Post on 05-Aug-2020
FunctionaI GIDisorders
LouisW.C.LiuMD,PhD,FRCPC
HeadofGastroenterology,UniversityHealthNetworkandSinaiHealthSystem
Director,MotilityUnit,UniversityHealthNetwork
TrendsinIBSHospitalizationsandFinancialBurdensinUSA
• UtilizedtheNationalInpatientSampledatabases,collectedaspartofAgencyforHealthcareCostandUtilizationProjectbyAgencyforHealthcareResearchandQuality
• HospitalizationsofadultswithprimarydiagnosisofIBSwerecapturedbyICD-9codes.
MASiddiqu etal,DDW2018,Su1196
• IBSrelatedEDvisitsincreasesovertimes• PrincipaldiagnosisadmissionwithIBSistrendingdown.
TrendsinIBShospitalizationsandfinancialburdensinUSA
MASiddiqu etal,DDW2018,Su1196
IBSwasrankedasoneofthetop10mostexpensiveGIdiseasesintheUS1
IBScomparedwithotherchronicconditionsinCanada
CanadianspermanentlyunabletoworkCanadianchronicdiseasesaccordingtoage
1. Fedorak RN, Vanner SJ, Paterson WG, Bridges RJ. CJG. 2012;26(5):252-256.2. Inadomi JM, Fennerty MB, Bjorkman D. APT. 2003 Oct 1; 18(7):671-823. Spiegel BM, Kanwal F, Naliboff B, Mayer E. AJG. 2005 Oct; 100(10):2262-734. Boivin M. CJG. 2001 Oct; 15 Suppl B():8B-11B.
ImpactonHealthcareUtilization
*12%havebeenhospitalizedinthelast12monthsforreasonsrelatingtoIBS.
GISociety.2016.Availableat:http://www.badgut.org/wp-content/uploads/IBS-Survey-Results-2016.pdf.LastaccessedApril,2018.
• 6millionCanadianslivingwithIBS
• TheannualhealthcaredirectcosttreatingIBSexceeds$6.5billionnotincludingover-the-countermedicationorprescriptions.
• ApatientwithIBSmisses13workdaysperyear,accountingfor$8billion inlostproductivityannually
Understanding Irritable Bowel Syndrome. www.cdhf.ca.
Comments:impactonpolicymakers,resourcedistributionandutilizationbyprivateandpublicpayers
IBS:Pathophysiology
ModifiedfromROMEIVSlideDeck.2016
• Background:previousstudyfocusedonearlyadverselifeevents<18yroradulthoodeventoccurring3-12mo ofthestudyenrollment;associationoflifeeventsinadulthoodwithIBSandHPAfunctionhasnotbeenstudied
• Aim:determinetherelationshipbetweenstressfullifeeventsinadulthoodofhavingIBS,symptomseverityandHPAresponsetohormonechallenge.
• Method: ROMEIII(IBS:n=129,meanage26.1,66%F)cf healthycontrols(n=108,meanage29.8yr,60%F).– CompleteLifeExperiencesSurvey(LES)of60potentialeventsoccurring
sinceage18.Eventswereratedashavinganegativetopositivelifeimpactonascaleof-3to+3.Scoring includednumberofnegativeevents,negativeeventimpactscore(sumofnegativelyscoredevents),andtotaleventimpactscore(sumofpositivelyandnegativelyscoredevents).AdverseChildhoodExperiencessurvey(ACE),IBS-SSSandIBS-QOLwerecollected
– HPAregulation:cortisolandACTHresponsetoCRFweremeasuredin68IBSand41HC(controlforage,sexandBMI)
Parker,Cetal.DDW2018,oralpresentation454,SundayJune3.Stressfullifeeventsinadulthoodincreaseriskofirritablebowelsyndromeandsymptomsseverity
StressfullifeeventsincreaseIBSandsymptomseverity
IBSsubjectshadahigheraveragenumberofnegativelyperceivedlifeevents(p=0.067),agreaternegativeeventimpactscore(p=0.022)andamorenegativetotaleventimpactscore(p<0.001).
• InIBSpatients,thethreelifeexperiencesurveyscoresincreasedIBS-SSS(p=0.059,p=0.025,andp=0.02)anddecreasedIBS-QOL(allp<0.001).
• GreaternegativelyperceivedlifeeventswasassociatedwithabluntedCRFstimulatedACTHresponseinIBSbutanincreasedresponseinHCs
Parker,Cetal.DDW2018,oralpresentation454,SundayJune3.Stressfullifeeventsinadulthoodincreaseriskofirritablebowelsyndromeandsymptomsseverity
StressfullifeeventsincreaseIBSandsymptomseverity
• Conclusions:– Negativelyperceived lifeeventsinadulthoodareassociatedwithincreasedoddsofhavingIBS,worsesymptomseverityandQOL.
