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Adapting High-Throughput Screening Methods and Assays for Biocontainment Laboratories

机译:适用于生物防护实验室的高通量筛选方法和分析

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摘要

High-throughput screening (HTS) has been integrated into the drug discovery process, and multiple assay formats have been widely used in many different disease areas but with limited focus on infectious agents. In recent years, there has been an increase in the number of HTS campaigns using infectious wild-type pathogens rather than surrogates or biochemical pathogen-derived targets. Concurrently, enhanced emerging pathogen surveillance and increased human mobility have resulted in an increase in the emergence and dissemination of infectious human pathogens with serious public health, economic, and social implications at global levels. Adapting the HTS drug discovery process to biocontainment laboratories to develop new drugs for these previously uncharacterized and highly pathogenic agents is now feasible, but HTS at higher biosafety levels (BSL) presents a number of unique challenges. HTS has been conducted with multiple bacterial and viral pathogens at both BSL-2 and BSL-3, and pilot screens have recently been extended to BSL-4 environments for both Nipah and Ebola viruses. These recent successful efforts demonstrate that HTS can be safely conducted at the highest levels of biological containment. This review outlines the specific issues that must be considered in the execution of an HTS drug discovery program for high-containment pathogens. We present an overview of the requirements for HTS in high-level biocontainment laboratories.
机译:高通量筛选(HTS)已集成到药物发现过程中,多种测定形式已广泛用于许多不同的疾病领域,但对传染原的关注有限。近年来,使用传染性野生型病原体而不是替代物或生化病原体来源的靶标进行的HTS运动数量有所增加。同时,增强的新兴病原体监测和增加的人类流动性导致感染性人类病原体的出现和传播增加,在全球范围内具有严重的公共卫生,经济和社会影响。现在,使HTS药物发现过程适应生物遏制实验室的需要,以开发针对这些先前未表征的和高致病性药物的新药是可行的,但是更高的生物安全水平(BSL)的HTS提出了许多独特的挑战。已在BSL-2和BSL-3上对多种细菌和病毒病原体进行了HTS,最近针对Nipah和埃博拉病毒的初筛已扩展到BSL-4环境。这些最近的成功努力表明,可以在最高水平的生物隔离中安全地进行高温超导。这篇评论概述了针对高含量病原体的HTS药物发现计划的执行中必须考虑的特定问题。我们概述了高级生物防护实验室中对HTS的要求。

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