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Single-cell RNA sequencing reveals profibrotic roles of distinct epithelial and mesenchymal lineages in pulmonary fibrosis

机译:单细胞RNA测序揭示了不同上皮和间充质谱系在肺纤维化中的血压性角色

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摘要

Pulmonary fibrosis (PF) is a form of chronic lung disease characterized by pathologic epithelial remodeling and accumulation of extracellular matrix (ECM). To comprehensively define the cell types, mechanisms, and mediators driving fibrotic remodeling in lungs with PF, we performed single-cell RNA sequencing of single-cell suspensions from 10 nonfibrotic control and 20 PF lungs. Analysis of 114,396 cells identified 31 distinct cell subsets/states. We report that a remarkable shift in epithelial cell phenotypes occurs in the peripheral lung in PF and identify several previously unrecognized epithelial cell phenotypes, including a KRT5sup?/sup / KRT17 sup+/sup pathologic, ECM-producing epithelial cell population that was highly enriched in PF lungs. Multiple fibroblast subtypes were observed to contribute to ECM expansion in a spatially discrete manner. Together, these data provide high-resolution insights into the complexity and plasticity of the distal lung epithelium in human disease and indicate a diversity of epithelial and mesenchymal cells contribute to pathologic lung fibrosis.
机译:肺纤维化(PF)是一种慢性肺病的形式,其特征是通过病理上皮重塑和细胞外基质(ECM)的积累。为了综合定义在用PF的肺部驱动纤维化重塑的细胞类型,机制和介质,我们对来自10个非纤维化控制和20pF肺的单细胞悬浮液进行单细胞RNA测序。分析114,396个细胞鉴定了31个不同的细胞亚群/州。我们认为上皮细胞表型的显着变化发生在PF中的外周肺中,并鉴定几种先前未被识别的上皮细胞表型,包括KRT5 / KRT17 + 病理学,ECM - 在PF肺中富集高度富集的上皮细胞群。观察到多个成纤维细胞亚型以在空间离散的方式上有助于ECM膨胀。这些数据在一起,提供了高分辨率的洞察力,进入人类疾病远端肺上皮的复杂性和可塑性,表明上皮和间充质细胞的多样性有助于病理肺纤维化。

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