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高通量香烟烟雾处理的支气管肺泡模型用于疾病相关表型化合物筛选。

A high-throughput cigarette smoke-treated bronchosphere model for disease-relevant phenotypic compound screening.

机构信息

Novartis Institutes for Biomedical Research, San Diego, California, United States of America.

出版信息

PLoS One. 2023 Jun 29;18(6):e0287809. doi: 10.1371/journal.pone.0287809. eCollection 2023.

Abstract

Cigarette smoking (CS) is the leading cause of COPD, and identifying the pathways that are driving pathogenesis in the airway due to CS exposure can aid in the discovery of novel therapies for COPD. An additional barrier to the identification of key pathways that are involved in the CS-induced pathogenesis is the difficulty in building relevant and high throughput models that can recapitulate the phenotypic and transcriptomic changes associated with CS exposure. To identify these drivers, we have developed a cigarette smoke extract (CSE)-treated bronchosphere assay in 384-well plate format that exhibits CSE-induced decreases in size and increase in luminal secretion of MUC5AC. Transcriptomic changes in CSE-treated bronchospheres resemble changes that occur in human smokers both with and without COPD compared to healthy groups, indicating that this model can capture human smoking signature. To identify new targets, we ran a small molecule compound deck screening with diversity in target mechanisms of action and identified hit compounds that attenuated CSE induced changes, either decreasing spheroid size or increasing secreted mucus. This work provides insight into the utility of this bronchopshere model to examine human respiratory disease impacted by CSE exposure and the ability to screen for therapeutics to reverse the pathogenic changes caused by CSE.

摘要

吸烟是 COPD 的主要病因,确定由于 CS 暴露导致气道发病机制的途径可以帮助发现 COPD 的新疗法。确定与 CS 诱导的发病机制相关的关键途径的另一个障碍是难以构建能够重现与 CS 暴露相关的表型和转录组变化的相关和高通量模型。为了确定这些驱动因素,我们开发了一种香烟烟雾提取物(CSE)处理的支气管球体测定法,在 384 孔板格式中显示 CSE 诱导的大小减小和 MUC5AC 管腔分泌增加。CSE 处理的支气管球体中的转录组变化与人类吸烟者(无论是否患有 COPD)与健康组相比发生的变化相似,表明该模型可以捕获人类吸烟特征。为了确定新的靶点,我们用具有不同作用机制靶点多样性的小分子化合物库进行了筛选,并鉴定出了能够减轻 CSE 诱导的变化的命中化合物,要么减小球体大小,要么增加分泌的粘液。这项工作深入了解了该支气管球体模型用于检查受 CSE 暴露影响的人类呼吸道疾病的效用,以及筛选用于逆转 CSE 引起的致病变化的治疗方法的能力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/eb0e/10310037/0101e4802b0b/pone.0287809.g001.jpg

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