropometric

BMI,weight,percentage

ofexcessweightloss

Pre-vspostbariatric

surgery

Anthropometric

Percentageofexcessweightloss

(weightedmean57.2%,range33%

to75%)

MeanBM

Iimprovedfrom46.3to

34.2

Reproductive

Hirsutism

Reproductive

Hirsutism(OR0.12,95%CI0.04to

0.36)

Metabolic

Psychologic

Orlistat

Graffetal(2016)56

Moderate

Unclear

Anthropometric

BMI,weight,waist

circumference

Insulin,HOMA-IR,

cholesterol,TG,HDL,

LDL

Anthropometric

8trials:reducedBMIand/orweight

5trials:reducedwaist-hipratioor

waistcircumference

Reproductive

Testosterone

Reproductive

7trials:reducedtestosterone

Metabolic

Insulin,HOMA-IR,

cholesterol,TG,HDL,

LDL

Metabolic

4trials:improvedlipidprofile(TG,

HDL,LDL)

5trials:reducedHOMA-IRand/or

insulin

Psychologic

OR,oddsratio;CI,confidenceinterval;T2DM,type2diabetesmellitus;BMI,bodymassindex;HDL,high-densitylipoprotein;LDL,low-densitylipoprotein;TG,triglycerides;HOMA-IR,homoeostaticmodel

assessment(ofinsulinresistance).

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drug).Nosignificantdifferenceswerereportedbetweentreatmentsforanthropometric,endocrineormetabolicoutcomes.Nostudyas-sessingpsychologicaloutcomeswasfound.

3.4.12 | Other therapy: acarbose

Acarbosewas compared against placebo in onemoderate qualityreviewincluding6trialsand263womenwithPCOS(AppendixS3,found in the Supporting Information).38 Acarbose was associatedwith improvement in endocrine (testosterone) and metabolic (tri-glyceride andHDL) outcomes.No significant change in anthropo-metric outcomeswas detected. Psychological outcomeswere notassessedbythereview.

3.4.13 | Other therapy: antioxidants

One low-quality systematic review assessed the efficacy of anti-oxidants54 (AppendixS3, found in theSupporting Information) in-volving 11 trials and 834 Iranianwomenwith PCOS. This reviewreportedonetrialforsoyvsplacebowhichimprovedendocrineout-comes(DHEASandtestosterone);onetrialforfolicacidvsplacebowithout any significant outcome; 3 trials for omega-3 vs placebowhichimprovedmetabolicoutcomes(increasedHDL,reducedtotalcholesterol, total cholesterol/HDL ratio, LDL/HDL ratio, triglycer-ides,LDL,glucose, insulinand insulin resistance);andone trial forzincvsplacebowhichimprovedendocrine(testosterone)andmeta-bolic outcomes (HOMA-IR, cholesterol, triglycerides and LDL).54 Nosignificantimprovementsinanthropometricoutcomeswerere-ported.54Psychologicaloutcomeswerenotassessedbythereview.

4  | DISCUSSION

This is thefirstoverviewofsystematic reviewsassessingpharma-cologicalorsurgicalinterventionsfornonreproductiveoutcomesinwomenwithPCOS,anditdemonstratesalackofhigh-qualitysys-tematicreviewsormeta-analysespresentingdatafromhigh-qualitystudies.

There isdiversity in thequalityof identified reviews in regardtotheuseofmetformin.MostdemonstratedareductioninBMIorwaist-hipratio,andsomereportedbenefitsinmetabolicoutcomesincludingbloodpressure,triglycerides,markersofglucosetoleranceandinsulinresistanceincomparisonwithplaceboorCOCP.Efficacyin hyperandrogenism is less convincing.Our findings support cur-rentevidence-basedguidelinesandspecialitysocietypositionstate-ments where metformin is recommended for women with PCOSwhofailedtoachievetargetweightlosswithlifestylemanagementorthosewithimpairedglucosetoleranceortype2diabetesmellitus,anditisalsonotrecommendedasatreatmentforhirsutismoracneduetoalackofefficacy.2,3,5,7,21,22,60

