The Short-Term Incidence of HKASLD HKASLD Hepatocellular ...

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The Short-Term Incidence of Hepatocellular Carcinoma Is Not Increased After Hepatitis C Treatment with Direct-Acting Antivirals: An ERCHIVES Study DK Li, YJ Ren, DS Fierer, S Rutledge, OS Shaikh, V Lo Re III, T Simon, A Abou-Samra, RT Chung, AA Butt Massachusetts General Hospital, Boston VA Pittsburgh Healthcare System, Pittsburgh Icahn School of Medicine, Mt Sinai, New York Perelman School of Medicine, University of Pennsylvania, Philadelphia Hamad Medical Corporation, Doha, Qatar Weill Cornell Medical College, Doha, Qatar & New York Accepted for Publication in HEPATOLOGY 2018 HKASLD Bi-monthly Scientific Meeting Journal Review James Y.Y. Fung 18 th Jan 2018 HKASLD HKASLD HKASLD HKASLD HKASLD HKASLD HKASLD HKASLD

Transcript of The Short-Term Incidence of HKASLD HKASLD Hepatocellular ...

TheShort-TermIncidenceofHepatocellularCarcinomaIsNot

IncreasedAfterHepatitisCTreatmentwithDirect-ActingAntivirals:

AnERCHIVESStudyDKLi,YJRen,DSFierer,SRutledge,OSShaikh,VLoReIII,T

Simon,AAbou-Samra,RTChung,AAButtMassachusettsGeneralHospital,Boston

VAPittsburghHealthcareSystem,PittsburghIcahnSchoolofMedicine,MtSinai,NewYork

PerelmanSchoolofMedicine,UniversityofPennsylvania,PhiladelphiaHamadMedicalCorporation,Doha,Qatar

WeillCornellMedicalCollege,Doha,Qatar&NewYork

AcceptedforPublicationinHEPATOLOGY2018HKASLDBi-monthlyScientificMeetingJournalReview

JamesY.Y.Fung18thJan2018

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Introduction•  IFN-inducedSVRhasbeenshowntoreduceHCCriskbyabout4-fold,regardlessofstageofliverdisease

•  TheextrapolationofthisbenefittoDAAsandtheexpectationofgreaterreductionhasnotbeenconsistent

•  ParadoxicalincreasedriskofHCCinpatientstreatedwithDAAtherapy

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•  7/16hadbeentreatedinitiallywithresectionand9/16withablation

•  MediantimefromHCCtreatmenttoDAAwas11.2m(25%-75%:3.6-23.2)

•  MediantimefromCRtoDAAwas1.7and1.3forHCCrecurrentpatient

•  MediantimefromCRtorecurrencewas3.5months(1.1-8)

•  RecurrencerateishigherthanobservedinhistoricalnonDAAtreatedcontrols

Reigetal.JHepatol2016;65:719-726

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•  Retrospectivecohortstudy•  344cirrhoticswithoutHCCat

timeofDAAs•  TreatedwithDAAsandFUfor24

weeks•  SVR91%•  59withHCChistory

–  19resections–  2resections+RFA–  2resections+TACE–  18RFA–  4RFA+TACE–  6PEI–  5TACE–  3Datanotcomplete

•  MedianintervalbetweenHCCtreatmentandDAA376days(range,45-2706)

ContiFetal.JHepatol2016;65:727-733

17/599/28526/344

7.6%

3.2%

28.8%

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ANRSC022HEPATHERCohort ANRSC012CirvirCohort

ANRSC023CUPILTCohort

13% 21%1/13(8%)31/66(47%)

2.2%

NoincreaseriskofrecurrenceofHCCwithDAA-treatedpatientscompared

withnon-treatedpatients

TheANRScollaborativestudygrouponHCC.JHepatol2016

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StudyAim

• WhetherDAAtreatmentisassociatedwithhigherratesofincidentHCCusingalarge,well-establishednationalcohortofHCV-infectedUnitedStatesVeteranswithoutapriordiagnosisofHCC

