university of copenhagen Former Abusers of Anabolic Androgenic Steroids Exhibit Decreased Testosterone Levels and Hypogonadal Symptoms Years after Cessation A Case-Control Study Rasmussen, Jon Jarløv; Selmer, Christian; Østergren, Peter Busch; Pedersen, Karen Boje; Schou, Morten; Gustafsson, Finn; Faber, Jens; Juul, Anders; Kistorp, Caroline Published in: PLOS ONE DOI: 10.1371/journal.pone.0161208 Publication date: 2016 Document version Publisher's PDF, also known as Version of record Document license: CC BY Citation for published version (APA): Rasmussen, J. J., Selmer, C., Østergren, P. B., Pedersen, K. B., Schou, M., Gustafsson, F., Faber, J., Juul, A., & Kistorp, C. (2016). Former Abusers of Anabolic Androgenic Steroids Exhibit Decreased Testosterone Levels and Hypogonadal Symptoms Years after Cessation: A Case-Control Study. PLOS ONE, 11(8), [e0161208]. https://doi.org/10.1371/journal.pone.0161208 Download date: 22. Jan. 2023 RESEARCHARTICLE Former Abusers of Anabolic Androgenic Steroids Exhibit Decreased Testosterone Levels and Hypogonadal Symptoms Years after Cessation: A Case-Control Study JonJarløvRasmussen1*,ChristianSelmer1,PeterBuschØstergren2,Karen BojePedersen3,MortenSchou4,FinnGustafsson5,JensFaber1,AndersJuul6, CarolineKistorp1 1 DepartmentofInternalMedicine,CopenhagenUniversityHospital,Herlev,Denmark,2 Departmentof a11111 Urology,CopenhagenUniversityHospital,Herlev,Denmark,3 DepartmentofInternalMedicine, CopenhagenUniversityHospital,Slagelse,Denmark,4 DepartmentofCardiology,CopenhagenUniversity Hospitals,HerlevandGentofte,Denmark,5 DepartmentofCardiology,theHeartCentre,Rigshospitalet, Copenhagen,Denmark,6 DepartmentofGrowthandReproduction,Rigshospitalet,Universityof Copenhagen,Denmark *[email protected] OPENACCESS Abstract Citation:RasmussenJJ,SelmerC,ØstergrenPB, PedersenKB,SchouM,GustafssonF,etal.(2016) FormerAbusersofAnabolicAndrogenicSteroids Aims ExhibitDecreasedTestosteroneLevelsand HypogonadalSymptomsYearsafterCessation:A Abuseofanabolicandrogenicsteroids(AAS)ishighlyprevalentamongmalerecreational Case-ControlStudy.PLoSONE11(8):e0161208. athletes.TheobjectiveofthisstudywastoinvestigatetheimpactofAASabuseonrepro- doi:10.1371/journal.pone.0161208 ductivehormonelevelsandsymptomssuggestiveofhypogonadismincurrentandformer Editor:DavidJ.Handelsman,UniversityofSydney, AASabusers. AUSTRALIA Received:May26,2016 Methods Accepted:August1,2016 Thisstudyhadacross-sectionalcase-controldesignandinvolved37currentAASabusers, Published:August17,2016 33formerAASabusers(mean(95%CI)elapseddurationsinceAAScessation:2.5(1.7; Copyright:©2016Rasmussenetal.Thisisanopen 3.7)years)and30healthycontrolparticipants.Allparticipantswereaged18–50yearsand accessarticledistributedunderthetermsofthe wereinvolvedinrecreationalstrengthtraining.Reproductivehormones(FSH,LH,testoster- CreativeCommonsAttributionLicense,whichpermits one,inhibinBandanti-Müllerianhormone(AMH))weremeasuredusingmorningblood unrestricteduse,distribution,andreproductioninany samples.Symptomsofhypogonadism(depressivesymptoms,fatigue,decreasedlibido medium,providedtheoriginalauthorandsourceare credited. anderectiledysfunction)wererecordedsystematically. DataAvailabilityStatement:Theparticipantsinthis studyareguaranteedtoremaincompletely