We report that thiazolidinediones were more effective thanmetforminorplaceboinreducingmarkersofinsulinresistance.30,31 Onlyoneof5reviewsshowedsuperiorityforthiazolidinedionesin

reducing testosterone.34 However, these benefits come with theprice of increased weight which is contradictory for PCOS giventhe high prevalence of obesity and the negative impact onmeta-bolic, endocrine and reproductive outcomes. Thiazolidinedionesmayalsoincreaserisksofbladdercancerandosteoporosis.2,5,7,61,62 Consideringtheserisks,thiazolidinedionesarenotrecommendedasroutinetreatmentforwomenwithPCOS.2,3,5,7,21,22

WereportherethattheCOCPwastheonlytreatmentmodalitythatimprovedclinicalhyperandrogenism.TheuseofCOCPwasnotassociatedwithworseninginsulinresistanceinthisreview.46,49,50,58 TheeffectsonlipidprofileweremorecontroversialasthepositiveeffectofincreaseinHDLmaybeoffsetbyanunfavourableincreaseintriglyceride.50Notably,thereviewbyDomecqetal49didnotre-portanythromboembolicorcardiovasculareventswithCOCPuse.There is consensus in recommendingCOCPs as first-line pharma-cological therapy foracne,hirsutismandoligo-/amenorrhoeawithcareful consideration of the potential risk of increased venousthromboembolism extrapolated from evidence from the generalpopulation.2,3,5,21Althoughpreviousstudieshaveraisedconcernsofworseninginsulinresistanceandtriglycerides,thereisnoavailableevidenceofincreasedcardiovasculareventswithlong-termusewithCOCP.2,7,63-65There is inadequateevidence tocompareor recom-mendspecificCOCPpreparationsorhormonalcomponents.

Whileanti-androgenshavebeenusedwidelytotreathirsutism,especially inpatientswherehirsutism isnot resolvedbyCOCPorwhereCOCPiscontraindicatedorpoorlytolerated,ourstudyfailedtofindanyevidence.2,3,21,60Theonlyreviewweretrievedfocusedon reporting the adverse events where flutamide was associatedwith hepatotoxicity in 2 case series.49One reason for the lack offindingsinourstudyislikelyrelatedtoourrestrictionpublicationsafter2009.Two reviewsbySwigloetal andBrownetal involving12and9RCTs,respectively,concludedthatanti-androgensareaneffectivetreatmentofhirsutismbuttheevidenceisweak.66,67BothreviewsincludedRCTsofsmallsamplesizes(14to82participants)andhighlightedtheneedofmorewell-designedRCTsinvestigatingtheuseofanti-androgensinwomenwithPCOS.

WeightlosstreatmentsinPCOSwereexploredby3reviewsinourstudy.Tworeviewsinvestigatingbariatricsurgerywereoflowqual-itywhich impactsontherobustnessoftheirresults.47,55WereportthatinwomenwithPCOS,bariatricsurgery-inducedweightloss,im-provedhirsutism,bloodpressure,glycaemicandlipidprofile.Orlistatimprovedanthropometric,endocrineandmetabolicoutcomeswhencomparedtoplacebobutnotmetformin.56However,weacknowledgethat there isencouragingevidence inthegeneralpopulationshow-ing that bariatric surgery improves weight loss andmetabolic out-comessuchasglycaemiccontrol,lipidprofileandbloodpressure.68-70 Bariatricsurgerywasrecommendedasasecond-linetherapytoim-provefertilityoutcomesinwomenwithPCOSbytheevidence-basedAustralianguidelineandtobeconsideredinmorbidlyobesewomenwithPCOSbytheEuropeanSocietyofEndocrinology.2,4Otherso-cieties concluded that better quality trialswith long-term data arerequiredbeforeincorporatingbariatricsurgeryintotheirrecommen-dationsforwomenwithPCOS.5,20Wefoundthatstatins,afamilyof

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cholesterol-loweringdrugs,areeffective in improvingthe lipidpro-file.36,42,44Giventhelackofdefinitebenefitsintreatmentofhyper-androgenaemiaoranovulation,paucityofdatainreproductive-agedwomenandconsideringthedisadvantageoftype2diabetesdevel-opment, statinsare reserved forwomenwithPCOSwhomeet thestandardindicationsforlipid-loweringtherapy.5,7,22,71

