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Large-Scale Drug Screen Identifies FDA-Approved Drugs for Repurposing in Sickle-Cell Disease

机译:大规模药物筛选识别FDA批准的药物用于在镰状细胞病中重新估算

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摘要

Sickle-cell disease (SCD) is a debilitating hematological disorder with very few approved treatment options. Therapeutic reactivation of fetal hemoglobin (HbF) is one of the most pursued methods for ameliorating the systemic manifestations of SCD. Despite this, very few pharmacological agents have advanced to clinical trials or marketing for use. In this study, we report the development of an HbF in situ intracellular immunoblot assay coupled to a high-throughput drug screen to identify Food and Drug Administration (FDA) approved drugs that can be repurposed clinically for treatment of SCD. Using this assay we evaluated the National Institute of Health (NIH) Clinical Collection (NCC), a publicly available library of 725 small molecules, and found nine candidates that can significantly re-express HbF in erythroid cell lines as well as primary erythroblasts derived from SCD patients. Furthermore, we show the strong effects on HbF expression of these candidates to occur with minimal cytotoxicity in 7 of the 9 drugs. Given these data and their proven history of use for other indications, we hypothesize that several of these candidate drugs warrant further investigation for use in SCD.
机译:镰状细胞疾病(SCD)是一种令人衰弱的血液障碍,批准的治疗方案很少。胎儿血红蛋白(HBF)的治疗重新激活是改善SCD的全身表现的最追求的方法之一。尽管如此,很少有药物药剂已经前进至临床试验或营销。在这项研究中,我们报告了含有高通量药物筛选的原位细胞内免疫印迹测定的HBF的开发,以鉴定食物和药物管理局(FDA)批准的药物,可临床治疗SCD。使用此测定,我们评估了国家健康研究所(NIH)临床收集(NCC),一个公开可用的725个小分子库,并发现九个候选物可以在红细胞细胞系中显着重新表达HBF,以及衍生自的原发性红细胞SCD患者。此外,我们展示了9种药物中7种中最小的细胞毒性发生了这些候选物的HBF表达的强烈影响。鉴于这些数据及其证明的使用历史为其他迹象,我们假设这些候选药物中的几个人在SCD中进一步调查。

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