Results anonymous.Datacontainexplicitdetailson FormerAASabusersexhibitedsignificantlylowermedian(25th–75thpercentiles)totaland demographicsofeachparticipantinthestudy.Ifthe datasetwouldbemadepubliclyavailable,wefear freetestosteronelevelsthancontrolparticipants(totaltestosterone:14.4(11.9–17.7)nmol/l someoftheparticipantscouldberecognizedandrisk vs.18.8(16.6–22.0)nmol/l)(P<0.01).Overall,27.2%(13.3;45.5)offormerAASabusers legalprosecutionsorevenretaliationfromcriminal exhibitedplasmatotaltestosteronelevelsbelowthelowerreferencelimit(12.1nmol/l) distributorsofanabolicandrogenicsteroids.Dataare whereasnocontrolparticipantsexhibitedtestosteronebelowthislimit(P<0.01).Gonado- availableuponrequestto:JonJarløvRasmussen,M. D.;email:[email protected],M. tropinsweresignificantlysuppressed,andinhibinBandAMHweresignificantlydecreased PLOSONE|DOI:10.1371/journal.pone.0161208 August17,2016 1/16 ReproductiveHormonesandHypogonadalSymptomsinAbusersofAnabolicAndrogenicSteroids D.,PhD;email:caroline.michaela.nervil. incurrentAASabuserscomparedwithformerAASabusersandcontrolparticipants(P< [email protected]. 0.01).ThegroupofformerAASabusershadhigherproportionsofparticipantswithdepres- Funding:FundedbyAntiDopingDenmark(no sivesymptoms((24.2%)(11.1;42.2)),erectiledysfunction((27.3%)(13.3;45.6))and specificgrantnumber,URL:http://www.antidoping.dk/ decreasedlibido((40.1%)(23.2;57.0))thantheothertwogroups(trendanalyses:P<0.05). ),ResearchFoundationofHerlevHospital(no specificgrantnumber,URL:https://www. Conclusions herlevhospital.dk/),DanishHeartFoundation(grant number:15-R99-A5797-22952,URL:https://www. FormerAASabusersexhibitedsignificantlylowerplasmatestosteronelevelsandhigher hjerteforeningen.dk/),andFacultyScholarshipfrom frequenciesofsymptomssuggestiveofhypogonadismthanhealthycontrolparticipants UniversityofCopenhagentoJJR(nospecificgrant number,URL:http://sund.ku.dk/).Thefundershadno yearsafterAAScessation.CurrentAASabusersexhibitedseverelydecreasedAMHand roleinstudydesign,datacollectionandanalysis, inhibinBindicativeofimpairedspermatogenesis. decisiontopublish,orpreparationofthemanuscript. CompetingInterests:JonJarløvRasmussenand CarolineKistorphavereceivedunrestrictedresearch grantsfrom‘AntiDopingDenmark’.Thisdoesnotalter Introduction theauthors'adherencetoPLOSONEpolicieson sharingdataandmaterials.‘AntiDopingDenmark’ Anabolicandrogenicsteroids(AAS)comprisetestosteroneanditssyntheticderivatives.These hadnoroleinpreparationofthestudy,datacollection compoundshavebeenusedfordecadesbyprofessionalathletestoenhancemusclestrength andanalysis,preparationofthemanuscriptor andperformance[1,2].ThesettingofAASabusehaschangedwithinrecentyears.Arecent decisiontopublishthefinalversionofthemanuscript meta-analysisestimatedthelifetimeprevalenceofAASabuseworldwideis6.4%amongmen and18.4%amongrecreationalathletes[3].Moreover,apreviousstudysuggestedthatprior AASabusewasthemostfrequentcauseofprofoundhypogonadismamongyoungmen(43%) [4].ThesefindingsindicateAASabuseisnowprevalentinthebroaderpopulation. OngoingAASabusecausesdramaticincreasesinplasmaandrogenlevelsthatultimately facilitateseverehypothalamic-pituitary-gonadal(HPG)-axissuppressionduetonegativefeed- backmechanismsinvolvingtestosteroneanditsmetabolites[5].HPG-axisinhibitionmay