– HPAresponsetotheseeventswerebluntedinIBSpatients.ThebluntedACTHresponseinIBSmaybeduetoincreasedhypothalamicCRFsecretionandresultingdownregulationofCRF1receptorsinthepituitarygland.PositivelifeeventsappeartomitigateadverseeffectsinIBS.
• Comments:helptoeducateandvalidatepatients,reinforcetheutilityofCBTandpsycho- andnon-pharmacologicaltherapy
StressfullifeeventsincreaseIBSandsymptomseverity
Parker,Cetal.DDW2018,oralpresentation454,SundayJune3.Stressfullifeeventsinadulthoodincreaseriskofirritablebowelsyndromeandsymptomsseverity
Louis Liu, Chris Andrews, David Armstrong, Alain Bitton, Brian Bressler, John MarshallContributing faculty members involved in the development of the algorithm
CARE Chronic Constipation Treatment Algorithm
e.g. Milk of Magnesia, Lactulose or PEG titrate to efficacy and tolerability +/- fibre supplementsEight-week trial at a reasonable dose prior to
reassessment of maintenance or escalation to step-up therapies
Additional Agents:Options as in slow transit*
(e.g. stimulant,osmotic laxative)
Additional Therapy:Pharmacological
eg. TCA, SSRI, SNRL antispasmodic
Non-Pharmacologicale.g. Medication,
Relaxation, Hypnosis
Fibre Supplements Osmotic Laxatives Prosecretory Agentse.g. Linaclotide Specialist Assessment for
Consideration of Anorectal Manometry, Defecography and Biofeedback Therapy
e.g. Linaclotide or PrucaloprideEight to twelve-week trial prior to reassessment for maintenance
or consideration of referral for specialist assessment
Prosecretory or Prokinetic Agents
Unsatisfactory Response or Intolerant to Side Effects
Specialist Assessment Recommended (Refer)
1. Glycerine suppository2. Stimulant laxatives (e.g. bisacodyl)3. Enema
Rescue Therapy
Constipation symptoms predominant
Functional abdominal pain predominant
TypeofConstipation?
LifestyleModifications(e.g.,DietaryFibre,Fluid,Exercise)
Inadequate Fibre Intake CIC/Slow Transit IBS-C Pelvic Floor DyssynergicDefecation
History&PhysicalIncludingCarefulPerineal/RectalExamination
AssessAlarmFeatures OptimizeManagementofSecondaryCauses
Alarm Features Identified No Alarm Features Identified Constipation Persists
Specialist AssessmentRecommended (Refer)
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Tse Y et al CJGH 2017
LinaclotideinJapanesepatientswithchronicconstipation• Background:PhaseIIandIIIstudiesforIBS-CinJapanshowedthat0.5mg/daywasthe
mosteffectivedose.AphaseIIdose-rangingstudyoflinaclotideinaJapanesechronicconstipation(CC)populationshowedthat0.5mg,adose3.4timeshigherthanthehighestapproveddoseintheUS,wasagainthemosteffectivedose.
• Aim: verifythat0.5mgoflinaclotideiseffectiveandsafeforCCpatientsinJapan.• Method: multicenter,phase3.ROMEIIICC.Phase1:4-weekplacebocontrol,
linaclotide0.5mgdaily.Phase2:52-weekopenlabel,doseadjustmentcanbemadeatweek4and12visits(0.25or0.5mg)dependingontolerability.
• Endpoints:– Primary:changeinSBM/weekatthe1stweekofadministration– Secondary:CSBM,stoolconsistency,andstrainingseverityscore
• Result:– Phase1:SBMfrequencyincreases(linaclotide,4.02vs1.48,p<0.001).CSBMinthelinaclotide
(52.7%vs26.1%inplacebo,p<0.001).Allsecondaryendpoints,werealsosignificantlygreaterinthelinaclotidegroup.Theincidenceofdiarrheawashigherinthelinaclotidegroup(13.0%vs1.1%inplacebogroup.Phase2:Patientsswitchedfromplacebotolinaclotideshowedarapidonsetofresponsewithinthe1stweekforchangeinSBMfrequency,similartothatinpatientswhocontinuedtoreceivelinaclotide.
– Themostcommondrug-relatedadverseeventwasmildorsometimesmoderatediarrhea.• Conclusion: Thisstudysuggeststhatalinaclotidedoseof0.5mg/dayiseffectiveand
safeforCCpatientsinJapan.• Comments:validatetheefficacyandsafetyofhigherdoseoflinaclotideusedin
clinicalpracticeinIBS-CandCCpatients.
SFukudo DDW2018,Tu1627
Responsesofrifaximinre-treatmentinIBS-Dpatientswithrecurrentsymptoms(Target3)
Lembo,Aetal.RepeatTreatmentWithRifaximin isSafeandEffectiveinPatientsWithDiarrhea-predominantIrritableBowelSyndrome.2016;Gastroenterol.
