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. 2018 Oct 4;12(10):e0006497.
doi: 10.1371/journal.pntd.0006497. eCollection 2018 Oct.

Development of standard clinical endpoints for use in dengue interventional trials

Kay M Tomashek  1 Bridget Wills  2 Lucy Chai See Lum  3 Laurent Thomas  4 Anna Durbin  5 Yee-Sin Leo  6 Norma de Bosch  7 Elsa Rojas  8 Kim Hendrickx  9 Martin Erpicum  10 Liane Agulto  1 Thomas Jaenisch  11 Hasitha Tissera  12 Piyarat Suntarattiwong  13 Beth Ann Collers  14 Derek Wallace  15 Alexander C Schmidt  16 Alexander Precioso  17   18 Federico Narvaez  19 Stephen J Thomas  20 Robert Edelman  21 João Bosco Siqueira  22 M Cristina Cassetti  1 Walla Dempsey  1 Duane J Gubler  23
Affiliations

Development of standard clinical endpoints for use in dengue interventional trials

Kay M Tomashek et al. PLoS Negl Trop Dis. .

Abstract

Dengue is a major public health problem worldwide. Although several drug candidates have been evaluated in randomized controlled trials, none has been effective and at present, early recognition of severe dengue and timely supportive care are used to reduce mortality. While the first dengue vaccine was recently licensed, and several other candidates are in late stage clinical trials, future decisions regarding widespread deployment of vaccines and/or therapeutics will require evidence of product safety, efficacy and effectiveness. Standard, quantifiable clinical endpoints are needed to ensure reproducibility and comparability of research findings. To address this need, we established a working group of dengue researchers and public health specialists to develop standardized endpoints and work towards consensus opinion on those endpoints. After discussion at two working group meetings and presentations at international conferences, a Delphi methodology-based query was used to finalize and operationalize the clinical endpoints. Participants were asked to select the best endpoints from proposed definitions or offer revised/new definitions, and to indicate whether contributing items should be designated as optional or required. After the third round of inquiry, 70% or greater agreement was reached on moderate and severe plasma leakage, moderate and severe bleeding, acute hepatitis and acute liver failure, and moderate and severe neurologic disease. There was less agreement regarding moderate and severe thrombocytopenia and moderate and severe myocarditis. Notably, 68% of participants agreed that a 50,000 to 20,000 mm3 platelet range be used to define moderate thrombocytopenia; however, they remained divided on whether a rapid decreasing trend or one platelet count should be case defining. While at least 70% agreement was reached on most endpoints, the process identified areas for further evaluation and standardization within the context of ongoing clinical studies. These endpoints can be used to harmonize data collection and improve comparability between dengue clinical trials.

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Conflict of interest statement

Beth-Ann G. Coller is an employee, shareholder and patent inventor of Merck & Co., Inc., Kenilworth, New Jersey, United States of America. Robert Edelman is a paid consultant to Takeda Pharmaceutical Company vaccine trials for service as Chairman of the Data and Safety Monitoring Board (DSMB) of Takeda's Tetravalent Dengue Vaccine Program. Alexander C. Schmidt is an employee and shareholder of the GlaxoSmithKline plc (GSK), Brentford, London, United Kingdom. Stephen J. Thomas has performed both paid and unpaid consultations and safety reviews for GSK Vaccines, Merck, Takeda, Sanofi Pasteur, Chugai Pharma, Themisbio, and Primevax. Derek Wallace is an employee of Takeda Pharmaceuticals International AG, Zurich, Switzerland. Bridget Wills is a paid consultant on the DSMB for the Takeda vaccine trials. No other authors have declared that a competing interest exists.

Figures

Fig 1
Fig 1. Participants in the Delphi inquiry.
See this image and copyright information in PMC

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