causelong-lastingspermatogenesisinhibitionandreductionsinbiomarkersofSertoli-cell function,anti-Müllerianhormone(AMH)andinhibinB.However,informationregardingthe impactofAASabuseonthesereproductivehormonesisverylimited[6,7]. Anabolicandrogenicsteroid-inducedhypogonadism(ASIH)iscommonamongformer AASabusersandusuallypresentsashypogonadotropichypogonadismduetoabruptdecreases inplasmaandrogenlevelsfollowingAAScessation[1,2,5,8].ScientificdataonASIHarelim- ited,buttheconditionischaracterisedbysymptomsandsignsofhypogonadismsuchas:testic- ularatrophy,lowplasmatestosteronelevels,impairedspermatogenesis,erectiledysfunction, fatigue,decreasedlibidoanddepressivesymptoms;andisconsideredtoresolvespontaneously within6to12months[2,5].Studiesinvestigatingtherecoveryphasesofyoungmenwith ASIHare,toourknowledge,virtuallynon-existent.Agrowingnumberofstudiesreporting cases,inwhichASIHmanifestationspersistedyearsafterAAScessation,suggestASIHisa morepermanentconditioninasubstantialproportionofformerAASabusers[9–16].This emerginggroupofyoungmenmaybecomeaconsiderablepublichealthconcerninthecoming years. Theobjectiveofthisstudywastocomparethereproductivehormonelevelsandsymptoms suggestiveofhypogonadisminyoungmenwithhistoriesofcurrentandformerAASabuse withthoseofhealthyage-matchedmen. ParticipantsandMethods StudyDesignandParticipants Weconductedacommunity-basedcross-sectionalcase-controlstudyinthegreaterCopenha- genareafromNovember2014toDecember2015.Youngmen(18–50years)involvedin PLOSONE|DOI:10.1371/journal.pone.0161208 August17,2016 2/16 ReproductiveHormonesandHypogonadalSymptomsinAbusersofAnabolicAndrogenicSteroids recreationalstrengthtrainingwereenrolledinoneofthefollowingthreegroups:1)current AASabusers2)formerAASabuserswhohaddiscontinuedAASabuse(cid:1)3monthsbefore enrollinginthestudyand3)age-matchedhealthycontrolparticipantswhodeniedeverhaving usedAAS.Wedidnotapplyspecificinclusioncriteriaregardingweeklyhoursofrecreational strengthtraining,nordidweapplyinclusioncriteriapertainingtotheextentofAASabuse. Exclusioncriteriaforthethreegroupswere:congenitalhypogonadalconditions,medicallypre- scribedtestosteronetherapy,knowncardiovasculardiseaseanddiabetesmellitus.Participants wererecruitedprimarilyfromfitnesscentresinthegreaterCopenhagenareaandbyinternet advertising.Thefitnesscentresincludedweightliftinggymnasiumswhicharenotundersur- veillancebytheDanishAntidopingAgencyandareknowntobefrequentedbyAASabusers. Theadvertisementwasasfollows(inDanish):‘Weareseekingyoungmenforaresearchproj- ect;inclusioncriteria:age18–50yearsandinvolvedinrecreationalstrengthtrainingorarecur- rentlyusingAASorhavepreviouslyusedAAS’.Theadvertisementdidnotdisclosethestudy entailedassessmentsof:androgenlevels,fertilitybiomarkers,libido,erectilefunctionorsymp- tomsofdepressionorfatigue. Ethics ThestudywasperformedinaccordancewiththeDeclarationofHelsinkiandallrelevantlegal regulationsinDenmark.PermissiontoconductthestudywasgrantedbytheDanishDataPro- tectionAgency(HEH-2014-095,I-Suite:03250)andethicalapprovalwasgrantedbytheCapi- talRegionalCommitteeonHealthResearchEthicsinDenmark(H-3-2014-127).Oraland writteninformedconsentwasobtainedfromallparticipantspriortoinclusion. Procedures