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Design&DataSource(I)•  RetrospectivecohortstudyofHCV-infectedpersonsinthe

ElectronicallyRetrievedCohortofHCVInfectedVeterans(ERCHIVES)database

•  AllHCV-infectedVeteransatanyUS-wideDeptofVeteranAffairsmedicalfacilitieswithanti-HCV+between2002and2016wereidentified

•  Demographic,clinical,labdatawereobtainedfromtheNationalPatientCareDatabaseandtheCorporateDataWarehouseHKASLD HKASLD

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Design&DataSource(II)

•  Pharmacyinformation,includingallprescriptionswritten,doses,duration,numberofpills,numberofrefills,anddateofrefills,wasretrievedfromthePharmacyBenefitsManagementdatabase.

•  Datamergedonestablishedalgorithms

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StudyParticipants

•  Inclusioncriteria– Anti-HCV+

•  Exclusioncriteria– HBV(HBsAg+)orHIVco-infection– Priortobaseline

•  DiagnosisofHCC•  MissingHCVRNAorFIB-4score•  IncompletedataforFIB-4calculationatleast12weeksafterbaseline•  MissingHCVRNAdataforcalculationofSVR12HKASLD HKASLD

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CohortGroups•  GroupA(IFN):–  ReceivedPEG+RBVfor≥28days–  IfmultiplecoursesofPR–1sttreatmentcourseusedasbaseline

–  StandardIFNexcluded

•  GroupB(DAA)–  ReceivedSOF/SMV±RBV;SOF/LED±RBV;SOF/DCL±RBV;PRoD±RBVfor≥28days

– OthernewerDAAsnotincluded(smallnumbers)

•  GroupC– NoHCVtreatmentfor≥28days

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BaselineDefinitions•  Fortreatedgroups– BaselinewasthedateofHCVtreatmentinitiation

•  Foruntreatedgroups– BaselineequaltothedurationofHCVinfectionpriortotreatmentinitiationinthecorrespondingtreatedperson•  Determiningtheaveragetimebetweenthefirstanti-HCV+dateandtreatmentinitiationdateforthetreatedgroup•  Addingthesamedurationtothetimebetweenthefirstanti-HCV+dateineachuntreatedpersonandassigningthatdateasbaselineHKASLD HKASLD

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DefinitionofCirrhosis

•  FIB-4score>3.5– FIB-4=(age[years]xAST[IU/L]/(plateletcount[plateletsx109/L]xALT½[IU/L])

•  Labdataobtainedatyearlyintervals– FIB-4scorerecalculatedateachinterval

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StudyOutcomes

•  Primaryoutcome– DevelopmentofincidentHCC

•  DefinedaspresenceofatleastoneinpatientortwooutpatientICD-9/10codesforHCCmade≥3monthsafterbaseline•  TimetodevelopmentofHCCdeterminedrelativefrombaseline•  GiventhatadvancedfibrosisisoneofthestrongestpredictorsofHCCdevelopment,primaryanalysiswasperformedonpersonswithbaselinecirrhosis(FIB-4>3.5)HKASLD HKASLD

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PatientCharacteristics

Age(yrs)

Sex,%maleRace,%WhiteBlack

HispanicOthers

Diabetes,%BMI,median

Alcohol,%

Smoking,%CurrentFormerNeverHKASLD HKASLD

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HCVGT,%123

4,5,6Missing

BaselineHCVRNAlog

PPIuseduringtreatment

StatinusepriortobaselineFIB-4baseline,%<1.45nofibrosis

>3.5cirrhosis1.45-3.5

MedianAFP

RBVuse,%Treatment,%

<8weeks8weeks12weeks24weeksSVR,%

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IncidenceRateofHCCbyTreatmentGroupandSVRStatus(EntireCohort)

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IncidenceRateofHCCbyTreatmentGroupandSVRStatus(CirrhoticsOnly)

