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Inhibitor development according to FVIII concentrate in PUPs: how to interpret current evidence? Alfonso Iorio Health Information Research Unit & Hamilton-Niagara.

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Presentation on theme: "Inhibitor development according to FVIII concentrate in PUPs: how to interpret current evidence? Alfonso Iorio Health Information Research Unit & Hamilton-Niagara."— Presentation transcript:

1 Inhibitor development according to FVIII concentrate in PUPs: how to interpret current evidence? Alfonso Iorio Health Information Research Unit & Hamilton-Niagara Hemophilia Program McMaster University

2 Disclosures for Alfonso Iorio In compliance with COI policy, EAHAD requires the following disclosures to the session audience: ShareholderNo relevant conflicts of interest to declare Grant / Research SupportBayer, Baxter, Biogen Idec, Novo Nordisk, Pfizer ConsultantBayer, Baxter, Novo Nordisk EmployeeNo relevant conflicts of interest to declare Paid InstructorNo relevant conflicts of interest to declare Speaker bureauNo relevant conflicts of interest to declare HonorariaBayer, Baxter, CSL, Octapharma, Pfizer Presentation includes discussion of the following off-label use of a drug or medical device:

3 Overview 1)Assessing causality: methodological notes 2)Appraising data on the concentrate dependent risk of inhibitors 3)Implications and perspectives

4 Overview 1)Assessing causality: methodological notes 2)Appraising data on the concentrate dependent risk of inhibitors 3)Implications and perspectives

5 TREATMENT ADVATE KOGENATE 0 ED 50 KOGENATE ADVATE

6 TREATMENT ADVATE KOGENATE RANDOM NEXT PATIENT Large deletion Deletion + history Point + history Point mutation Family history Point mutation Family history Point mutation Point + history Family history Deletion + history MULTIVARIABLE ANALYSIS MULTIVARIABLE ANALYSIS

7 Family history Gene mutation Brand MULTIVARIABLE ANALYSIS MULTIVARIABLE ANALYSIS

8 Gene mutation Family history Brand MULTIVARIABLE ANALYSIS MULTIVARIABLE ANALYSIS ??Unknow n ?? ??Unknow n ?? ?

9 Gene mutation Family history Brand MULTIVARIABLE ANALYSIS MULTIVARIABLE ANALYSIS ??Unknow n ?? ??Unknow n ?? Kogenate/ Advate ?

10

11

12 Assessing causality – summary notes Selection by indication Selection by indication – Unbalanced risk of event at baseline Center effect – The effect of center is a proxy for what you cannot measure it is constantly checked even in randomized trials Methods exists for small centers – Center effect and “center size” effect ARE NOT the same McGilchrist, CA et al. Regression with frailty in survival analysis. Biometrics, 1991 47, 461-6. Hougaard, P. Frailty models for survival data. Lifetime Data Analysis, 1995, 1, 255-273.

13 Overview 1)Assessing causality: methodological notes 2)Appraising data on the concentrate dependent risk of inhibitors 3)Implications and perspectives

14 Concentrate based risk of inhibitors RODIN France Coag UK UKHCDO Vazina EUHASS EAHAD Metanalysis For each one: Design Main result Key to appraisal Does it point to a true difference of K vs A as the most likely explanation?

15 Evidence profiling StudyDesignMain resultinterpretationContribution RODIN UKHCDO France C Vezina EUHASS EAHAD IPD

16 Evidence profiling StudyDesignMain resultinterpretationContribution RODINP, R, IC, MC Year: 2000-2010 Tot: 340 (574) RC, RD: 28.2, 9.0% Post hoc Multivariable (+) Hypothesis generation UKHCDO France C Vezina EUHASS EAHAD IPD P = prospective; R = retrospective; IC – Inception cohort; MC = Multisite

17 Evidence profiling StudyDesignMain resultinterpretationContribution RODINP, R, MCYear: 2000-2010 Tot: 340 (574) RC, RD: 28.2, 9.0% Post hoc Multivariable (+) Hypothesis generation UKHCDOR, IC, SCYear: 2000-2010 Tot: 300 (407) RC, RD: 23.8, 11.3% Time effect, B-DD f-VIII, RODIN effect Generate alternative hypothesis France C Vezina EUHASS EAHAD IPD P = prospective; R = retrospective; IC – Inception cohort; MC = Multisite, SC = single country

18 Kogenate Advate Dashed line = RODIN centers Advate 3/1226/11713/43 Kogenate 24/6516/315/32 UKHCDO cohort: effect of time and … RODIN?