AllprocedureswereperformedduringonevisitattheCentreofEndocrinologyandMetabo- lism,DepartmentofInternalMedicine,CopenhagenUniversityHospital,Herlev,Denmark. Participantsattendedtheresearchlabbetween07:30and09:00a.m.afteraminimumofeight hoursofovernightfasting.Theywereplacedinthesupinepositionforaminimumof30min- utes.Allbloodsampleswerethencollectedviaacannulaintherightmediancubitalvein. Oneinvestigator(JJR)obtainedadetailedAASabusehistory(totalduration,compounds, doses,useofotherperformanceenhancingdrugs)duringaclinicalinterview,usingastruc- turedquestionnaire.WeusedtotalnumbersofweeksofAASabuseandtotalnumbersofAAS compoundsusedasmeasuresoftheextentofAASabuse.Wedidnotcalculateoverallaverage AASdosesintheAASparticipantsbecausethepharmacodynamicsandpharmacokineticsof AAScompoundscanvaryconsiderablydependingontheirchemicalstructures[1].Further- more,AASabusersoftenusenumerousAAScompoundsandalterdosesintermittentlyduring a‘cycle’[17].Otherinformationsuchasmedicalhistory,illicitdruguse,smokinghabits,alco- holuse,strengthtraininghistory(totaldurationandweeklyhoursoftraining)anddemograph- icswerealsoobtained.Testicularsize(ml)wasassessedinallparticipantusingPrader’s orchidometer,whichhasshownstrongcorrelationswithultrasoundtesticularsizeestimations [18]. LaboratoryAnalyses Plasmatotaltestosterone,androstendione,dehydroepiandrosteronsulfate(DHEAS)and 17-hydroxyprogesteronewereallmeasuredusingliquidchromatography-massspectrometry (LC-MS/MS),accordingtotheCHSMSMSsteroidskit(PerkinElmer,Massachusetts,USA). Theinter-assaycoefficientofvariation(CV)was<10.0%forallsteroidhormones.Sexualhor- mone-bindingglobulin(SHBG)wasanalysedbysandwichchemiluminescence-based PLOSONE|DOI:10.1371/journal.pone.0161208 August17,2016 3/16 ReproductiveHormonesandHypogonadalSymptomsinAbusersofAnabolicAndrogenicSteroids immunoassay(Siemens,Munich,Germany)andtheCVwas<7.0%.Freetestosteronewascal- culatedusingthemethodsuggestedbyBartsch[19].Lowreferencelimits(2.5percentile)for plasmatotaltestosteroneinyoungmendifferamongstudiesdependingonestimationinsub- groupsofnonobeseeugonadalhealthyyoungmen(10.4–12.1nmol/l)ormorepopulation-rep- resentativecohorts(6.6–7.4nmol/l)[20–23].Therefore,weassessedproportionsofthecontrol groupandgroupofformerAASwhoexhibitedlowtotaltestosteronelevelsusinglowerrefer- encelimitsforbothasubgroupofeugonadalnonobesehealthysubgroupofyoungmen(12.1 nmol)andapooledpopulation-representativecohort(6.6nmol/l).Gonadotropinsweremea- suredbyasandwichelectrochemiluminescence-immunoassay(ECLIA)(Cobas,Roche,Swit- zerland)andtheCVswere<7.0%.SeruminhibinBandanti-Müllerianhormone(AMH) levelswereusedasmarkersofSertoli-cellfunctionandspermatogenesis[24–26].Serumwas keptfrozenat-80°Cuntilneededforanalysisonthesamebatch.InhibinBwasmeasuredbya three-stepsandwich-ELISAassay(inhibinBgenII)(BeckmanCoulter,California,USA).The intra-assayvariationswere<10.3%,<8.6%and<7.6%atlevelsof36.3,111.4and616.4pg/ ml,respectively.SeruminhibinBisstronglyassociatedwithspermconcentrationsandsperm countsespeciallyuptoalevelof150pg/ml[25].Weusedareferencelimitof(cid:3)92pg/mlas cut-offforimpairedspermatogenesisbasedontheresultsofarecentstudy[24].AMHwasana- lysedbyatwo–stepsandwichelectrochemiluminescenceassay(BeckmanCoulter,California, USA)andtheintra-assayvariationswere<1.77%,<2.48%and<2.39%atlevelsof7.04, 