Ourreviewincludedseveralnonconventionalinterventionsthatarenot recommendedbyanyguidelinesor specialty societyposi-tion statements. Although the evidence is not robust, there maybesomebenefitswiththeuseofvitaminDandinositol.WefoundseveralmoderatequalityreviewsassessingvitaminDdemonstratedreductionsintriglycerideandtestosteronelevels.Onehigh-qualityreviewbyPergialiotisetalreportedbeneficialeffectsofvitaminDinreducingDHEAS, insulinresistanceandcholesterol.57 Inositol isa nutritional supplementwith proposed insulin-sensitizing charac-teristics.5,43,48Asreportedhereinlowtomoderatequalityreviews,they may have advantageous effects in nonreproductive-relatedendocrine andmetabolic outcomes including improving biochemi-calhyperandrogenismandinsulinresistance.Noconclusioncanbemade regarding the use of acarbose, N-acetyl-cysteine, soy, folicacid,omega-3orzincinwomenwithPCOSasthenumberofstudiesinvolvedislimited.

Ourstudyhasseveralstrengths.Beinganoverviewofsystem-atic reviews,we collated evidence of interventions for PCOS in anonbiased and systematic manner.We reported our findings fol-lowingthePRISMAguidelinesutilizingrigorousmethodologywithduplication in all study tasks.However,we note study limitationsincludingthediverseAMSTARqualityoftheincludedreviewsandthe lackof clear interpretationof thequalityof individual studieswithintheincludedsystematicreviews.However,performingaddi-tionalqualityassessmentofmorethan350includedstudieswouldbeunfeasible.Wealsoexcludedpublicationsbeforeyear2009asanattempttofilteroutreviewsthatdidnotfollowthePRISMAguide-lines.AssomeinterventionsforPCOShavebeenusedfordecades,wemayhaveexcludedsignificantearlierstudies,albeitpotentiallyoflowerquality.Inourstudy,wefoundthatonlyanti-androgenswereaffectedbythislimitation.66,67

Lastly, quality of future systematic reviews may be strength-enedbyaddressingreportingconflictofinterestofincludedstudies,registering for an apriori protocol andprovides a list of excludedstudies.Wealsoidentifiedsignificantgapsinknowledgeregardingthelackofdataonpsychologicaloutcomesintreatmentofwomenwith PCOS.We retrieved included psychological outcomes as anoutcomeofinterestonlyin2reviews39,47despitethewidelyknownincreasedprevalenceofdepression,anxietyandlowerqualityoflifeinwomenwithPCOSwhichfuturestudiesshouldaddress.72

5  | CONCLUSIONS

This overview of systematic reviews consolidates the evidence oftreatmentoptionsfornonreproductiverelatedoutcomesinwomenwith PCOS.We call attention to the lack of studies investigating

psychological outcomes in any intervention in womenwith PCOSwarrantingfurtherexamination.Overall,wenoteevidenceformet-forminandCOCPuseinnonreproductiveoutcomesinPCOS,cautionagainstthiazolidinedionesandhighlightthatfurtherresearchiswar-rantedinanumberofinterventionssuchasstatins,bariatricsurgery,vitaminDorinositoltoclarifyoutstandingclinicalgaps.

ACKNOWLEDG MENT

ChauTTayissupportedbyaCREinPCOSentrylevelscholarship,HelenaJTeedeissupportedbyanNHMRCPractitionerFellowship,AnjuEJohamissupportedbyaNHMRCEarlyCareerFellowshipandLisa JMoran is supportedbyaNationalHeartFoundationFutureLeaderFellowship.

CONFLIC T OF INTERE S T

Nothingtodeclare.

ORCID

Chau T. Tay http://orcid.org/0000-0001-6228-2654

Helena J. Teede http://orcid.org/0000-0001-7609-577X

Anju E. Joham http://orcid.org/0000-0002-6307-2568

Lisa J. Moran http://orcid.org/0000-0001-5772-6484

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SUPPORTING INFORMATION

Additional supporting information may be found online in theSupportingInformationsectionattheendofthearticle.

How to cite this article:TayCT,JohamAE,HiamDS,etal.Pharmacologicalandsurgicaltreatmentofnonreproductiveoutcomesinpolycysticovarysyndrome:Anoverviewofsystematicreviews.Clin Endocrinol (Oxf). 2018;89:535–553. https://doi.org/10.1111/cen.13753