| Literature DB >> 31593599 |
Sophia B Georghiou1, Samuel G Schumacher1, Timothy C Rodwell1, Rebecca E Colman1, Paolo Miotto2, Christopher Gilpin3, Nazir Ismail4,5,6, Camilla Rodrigues7, Rob Warren8, Karin Weyer3, Matteo Zignol3, Sonia Arafah1, Daniela Maria Cirillo2, Claudia M Denkinger1,9.
Abstract
The development and implementation of rapid molecular diagnostics for tuberculosis (TB) drug-susceptibility testing is critical to inform treatment of patients and to prevent the emergence and spread of resistance. Optimal trial planning for existing tests and those in development will be critical to rapidly gather the evidence necessary to inform World Health Organization review and to support potential policy recommendations. The evidence necessary includes an assessment of the performance for TB and resistance detection as well as an assessment of the operational characteristics of these platforms. The performance assessment should include analytical studies to confirm the limit of detection and assay ability to detect mutations conferring resistance across globally representative strains. The analytical evaluation is typically followed by multisite clinical evaluation studies to confirm diagnostic performance in sites and populations of intended use. This paper summarizes the considerations for the design of these analytical and clinical studies.Entities:
Keywords: WHO End TB Strategy; diagnostics; drug-susceptibility testing; target product profile; tuberculosis
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Year: 2019 PMID: 31593599 DOI: 10.1093/infdis/jiz106
Source DB: PubMed Journal: J Infect Dis ISSN: 0022-1899 Impact factor: 5.226