Reporting and evaluaton of HIV-related clinical endpoints in two multicenter international clinical trials

Alan R. Lifson; Frank S. Rhame; Waldo H. Belloso; Ulrik B. Dragsted; Wafaa M. El-Sadr; Jose M. Gatell; Jennifer F. Hoy; Eric A. Krum; Ray Nelson; Court Pedersen; Sarah L. Pett; Richard T. Davey; James Neaton; Donald Abrams; Pedro Cahn; Bonaventura Clotet; David Cooper; Janet Darbyshire; Lehrman Sandra; Sean Emery; Ulrich Hengge; H. Clifford Lane; Joep Lange; Guido Levy; Yves Levy; Jens Lundgren; Ron Mitsuyasu; Jean Pierre Routy; Giuseppe Tambussi

doi:10.1310/7MER-XFA7-1762-E2WR

Reporting and evaluaton of HIV-related clinical endpoints in two multicenter international clinical trials

Alan R. Lifson, Frank S. Rhame, Waldo H. Belloso, Ulrik B. Dragsted, Wafaa M. El-Sadr, Jose M. Gatell, Jennifer F. Hoy, Eric A. Krum, Ray Nelson, Court Pedersen, Sarah L. Pett, Richard T. Davey, James Neaton, Donald Abrams, Pedro Cahn, Bonaventura Clotet, David Cooper, Janet Darbyshire, Lehrman Sandra, Sean EmeryUlrich Hengge, H. Clifford Lane, Joep Lange, Guido Levy, Yves Levy, Jens Lundgren, Ron Mitsuyasu, Jean Pierre Routy, Giuseppe Tambussi

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Abstract

Purpose: The processes for reporting and review of progression of HIV disease clinical endpoints are described for two large phase III international clinical trials. Method: SILCAAT and ESPRIT are multicenter randomized HIV trials evaluating the impact of interleukin-2 on disease progression and death in HIV-infected patients receiving antiretroviral therapy. We report definitions used for HIV progression of disease endpoints, procedures for site reporting of such events, processes for independent review of reported events by an Endpoint Review Committee (ERC), and the procedure for adjudication of differences of opinion between reviewers. Results: Of 473 events reported through May 1, 2006, 28% were judged by an ERC to meet "confirmed" criteria and 38% to meet "probable" criteria; 34% were classified "does not meet criteria." For diseases with >5 case reports, the proportion accepted as either "confirmed" or "probable" events was highest for cervical cancer (100%), non-Hodgkin's lymphoma (88%), cryptococcosis (82%), and cryptosporidiosis (80%) and was lowest for HIV encephalopathy (25%), HIV wasting syndrome (33%), and multidermatomal herpes zoster (35%). 25% of cases required adjudication between reviewers before diagnostic certainty was assigned. Conclusion: Important requirements for HIV trials using clinical endpoints include objective definitions of "confirmed" and "probable," a formal reporting process with adequate information and supporting source documentation, evaluation by independent blinded reviewers, and procedures for adjudication.

Original language	English (US)
Pages (from-to)	125-141
Number of pages	17
Journal	HIV Clinical Trials
Volume	7
Issue number	3
DOIs	https://doi.org/10.1310/7MER-XFA7-1762-E2WR
State	Published - May 2006

Keywords

Clinical endpoints
Clinical trials
Human immunodeficiency virus

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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Lifson, A. R., Rhame, F. S., Belloso, W. H., Dragsted, U. B., El-Sadr, W. M., Gatell, J. M., Hoy, J. F., Krum, E. A., Nelson, R., Pedersen, C., Pett, S. L., Davey, R. T., Neaton, J., Abrams, D., Cahn, P., Clotet, B., Cooper, D., Darbyshire, J., Sandra, L., ... Tambussi, G. (2006). Reporting and evaluaton of HIV-related clinical endpoints in two multicenter international clinical trials. HIV Clinical Trials, 7(3), 125-141. https://doi.org/10.1310/7MER-XFA7-1762-E2WR

Lifson, AR, Rhame, FS, Belloso, WH, Dragsted, UB, El-Sadr, WM, Gatell, JM, Hoy, JF, Krum, EA, Nelson, R, Pedersen, C, Pett, SL, Davey, RT, Neaton, J, Abrams, D, Cahn, P, Clotet, B, Cooper, D, Darbyshire, J, Sandra, L, Emery, S, Hengge, U, Lane, HC, Lange, J, Levy, G, Levy, Y, Lundgren, J, Mitsuyasu, R, Routy, JP & Tambussi, G 2006, 'Reporting and evaluaton of HIV-related clinical endpoints in two multicenter international clinical trials', HIV Clinical Trials, vol. 7, no. 3, pp. 125-141. https://doi.org/10.1310/7MER-XFA7-1762-E2WR

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abstract = "Purpose: The processes for reporting and review of progression of HIV disease clinical endpoints are described for two large phase III international clinical trials. Method: SILCAAT and ESPRIT are multicenter randomized HIV trials evaluating the impact of interleukin-2 on disease progression and death in HIV-infected patients receiving antiretroviral therapy. We report definitions used for HIV progression of disease endpoints, procedures for site reporting of such events, processes for independent review of reported events by an Endpoint Review Committee (ERC), and the procedure for adjudication of differences of opinion between reviewers. Results: Of 473 events reported through May 1, 2006, 28% were judged by an ERC to meet {"}confirmed{"} criteria and 38% to meet {"}probable{"} criteria; 34% were classified {"}does not meet criteria.{"} For diseases with >5 case reports, the proportion accepted as either {"}confirmed{"} or {"}probable{"} events was highest for cervical cancer (100%), non-Hodgkin's lymphoma (88%), cryptococcosis (82%), and cryptosporidiosis (80%) and was lowest for HIV encephalopathy (25%), HIV wasting syndrome (33%), and multidermatomal herpes zoster (35%). 25% of cases required adjudication between reviewers before diagnostic certainty was assigned. Conclusion: Important requirements for HIV trials using clinical endpoints include objective definitions of {"}confirmed{"} and {"}probable,{"} a formal reporting process with adequate information and supporting source documentation, evaluation by independent blinded reviewers, and procedures for adjudication.",