CharacterizationofLong-termRifaximinResponders
• Aim:BLcharacteristicsthatpredictlong–termresponse• Methods: posthocanalysisofaphase3,IBS-Dwhomaintainedresponse
withrepeatrifaximintreatment(Target3).Long-termresponsewasdefinedasa≥30%decreasefrombaselineinmeanweeklypainscoreand≥50%decreasefrombaselineinnumberofdays/weekwithBSStype6or7stoolfor≥2offirst4weekspost-treatmentduringtheprimaryevaluationperiodandwasmaintainedthroughthesecond 4-weekfollow-upphase.
• Abdominalpain(0-10),bloating(0-6),andIBSsymptoms(0-6)• Results: 571observedcase;rifaximin(n=290);placebo(n=281).
– Long-termresponsewasachievedby39(13.4%)rifaximin- and21(7.5%)placebo-treatedpatients(P=0.01).
– long-termrifaximinrespondershadasignificantlygreatermeannumberofdailyBM(4.7vs3.2, P=0.0001)andgreaternumberofdayswithstoolurgency(6.4vs4.8; P=0.0001),greatermeandailybaselineabdominalpain(5.8vs4.4, P=0.0002),bloating(4.5vs3.6, P=0.0001)andIBSsymptoms(4.4vs3.6; P=0.0004).
• Conclusions: IBS-Dpatientswithmoreseveresymptomsappearedmorelikelytomaintainlong-termresponsetoshort-courserifaximin.
• Comments: encouragingresultsgivenpositiveresponsetomoreseverepatients(deltaaffect).The‘long-term”definitionisrelativeshort-term.Postmarketingclinicalexperienceofobservationalcohortwillprovidemoreinformation.
LWeinstocketalDDW2018,Su1190
RifaximinandCDiffInfection• Aim:determinetheimpactofrifaximintreatmentonthe
developmentof Cdifficileinfection• Method:posthocanalysisofaphase3,randomized,double-
blind(DB)placebo-controlled,52-weekstudy(Target3)inadultIBS-Dpatients,rifaximin550mgTIDx2weeks
• Results:n=2357,37patientsexcluded(positiveEIAatBL)– 3patientsdidnothavestoolsamplesatBLwerepositiveatthe
endofstudy(mighthavebeenasymptomaticcarriers).– 1developedCdiff37daysaftercompletionoftreatment(UTI
treatedwithcefdinirx10days• Conclusion:NoreportedCdiffcase
• Comments:consistentwithreportedsafetyprofileinotherstudies(HE)andpost-marketingmonitoringdata
MPimenteletal,DDW2018,Su1195.
Ondansetronimprovesstoolsconsistency,frequencyurgency,andbloating,butnotpain,inIBS-Dpatients
ModifiedandadaptedfromtheROMEIVslidedeck,2016
Garsed etal.Gut2014Oct;63(10):1617-16255-week randomized, double-blind, placebo-controlled crossover study
N=120
Titrateupto8mgTID
OndansetronandIBS-D
Plasse T,BartonGetal.DDW2018.Su1188
Population:Phase2IBS-D,ROMEIIIwithpainintensity≧ 3(10VAS),multicenterUSInterventions:Ondansetron12mgbimodalrelease(BRO,3mgimmediateand9mgextendedrelease)x8weeks,randomized60:40(BROtoplacebo)Endpoints:• stoolconsistencyresponse≧50%reductionindays/wk with≧ 1BMwithBSS6or7cf
baseline;• Painresponse≧ 30%reductionofweeklyavg worsepainoverthepast24hr cf baseline• Compositeresponse:achievestoolconsistencyresponseandpainresponseinthesame
week.
30%male,medianage40yr,medianIBS-D,averageBSS5.8,medianworsepain5,medianCRP2.0mg/L(UNL=5.0mg/L)
Comments:Similaraspreviousstudy,nodataonloperamide(orpreviousmedication)use
TESinCC
• Background:Transabdominalelectricalstimulation(TES)hasshownpromisingresultsinchildrenthatincreasedthecolonictransittimeanddefaecationfrequency,andimproveQoL.
• Method:2tertiaryhospitals,ROMEIII,CC.Rhythm.IC,60mindaily
• Endpoints:PAC-SYM,PAC-QoLatwk 10(for8wktreatmentgroup),atwk 18(16wk Txgroup)cfBL)
NTalley,DDW2018,Mo1538
Rhythm.IC device
Studyprotocol• Battery-operated• ThroughtheabdomenatT10-L3andoverS3-4for60mindaily.• Stimulationusedacarrierfrequencyof4000Hzandmodulationof80-
160Hzatastronglevel(max40mAmps).NTalley,DDW2018,Mo1538
http://www.githerapies.com/technology-product
TESinCC
NTalley,DDW2018,Mo1538
Conclusion:Fromthisinitialpilottrial,Rhythm.IC wouldappeartoprovideavaluableclinicaltherapyforadultssufferingchronicconstipation.