34.88and105.66pmol/l,respectively. SymptomsIndicatingHypogonadism TheBeckDepressionInventory-II(BDI-II)questionnairewasusedtoevaluateparticipants regardingthepresenceofdepressivesymptoms[27].TheBDI-IIisa21-questionmultiple- choiceself-reportedpsychometrictest,andeachofitsquestionsisscoredusingascaleranging from0(minimum)to3(maximum).Atotalscore(cid:3)10isconsiderednormal,andtheBDI-II isstronglycorrelatedwithothervalidatedpsychometrictestsusedinprimarycaresettings [28].Questionnumber21oftheBDI-IIwasusedtoassesslibidoamongtheparticipantsand weconsideredascore<1normal.Erectilefunctionwasevaluatedusingthefive-itemversion oftheInternationalIndexofErectileFunction(IIEF-5)questionnaire[29].Thequestionnaire ishighlyvalidatedandconsistsoffivequestionsscoredusingascalerangingfrom1to5.A totalscore(cid:1)22indicatesnormalerectilefunction.TheShortForm-36(SF-36)questionnaire wasusedtoassess‘energy/fatigue’.Lowerscoresweresuggestiveofmorepronouncedfatigue symptoms[30]. StatisticalAnalyses Categoricalvariableswerecomparedusingachi-squaretestorFisher’sexacttestasappropri- ate.Thenon-parametricCochran-Armitagetrendtestwasusedtoassesstrendsinhypogona- dalsymptomsandimpairedspermatogenesisacrossthegroups.Theordinalorderingofthe groupsfortrendanalyseswasspecifiedapriori.Assumptionsofnormaldistributionswith respecttonumericalvariableswereevaluatedbyhistogramsandbyassessingthelinearityof residualsinaquantileplot.Equalityofvariancewasassessedusingresidualsofvariablesdrawn againstpredictedvaluesandusingLevene’stest.Numericalvariableswerecomparedacross thegroupsbyanalysisofvariance(ANOVA)andpresentedasmean(standarderror)ifthe assumptionsofanormaldistributionandequalityofvariancewerefulfilled.Furthermore, numericalvariableswerecomparedpairwiseamongthethreegroupswithTukey’spost-hoc test.Thenon-parametricKruskal-Wallis’test(withBoneferroni’spost-hoctest)wasusedto comparenon-normallydistributedvariableswhichcouldnotbelogarithmicallytransformed PLOSONE|DOI:10.1371/journal.pone.0161208 August17,2016 4/16 ReproductiveHormonesandHypogonadalSymptomsinAbusersofAnabolicAndrogenicSteroids toanadequatenormaldistribution.Thesevariablesarepresentedasmedians(25th–75thper- centiles).Weusedpiecewiselinearregression(linearsplines),allowingvaryingslopes,to modelnonlinearassociations.Missingdatawererare((cid:4)2%forquestionnaires,noneforall otherdata)andwereaddressedviamultipleimputationsusingthefullyconditionalspecifica- tionmethod[31].P-values<0.05wereconsideredstatisticallysignificant.Alldatawereana- lysedusingSASversion9.4(SASInstituteInc.,NorthCarolina,USA). Results CharacteristicsofParticipants Atotalof37currentAASabusers,33formerAASabusersand31controlparticipantsvolun- teeredtoparticipateinthestudy.Oneparticipantfromthecontrolgroupwasexcludeddueto cryptorchidismwhichwasdiagnosedduringthestudy,so30controlparticipantswere includedinthefinalanalyses.Theparticipantsinthethreegroupsdidnotdiffersignificantly withrespecttoage,smokinghistory,illicitdrugabusehistory,incomeormaritalstatus,but currentAASabusersperformedstrengthtrainingmorehoursperweekthanparticipantsinthe othertwogroups(P<0.05)(Table1). Ahigherproportionofparticipantsinthecontrolgrouphadauniversitydegreethanthe