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A suite of phenotypic assays to ensure pipeline diversity when prioritizing drug-like Cryptosporidium growth inhibitors

机译:一套表型测定法可在确定药物样隐孢子虫生长抑制剂的优先级时确保管道多样性

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摘要

Cryptosporidiosis is a leading cause of life-threatening diarrhea in children, and the only currently approved drug is ineffective in malnourished children and immunocompromised people. Large-scale phenotypic screens are ongoing to identify anticryptosporidial compounds, but optimal approaches to prioritize inhibitors and establish a mechanistically diverse drug development pipeline are unknown. Here, we present a panel of medium-throughput mode of action assays that enable testing of compounds in several stages of the Cryptosporidium life cycle. Phenotypic profiles are given for thirty-nine anticryptosporidials. Using a clustering algorithm, the compounds sort by phenotypic profile into distinct groups of inhibitors that are either chemical analogs (i.e. same molecular mechanism of action (MMOA)) or known to have similar MMOA. Furthermore, compounds belonging to multiple phenotypic clusters are efficacious in a chronic mouse model of cryptosporidiosis. This suite of phenotypic assays should ensure a drug development pipeline with diverse MMOA without the need to identify underlying mechanisms.
机译:隐孢子虫病是导致儿童致命性腹泻的主要原因,目前唯一批准的药物对营养不良的儿童和免疫功能低下的人无效。正在进行大规模的表型筛选以鉴定抗隐孢子虫化合物,但是对抑制剂进行优先排序并建立机制多样的药物开发流程的最佳方法尚不清楚。在这里,我们介绍了一组中通量的作用模式测定法,该方法能够在隐孢子虫生命周期的多个阶段中测试化合物。给出了39种抗隐孢子虫的表型概况。使用聚类算法,这些化合物按表型分布分为不同的抑制剂组,这些抑制剂要么是化学类似物(即相同的分子作用机理(MMOA)),要么已知具有相似的MMOA。此外,属于多个表型簇的化合物在隐孢子虫病的慢性小鼠模型中是有效的。这套表型测定法应确保具有多种MMOA的药物开发流程,而无需确定潜在的机制。

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