19 Evidence profiling StudyDesignMain resultinterpretationContribution RODINP, R, IC, MC Year: 2000-2010 Tot: 340 (574) RC, RD: 28.2, 9.0% Post hoc Multivariable (+) Hypothesis generation UKHCDOR, IC, SCYear: 2000-2010 Tot: 300 (407) RC, RD: 23.8, 11.3% Time effect, Refacto, RODIN effect Generate alternative hypothesis France CoagR, IC, SCYear: 2000-2010 Tot: 234 (303) RC, RD: 30.0, 15.0% “center” effect Multivariable (-) RODIN effect ?? Generate a second alternative hypothesis Vezina EUHASS EAHAD IPD P = prospective; R = registry; MC = multiple centers/countries, IC = inception cohort, SC = single country

20 Kreuz W, Gill JC, Rothchild C et al. Thrombosis and Haemostasis 2005; 93:457-467 15% inhibitor rate with Kogenate (1997-2001)

21 Evidence profiling StudyDesignMain resultinterpretationContribution RODINP, R, IC, MC Year: 2000-2010 Tot: 340 (574) RC, RD: 28.2, 9.0% Post hocHypothesis generation UKHCDOR, IC, SCYear: 2000-2010 Tot: 300 (407) RC, RD: 23.8, 11.3% Time effect, B-DD f-VIII, RODIN effect Generate alternative hypothesis France CR, IC, SCYear: 2000-2010 Tot: 234 (303) RC, RD: 30.0, 15.0% Strong “center” effect RODIN effect ?? Generate a second alternative hypothesis VezinaS, SCY:2005-2010 Tot:86 (99) RC, RD: 36.0, 6.0% Higher rate with Advate You cannot “export” results? EUHASS EAHAD IPD P = prospective; R = registry; MC = multiple centers/countries, IC = inception cohort, SC = single country; S = survey

22 Evidence profiling StudyDesignMain resultinterpretationContribution RODINP, R, IC, MC Year: 2000-2010 Tot: 340 (574) RC, RD: 28.2, 9.0% Post hocHypothesis generation UKHCDOR, IC, SCYear: 2000-2010 Tot: 300 (407) RC, RD: 23.8, 11.3% Time effect, B-DD f-VIII, RODIN effect Generate alternative hypothesis France CR, IC, SCYear: 2000-2010 Tot: 234 (303) RC, RD: 30.0, 15.0% Strong “center” effect RODIN effect ?? Generate a second alternative hypothesis VezinaS, SCY:2005-2010 Tot:86 (99) RC, RD: 36.0, 6.0% Higher rate with Advate You cannot “export” results? EUHASSP, DC, MCY: 2009-2013 Tot: 284 (417) RC, RD: 26.2, 4.5% RODIN effectNon-confirmatory EAHAD IPD P = prospective; R = registry; MC = multiple centers/countries, IC = inception cohort, SC = single country; S = survey; DC = dynamic cohort;

23 EUHASS EUHASS - RODIN P95% CIP Plasma D0.220.110.350.210.100.37 Recomb0.260.220.310.240.190.29 Advate0.260.190.340.260.180.36 Helixate0.320.180.500.330.180.52 Kogenate0.300.220.400.220.130.34 Refacto0.290.170.430.270.150.43

24 Evidence profiling StudyDesignMain resultinterpretationContribution RODINP, R, IC, MC Year: 2000-2010 Tot: 340 (574) RC, RD: 28.2, 9.0% Post hocHypothesis generation UKHCDOR, IC, SCYear: 2000-2010 Tot: 300 (407) RC, RD: 23.8, 11.3% Time effect, B-DD f-VIII, RODIN effect Generate alternative hypothesis France CR, IC, SCYear: 2000-2010 Tot: 234 (303) RC, RD: 30.0, 15.0% Strong “center” effect RODIN effect ?? Generate a second alternative hypothesis VezinaS, SCY:2005-2010 Tot:86 (99) RC, RD: 36.0, 6.0% Higher rate with Advate You cannot “export” results? EUHASSP, DC, MCY:2009-2013 Tot:284 (417) RC, RD: 26.2, 4.5% RODIN effectNon-confirmatory EAHAD IPD MA, MCY: 1994-2003 Tot: 80 (761) RC, RD: 40, 6.6% Any of the previous Non confirmatory Direction of effect Inconsistency P = prospective; R = registry; MC = multiple centers/countries, IC = inception cohort, SC = single country; S = survey; DC = dynamic cohort; MA = meta-analysis

25

26 Appraisal: final notes Substantial unexplained variability – UK: by year, RODIN participation – France-Coag: by center effect – RODIN: details unreported !!!! “Discordant” evidence – From different designs Meta-analysis Dynamic cohort – From different populations ??? PTP EUHASS, Xi

27 Overview 1)Assessing causality: methodological notes 2)Appraising data on the concentrate dependent risk of inhibitors 3)Implications and perspectives

28 Randomized controlled trial – Objective: ruling out OR 1.6 – Sample size requirements

29 Implications If we trust RODIN & Co, we would have to: – Consider extensive testing in at least 150 PUPs for 50 ED before feeling safe – Consider implications for PTPs

30 EUHASS – PTPs Advate 0.11 (0.03 – 0.25) Kogenate 0.17 (0.06 - 0.37) OR = 1.54 (0.24 – 12) Xi, PTP meta-analysis Advate 0.10 (0.05 – 0.18) Kogenate 0.26 (0.16 - 0.44) Kogenate 0.11 (0.05 - 0.23) OR = 2.6 (0.88 – 8.8) Aledort BDD meta-analysis Kogenate vs Advate High titer HR = 1.75 (0.05 – 65.5) All inhibitors HR, 2.43 (0.31–19.2) Kogenate Advate

31 Conclusion Is the RODIN & Co party over? The is no free lunch at the “risk of inhibitor study club” Either we accept to adopt better methods for prospective assessment, or we have to adapt to live with some uncertainty

32 Thank you !!! Download these slides at: Hemophilia.mcmaster.ca Join the WAPPS network at: www.wapps-hemo.org

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