participantsintheothertwogroups(P<0.01).ThetotaldurationofaccumulatedAASabuse (geometricmean(95%CI))notedamongcurrentAASabusers(142.3(99.7;203.1)weeks)was notsignificantlydifferentfromthatnotedamongformerAASabusers(111.8(81.3;153.7) Table1. Demographiccharacteristicsandanabolicandrogenicsteroids(AAS)abuseinthethreegroups. Variable Controlgroup CurrentAASabusers FormerAASabusers p-value n=30 n=37 n=33 Demographiccharacteristics Age(years)¶ 31.5(1.2) 31.4(1.4) 34.8(1.2) 0.11 Recreationalstrengthtraining(hours/week)¶ 6.5(0.5) 9.2(0.7)a 6.9(0.7) 0.01 Cohabiting(%) 73.3 67.6 57.6 0.41 Income(US$/year) 51,700(5400) 43,000(7700) 60,800(7600) 0.35 Universitydegree(%) 30.0b 0.0 0.0 <0.01 Historyofsmoking(%) 26.7 43.2 51.5 0.10 Alcoholintake<once/week(%) 56.7c 86.5 72.7 0.02 Experiencewithillicitdrugs(%) 56.7 70.3 69.7 0.43 Anabolicandrogenicsteroidsabuse AccumulateddurationofAASabuse(weeks) - 142.3(99.7–203.1) 111.8(81.3–153.7) 0.32 AASabuseduringelapsedperiod(years) - 5.7(4.5–7.2) 6.3(4.5–8.8) 0.46 ElapseddurationsinceAAScessation(years) - - 2.5(1.7–3.7) - NumberofAAScompoundsused(n)● 8(4–9) 6(4–9) 0.32 Post-cycletherapy - RegularlyusedhCG(%) - 48.7 57.6 0.46 Regularlyusedaromataseinhibitors/antioestrogen(%) - 48.7 33.3 0.19 Resultsaregeometricmeans(95%confidenceinterval)unlessotherwisestated. ¶Mean(standarderror) ●Median(25th–75thpercentiles) Tukey’spost-hoctest(meanandgeometricmean)orBonferroni’spost-hoctest(medians) asignificantdifferencebetweencurrentAASabusersandtheothertwogroups bsignificantdifferencebetweencurrentAASabusersandtheothertwogroups csignificantdifferencebetweencontrolparticipantsandcurrentAASabusers doi:10.1371/journal.pone.0161208.t001 PLOSONE|DOI:10.1371/journal.pone.0161208 August17,2016 5/16 ReproductiveHormonesandHypogonadalSymptomsinAbusersofAnabolicAndrogenicSteroids weeks),andthenumbersofAAScompoundsuseddidalsonotdifferbetweenthetwogroups. Thetwogroupsreportedpreviousandcurrentexperiencewithvaryingdosesofnumerous AAScompounds,ofwhichtestosteroneesters,trenbolone,nandrolone,stanozolol,sustanon andboldenonewerethemostwidelyused(S1Table).Highproportionsofbothcurrentand formerAASabusersreportedregularlyusinghCGoraromataseinhibitorsfollowingAAS cycles.TheelapseddurationsinceAAScessation(geometricmean(95%CI))was2.5(1.7;3.7) yearsamongformerAASabusers.NoneoftheseparticipantsreportedhavingusedAASwithin sixmonthsandonly15.2%(95%CI)(3.0;27.4)reportedelapsedtimeintervalof6–12months sinceAAScessation.ElevenformerAASabusershadpreviouslybeenreferredtoanendocrine clinicforgynaecomastia,butnonehadbeentreatedforgynaecomastia,hypogonadismorinfer- tility.TheseparticipantsdidnotdifferfromotherformerAASabusersintermsofdemo- graphiccharacteristics,AASabuse,laboratoryresultsorfrequencyofhypogonadalsymptoms. ReproductiveHormones Testicularsizedifferedsignificantlyamongthethreegroups.CurrentAASabusershadthe smallesttesticularvolume(12.2(0.7)ml)andformerAASabusershadavolumeof17.4(0.8) mlwhichwas4.8(2.9;6.8)mlsmallerthanthatofthecontrolparticipantswhohadlargesttes- ticularvolume(Table2).Plasmatotalandfreetestosteronelevelsweresignificantlylower amongformerAASabusersthanamongcontrolparticipantsandcurrentAASabusers,thelat- terofwhomexhibitedsignificantlyincreasedplasmatestosteronelevels,asexpected.The 