Literature DB >> 10077169

Clinical trials using HIV-1 RNA-based primary endpoints: statistical analysis and potential biases.

I C Marschner1, R A Betensky, V DeGruttola, S M Hammer, D R Kuritzkes.   

Abstract

Clinical trial endpoints based on magnitude of reduction in HIV-1 RNA levels provide an important complement to endpoints based on percentage of patients achieving complete virologic suppression. However, interpretation of magnitude of reduction can be biased by measurement limitations of virologic assays, particularly lower and upper limits of quantification. Using data from two AIDS Clinical Trials Group (ACTG) studies, widely used crude methods of analyzing HIV-1 RNA reductions were compared with methods that take into account censoring of HIV-1 RNA measurements. Such methods include Kaplan-Meier and censored regression analyses. It was found that standard crude methods of analysis consistently underestimated treatment effects. In some cases, the bias induced by crude methods masked statistically significant differences between treatment arms. Although statistically significant, adjustment for baseline HIV-1 RNA levels had little effect on estimated treatment differences. Furthermore, convenient parametric analyses performed as well as more complex nonparametric analyses. It is concluded that conveniently implemented censored data analyses should be conducted in preference to widely used crude analyses of magnitude of HIV-1 RNA reduction. To obtain complete information about virologic response to antiretroviral therapy, such analyses of magnitude of virologic response should be used to complement analyses of the percentage of patients having complete virologic suppression.

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Year:  1999        PMID: 10077169     DOI: 10.1097/00042560-199903010-00002

Source DB:  PubMed          Journal:  J Acquir Immune Defic Syndr Hum Retrovirol        ISSN: 1077-9450


  9 in total

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Journal:  Lifetime Data Anal       Date:  2004-12       Impact factor: 1.588

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4.  Clinically relevant genotype interpretation of resistance to didanosine.

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Journal:  Antimicrob Agents Chemother       Date:  2005-05       Impact factor: 5.191

5.  Superiority of directly administered antiretroviral therapy over self-administered therapy among HIV-infected drug users: a prospective, randomized, controlled trial.

Authors:  Frederick L Altice; Duncan Smith-Rohrberg Maru; R Douglas Bruce; Sandra A Springer; Gerald H Friedland
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6.  Persistence of virological benefits following directly administered antiretroviral therapy among drug users: results from a randomized controlled trial.

Authors:  Duncan Smith-Rohrberg Maru; Robert Douglas Bruce; Mary Walton; Sandra A Springer; Frederick L Altice
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7.  Investigation of Super Learner Methodology on HIV-1 Small Sample: Application on Jaguar Trial Data.

Authors:  Allal Houssaïni; Lambert Assoumou; Anne Geneviève Marcelin; Jean Michel Molina; Vincent Calvez; Philippe Flandre
Journal:  AIDS Res Treat       Date:  2012-04-03

8.  Statistical analysis of single-copy assays when some observations are zero.

Authors:  Peter Bacchetti; Ronald J Bosch; Eileen P Scully; Xutao Deng; Michael P Busch; Steven G Deeks; Sharon R Lewin
Journal:  J Virus Erad       Date:  2019-09-18

9.  Resumption of HIV replication is associated with monocyte/macrophage derived cytokine and chemokine changes: results from a large international clinical trial.

Authors:  Alessandro Cozzi-Lepri; Martyn A French; John Baxter; Pablo Okhuysen; Montserrat Plana; Jacqueline Neuhaus; Alan Landay
Journal:  AIDS       Date:  2011-06-01       Impact factor: 4.177

  9 in total

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