Comments:non-randomized,largeplaceboeffectinFGIpatients,non-standardoutcomesforCCstudies;probablysafe.Costcanbealimitingfactor.
n=17;meanage48.3years,94%female
FMTCinIBS-D
• Aim:investigatedthesafetyandefficacyofFMTc inarandomized,placebo-controlledtrial.
• Methods:multicenter,placebo-controlledRCTinadultmoderate-severeIBS-D.Subjectswererandomized1:1toFMTc followedbyplacebocapsules(Pc)orPcfollowedbyFMTc.– 25FMTc (50gmsofstoolfromahealthydonor)or25Pcandwere
followedfor12weeks.– Allsubjectscrossedoverintothealternatearmat12weeksandwere
followedforanother12weeks.• Outcomes:primary- decreaseinIBS-SSS≥50pointsat12weeks;
Secondary- IBS-QOLscores,HospitalAnxietyandDepressionScale(HADS)scoresandmeanBSSscores.Pre- andpost-interventionstoolsampleswerecollectedinallsubjectsfor16smicrobiomeanalysis.
OCAroniadis etal.DDW2018,OralpresentationNumber:742(mo 16:16-16:32)
• AEswerenotsignificantlydifferentbetweengroups;therewerenoseriousAEs.
• Preliminarymicrobiomeanalysesperformedatbaselinein12of48subjectsdistinguishedFMTrespondersfromnon-responders(AUC=0.93,p=0.09)basedontheabundanceofbacterialspecies,including V.dispar,B.eggerthii,B.uniformis,E.dolichum,B.acidifaciens.
OCAroniadis etal.DDW2018,OralpresentationNumber:742(mo 16:16-16:32)
• Conclusion: FMTc didnotinducesignificantsymptomreliefat12weekscomparedwithplacebo.SubgroupanalysissuggestedthatFMTmaybemoreeffectiveinpatientswithPI-IBS.
FMTCinIBS-D
• Comments:smallsamplesize,48subjectsin3centersbetween2015-2017.Promisingalternatives,certainlymorestudieswillbeperformed,particularlytoidentifytheIBSsub-group,eg post-infectionIBS-D,thatwillmorelikelyrespond.
OCAroniadis etal.DDW2018,OralpresentationNumber:742(mo 16:16-16:32)
MoxibustiononIBS-DMoxibustionisatraditionalacupuncturemethodthatworksbyheatingacupuncturepointswithlightedmoxa
ST-36
MoxibustiononIBS-D• Method:24-weekRCT(6wk treatment,18-wkfollow-up),RomeIIIcriteria,
IBS-D,moxibustion(at43°C± 1°C)vssham(37°C± 1°C),3treatmentsperweekx6weeks.Fouracupoints- ST25(Tianshu,bilateral)andST36(Zusanli,bilateral)
• Outcomes:– Primary:IBSAdequateRelief(IBS-AR)atweek6,week7andweek24,– Secondary:IBS- SSSscores(response>50pt reduction),BSSscore,stool
urgencyassessedatweek6,12,18and24.IBS-QOLwasmeasuredatweek6.• Results:N=104(60.0%F),IBS-ARinmoxibustiongroupwas76.9%vs
42.3%inplacebo(p<0.001)atweek6,remainedsignificantatweek24.IBD– AllsecondaryoutcomesweresignificantlyimprovedexceptIBS-QoLatweek6
• AE:1ineachgrouphadmildscald
• Comments:newpossibletherapeuticoption.GeneralizabilityandMoAneedsfurtherstudy.EfficacyisalsobeingevaluatedinIBD.
LiuH,etal.DDW2018,oralpresentation1025,Tue15:00- 15:30
KeyNewsoutofDDW• Epidemiology
– IBSimposesasignificantfinancialburdeninhealthcareandsociety
– impactsonpolicymakersinresourcesdistribution• Pathogenesis
– StressincreasesIBSoddsandsymptomseverity• Therapies
– MayusehigherdoseoflinaclotideinJapanese(Asian)IBS-Cpatients
– Rifaximin• Additionaldataonbloating,consistentwithclinicalexperience• Noevidenceofincreaseopportunisticinfections(presentation458)orCdiffinposthocanalysis
• ExpectingNoC inDec18andwillbecomeavailableinCanadainspring2019
• Long-termeffects/AEsinrecurrent/chronicusesremainuncertainandwillneedongoingmonitoring.
Thankyou!
EnjoyWashington,DCandDDW2018!