2.5th–97.5thpercentilesfortotaltestosteronerangedfrom12.4–32.3nmol/lamongthecontrol participantsand5.7–31.4nmol/lamongformerAASabusers. AhighpercentageofparticipantsinthegroupofformerAASabusers(27.2%(13.3;45.5)) werebelowthelowerreferencelimitforplasmatotaltestosteroneestimatedinnonobeseeugo- nadalhealthyyoungmen(12.1nmol/l)whereasnoparticipantsinthecontrolgroup(0.0% Table2. Reproductivehormonelevelsinthethreegroups. Variable Controlgroup CurrentAASabusers FormerAASabusers p-value n=30 n=37 n=33 Testicularsize(ml)¶ 22.3(0.6)b 12.2(0.7) 17.4(0.8) <0.01 P-totaltestosterone(nmol/l) 18.8(16.6–22.0)b 98.3(47.4–122.7) 14.4(11.9–17.7) <0.01 P-freetestosterone(pmol/l) 480(420–530)b 3780(1870–5500) 410(320–480) <0.01 P-androstendione(nmol/l)● 2.53(2.27–2.82) 6.92(5.41–8.84)a 2.33(2.06–2.63) <0.01 P-DHEAS(nmol/l)¶ 4805(391) 4929(490) 4348(302) 0.55 P-SHBG(nmol/l)● 33.3(29.1–38.1) 8.4(6.3–11.1)a 26.2(20.7–33.1) <0.01 P-17hydroxyprogesterone(nmol/l)● 2.88(2.49–3.33) 0.14(0.10–0.18)a 2.42(1.86–3.15) <0.01 P-FSH(U/l) 4.2(3.2–5.7) 0.3(0.1–0.4)a 4.4(3.3–6.2) <0.01 P-LH(U/l) 3.1(2.5–3.9) <0.1(<0.1–0.1)a 3.6(2.2–4.3) <0.01 S-inhibinB(pg/ml)¶ 175(9) 81(8)a 170(11) <0.01 S-AMH(pmol/l)● 49.5(41.6–59.0) 21.6(16.3–28.7)a 44.7(37.2–53.7) <0.01 Resultsaremedians(25th–75thpercentiles)unlessotherwisestated. ¶Mean(standarderror) ●Geometricmean(95%confidenceinterval) Tukey’spost-hoctest(meanandgeometricmean)orBonferroni’spost-hoctest(medians) asignificantdifferencebetweenthegroupofcurrentAASabusersandthetwoothergroups bsignificantdifferenceamongallthreegroups AAS,anabolicandrogenicsteroids,AMH,anti-Müllerianhormone;DHEAS,dehydroepiandrosteronsulfate;FSH,follicle-stimulatinghormone;LH, luteinizinghormone;P-,plasma;S-,serumSHBG,sexualhormone-bindingglobulin. doi:10.1371/journal.pone.0161208.t002 PLOSONE|DOI:10.1371/journal.pone.0161208 August17,2016 6/16 ReproductiveHormonesandHypogonadalSymptomsinAbusersofAnabolicAndrogenicSteroids Fig1.AssociationbetweenaccumulateddurationofAASabuse(log2scale)andtestissizeincurrentAASabusers(splinefunction)and formerAASabusers.Footnote:AAS,anabolicandrogenicsteroids. doi:10.1371/journal.pone.0161208.g001 (0.0;11.6))werebelowthislimit(P<0.01).Further,amongformerAASabusers3.3%(0.01; 15.8)werebelowthelowerreferencelimitforplasmatotaltestosteroneestimatedinapooled population-representativecohort(6.6nmol/l).Plasmagonadotropins,SHBG,17-hydroxypro- gesterone,serumAMHandinhibinBdidnotdiffersignificantlybetweenformerAASabusers andcontrolparticipants,butweremarkedlydecreasedamongcurrentAASabusers(P<0.01). TherewerehigherpercentagesofparticipantswithseruminhibinBlevelsbelowthelimitof impairedspermatogenesis(92pg/ml)amongcurrentAASabusers(56.8%(39.5;72.7))andfor- merAASabusers(9.1%(1.9;24.3))thanamongcontrolparticipants(3.3%(0.01;17.2))(trend analysis:P<0.01). AccumulateddurationofAASabusewasassociatedwithreducedtesticularsizeinformer abusers(log2coefficient(B)(95%CI):-1.3(-2.4;-0.2),P=0.02)andcurrentAASabusers(dur- ingtheinitial32weeksofAASabuse,splinefunction,log2coefficient(B):-5.4(-10.8;-0.02), P=0.049)(Fig1).Wedidnotobserveanysignificantassociationsbetweenplasmatotaltestos- teronelevelsandaccumulateddurationofAASabuse(log2coefficient(B):0.09(-0.04;0.22), PLOSONE|DOI:10.1371/journal.pone.0161208 