TreatmentGroup

AllcirrhoticsIFN

DAAregimensUntreatedcontrols

SVR12subgroupIFN

DAAregimens

NonSVR12subgroupIFN

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ProbabilityofHCCDevelopmentinCirrhoticPersonwhoachievedSVR

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BaselineCohortCharacteristicsfromFIB-4SensitivityAnalysis

(Limiting

definitionofbaselineFIB-4towithin12monthspriortobaseline)

Overall1933FIB-4valuesexcluded209IFN82DAA

1642untreated

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IncidenceRateofHCCinPersonswithCirrhosis,byTreatmentGroupandSVR

StatusinFIB-4SensitivityAnalysis

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BaselineCharacteristics

ofDAASubgroups

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IncidenceRateofHCCinPersonswithCirrhosis,byDAATreatmentandSVRStatus

TreatmentGroup

CirrhoticsIFN

SOF/SMVSOF/LED

SVR12subgroupIFN

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NonSVR12subgroupIFN

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p=0.07

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Age,per10yearincreaseMalesex

RaceWhite(comparator)

BlackHispanic

Other/MissingDiabetes

BMI(per1unitincrease)Alcoholabusehistory

SmokinghistoryNon-smoker(comparator)

CurrentsmokerFormersmoker

MissingHCVgenotype,%1(comparator)

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4,5,6Missing

HCVRNA,per1logincreasePPIuse(baselineonwards)

StatinuseAFP>20(vs20orbelow)

TreatmentregimenPeg/RBV(comparator)

AnyDAAAttainmentofSVR

PredictorsfortheDevelopmentofHCCinPersonswithCirrhosisbasedon

Multivariate,CoxProportional

HazardsAnalysis

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PredictorsfortheDevelopmentofHCCinCirrhotics

BasedonMultivariateCoxProportional

HazardsAnalysisinFIB-4

SensitivityAnalysis

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Discussion•  DAA-treatedpersonsdidhaveasignificantlyhigherHCC

ratethanIFN-treatedpersons(overallgroup)–  Higherrateofknownriskfactors

•  Cirrhosis,olderage,higherbaselineAFP

•  AnalyzingcirrhoticpatientsaloneshowednodifferenceinHCC-freesurvivalbetweenDAAandIFNgroups–  LowerHCCincidenceinsensitivityanalysis

•  Pre-treatmentriskofHCCisthemaindriverofpost-treatmentriskofHCCHKASLD HKASLD

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Discussion•  HigherprevalenceofunderlyingHCCrisks

amongDAApatientsdueto“warehousing”?•  TreatmentwithearliestDAAregimensmay

besurrogateforhigherbaselineHCCrisk•  Failedtherapy,cirrhotics

•  PersonstreatedwithSIM/SOFhadhigherratesofcirrhosis(c/wIFN/laterDAAs)

•  PreviousstudieshavenotprovidedbaselinedataincombinationwithDAAregimens

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Discussion

•  Incontrasttopreviousstudies,DAAtreatmentisnotassociatedwithhigherriskofHCCcomparedtoIFNtreatmentwhencontrollingfordifferencesinbaselineHCCriskfactors

•  AchievementofSVRwithantiviralregimenisthemostimportantdeterminantofalowerHCCrisk

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StudyLimitations•  Relativelyshortfollow-uptimeinDAAcohort•  Potentialforlimitedgeneralizability– Veterans,males,highersmoking&alcoholuse

•  Retrospectivecohortstudy– Prospectivestudiesunlikely

•  Lackofliverhistologyfordiagnosingcirrhosis•  LackofinforegardingHCCsurveillancepractices

•  ExcludedthosewithpriorHCCHKASLD HKASLD

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StudyConclusion

•  IncirrhoticswithchronicHCVinfection,therewasnoassociationbetweenHCCincidenceratesandDAAtreatmentcomparedtoIFN

•  InsufficientcontrollingforbaselinerisksforHCCandselectionbiaslikelydrovepreviouslyreportedassociationsbetweenDAAtreatmentandincreasedHCCrisk

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