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author = "Lifson, {Alan R.} and Rhame, {Frank S.} and Belloso, {Waldo H.} and Dragsted, {Ulrik B.} and El-Sadr, {Wafaa M.} and Gatell, {Jose M.} and Hoy, {Jennifer F.} and Krum, {Eric A.} and Ray Nelson and Court Pedersen and Pett, {Sarah L.} and Davey, {Richard T.} and James Neaton and Donald Abrams and Pedro Cahn and Bonaventura Clotet and David Cooper and Janet Darbyshire and Lehrman Sandra and Sean Emery and Ulrich Hengge and Lane, {H. Clifford} and Joep Lange and Guido Levy and Yves Levy and Jens Lundgren and Ron Mitsuyasu and Routy, {Jean Pierre} and Giuseppe Tambussi",

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T1 - Reporting and evaluaton of HIV-related clinical endpoints in two multicenter international clinical trials

AU - Lifson, Alan R.

AU - Rhame, Frank S.

AU - Belloso, Waldo H.

AU - Dragsted, Ulrik B.

AU - El-Sadr, Wafaa M.

AU - Gatell, Jose M.

AU - Hoy, Jennifer F.

AU - Krum, Eric A.

AU - Nelson, Ray

AU - Pedersen, Court

AU - Pett, Sarah L.

AU - Davey, Richard T.

AU - Neaton, James

AU - Abrams, Donald

AU - Cahn, Pedro

AU - Clotet, Bonaventura

AU - Cooper, David

AU - Darbyshire, Janet

AU - Sandra, Lehrman

AU - Emery, Sean

AU - Hengge, Ulrich

AU - Lane, H. Clifford

AU - Lange, Joep

AU - Levy, Guido

AU - Levy, Yves

AU - Lundgren, Jens

AU - Mitsuyasu, Ron

AU - Routy, Jean Pierre

AU - Tambussi, Giuseppe

PY - 2006/5

Y1 - 2006/5

N2 - Purpose: The processes for reporting and review of progression of HIV disease clinical endpoints are described for two large phase III international clinical trials. Method: SILCAAT and ESPRIT are multicenter randomized HIV trials evaluating the impact of interleukin-2 on disease progression and death in HIV-infected patients receiving antiretroviral therapy. We report definitions used for HIV progression of disease endpoints, procedures for site reporting of such events, processes for independent review of reported events by an Endpoint Review Committee (ERC), and the procedure for adjudication of differences of opinion between reviewers. Results: Of 473 events reported through May 1, 2006, 28% were judged by an ERC to meet "confirmed" criteria and 38% to meet "probable" criteria; 34% were classified "does not meet criteria." For diseases with >5 case reports, the proportion accepted as either "confirmed" or "probable" events was highest for cervical cancer (100%), non-Hodgkin's lymphoma (88%), cryptococcosis (82%), and cryptosporidiosis (80%) and was lowest for HIV encephalopathy (25%), HIV wasting syndrome (33%), and multidermatomal herpes zoster (35%). 25% of cases required adjudication between reviewers before diagnostic certainty was assigned. Conclusion: Important requirements for HIV trials using clinical endpoints include objective definitions of "confirmed" and "probable," a formal reporting process with adequate information and supporting source documentation, evaluation by independent blinded reviewers, and procedures for adjudication.

AB - Purpose: The processes for reporting and review of progression of HIV disease clinical endpoints are described for two large phase III international clinical trials. Method: SILCAAT and ESPRIT are multicenter randomized HIV trials evaluating the impact of interleukin-2 on disease progression and death in HIV-infected patients receiving antiretroviral therapy. We report definitions used for HIV progression of disease endpoints, procedures for site reporting of such events, processes for independent review of reported events by an Endpoint Review Committee (ERC), and the procedure for adjudication of differences of opinion between reviewers. Results: Of 473 events reported through May 1, 2006, 28% were judged by an ERC to meet "confirmed" criteria and 38% to meet "probable" criteria; 34% were classified "does not meet criteria." For diseases with >5 case reports, the proportion accepted as either "confirmed" or "probable" events was highest for cervical cancer (100%), non-Hodgkin's lymphoma (88%), cryptococcosis (82%), and cryptosporidiosis (80%) and was lowest for HIV encephalopathy (25%), HIV wasting syndrome (33%), and multidermatomal herpes zoster (35%). 25% of cases required adjudication between reviewers before diagnostic certainty was assigned. Conclusion: Important requirements for HIV trials using clinical endpoints include objective definitions of "confirmed" and "probable," a formal reporting process with adequate information and supporting source documentation, evaluation by independent blinded reviewers, and procedures for adjudication.

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KW - Human immunodeficiency virus

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AN - SCOPUS:33748155708

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ER -

Reporting and evaluaton of HIV-related clinical endpoints in two multicenter international clinical trials

Abstract

Keywords

UN SDGs

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