August17,2016 7/16 ReproductiveHormonesandHypogonadalSymptomsinAbusersofAnabolicAndrogenicSteroids Fig2.AssociationbetweenaccumulateddurationofAASabuse(log2scale)andplasmatotaltestosteronelevels(log2 scale)informerAASabusers.Footnote:AAS,anabolicandrogenicsteroids. doi:10.1371/journal.pone.0161208.g002 P=0.17)(Fig2)orelapseddurationsinceAAScessation(log2coefficient(B):0.05(-0.7;0.17), P=0.42)(Fig3)amongformerAASabusers. AmongcurrentAASabusers,increasingaccumulateddurationofAASabusewasassociated withdecreasingseruminhibinBlevels,whichreachedaplateauafter64weeksofaccumulated AASabuse(splinefunction,log2coefficient(B):-47.9(-80.3;-15.6),P<0.01)(Fig4).Increas- ingaccumulateddurationofAASabusewasalsoassociatedwithdecreasingAMHlevels amongcurrentAASabusers(log2coefficient(B):-0.3(-0.5;-0.04),P=0.03)(Fig5). SymptomsIndicatingHypogonadism FormerAASabusersexhibitedthehighestfrequenciesofparticipantswithdepressivesymp- toms(24.2%(11.1;42.2)),erectiledysfunction(27.3%(13.3;45.6))anddecreasedlibido(40.1% (23.2;57.0))comparedwiththeothertwogroups(trendanalyses:P<0.05forallthreeparam- eters)(Fig6,S2Table).FormerAASabusershadalowerscoreontheSF-36questionnairewith respectto‘energy/fatigue’(58.9(4.3))thanthecontrolgroup(73.5(2.6))andcurrentAAS abusers(69.2(4.5))indicatingformerAASabusersexhibitedsignificantlymorepronounced fatiguesymptomsthantheircounterparts(P<0.05).Wedidnotobserveanysignificantasso- ciationsbetweensymptomsandhormonallevelsorextentofAASabuseamongformerAAS abusers. PLOSONE|DOI:10.1371/journal.pone.0161208 August17,2016 8/16 ReproductiveHormonesandHypogonadalSymptomsinAbusersofAnabolicAndrogenicSteroids Fig3.AssociationbetweenelapseddurationsinceAAScessation(log2scale)andplasmatotaltestosteronelevels(log2 scale)informerAASabusers.Footnote:AAS,anabolicandrogenicsteroids. doi:10.1371/journal.pone.0161208.g003 Discussion ThekeyfindingsofthisstudywerethatthegroupofformerAASabusersexhibitedsignifi- cantlylowerplasmatotalandfreetestosterone,smallertesticularsizes,andfeaturedahigher proportionofparticipantswithdepressivesymptoms,fatigue,erectiledysfunctionand decreasedlibidothanthecontrolgroupmorethantwoyearsafterAAScessation.Theseresults indicatethataconsiderableproportionofformerAASabusersexhibitedpersistentASIHfea- tures,suchasbiochemicalandfunctionalhypogonadism,yearsafterAAScessation. WeassessedpercentagesofthegroupsofcontrolparticipantsandformerAASabusers belowthereferencelimitforplasmatotaltestosteroneusingreferencerangesforbothasub- groupofnonobeseeugonadalhealthyyoungmen(12.1nmol/l)andapooledpopulation-repre- sentativecohort(6.6nmol/l).OurfindingswerethatahighproportionofformerAASabusers werebelowthereferencelimitforeugonadalnonobesehealthyyoungmencomparedwith noneofthecontrolparticipants,butonly3.3%offormerAASabuserswerebelowthelower referencelimitusingthepooledpopulation-representativecohortestimation.Thesefindings suggestaratherhighproportionofformerAASabusersexhibittestosteronelevelsinthelow areaofthenormalrangeyearsafterAAScessation,whereasonlyasmallproportionofformer AASabusersexhibitpersistentlymarkedlowtestosteronelevels. PLOSONE|DOI:10.1371/journal.pone.0161208 August17,2016 9/16
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