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人肺泡I型细胞中与衰老相关的分子变化

Aging-Associated Molecular Changes in Human Alveolar Type I Cells.

作者信息

Liu Xue, Zhang Xuexi, Liang Jiurong, Noble Paul W, Jiang Dianhua

机构信息

Department of Medicine and Women's Guild Lung Institute, Cedars-Sinai Medical Center, Los Angeles, CA 90048, USA.

Department of Biomedical Sciences, Cedars-Sinai Medical Center, Los Angeles, CA 90048, USA.

出版信息

J Respir Biol Transl Med. 2024 Sep;1(3). doi: 10.35534/jrbtm.2024.10012. Epub 2024 Jul 22.

Abstract

Human alveolar type I (AT1) cells are specialized epithelial cells that line the alveoli in the lungs where gas exchange occurs. The primary function of AT1 cells is not only to facilitate efficient gas exchange between the air and the blood in the lungs, but also to contribute to the structural integrity of the alveoli to maintain lung function and homeostasis. Aging has notable effects on the structure, function, and regenerative capacity of human AT1 cells. However, our understanding of the molecular mechanisms driving these age-related changes in AT1 cells remains limited. Leveraging a recent single-cell transcriptomics dataset we generated on healthy human lungs, we identified a series of significant molecular alterations in AT1 cells from aged lungs. Notably, the aged AT1 cells exhibited increased cellular senescence and chemokine gene expression, alongside diminished epithelial features such as decreases in cell junctions, endocytosis, and pulmonary matrisome gene expression. Gene set analyses also indicated that aged AT1 cells were resistant to apoptosis, a crucial mechanism for turnover and renewal of AT1 cells, thereby ensuring alveolar integrity and function. Further research on these alterations is imperative to fully elucidate the impact on AT1 cells and is indispensable for developing effective therapies to preserve lung function and promote healthy aging.

摘要

人肺泡I型(AT1)细胞是一种特殊的上皮细胞,排列在肺部进行气体交换的肺泡内。AT1细胞的主要功能不仅是促进肺内空气与血液之间的高效气体交换,还对肺泡的结构完整性做出贡献,以维持肺功能和内环境稳定。衰老对人AT1细胞的结构、功能和再生能力有显著影响。然而,我们对驱动AT1细胞这些与年龄相关变化的分子机制的了解仍然有限。利用我们最近生成的关于健康人肺的单细胞转录组学数据集,我们在老年肺的AT1细胞中鉴定出一系列显著的分子改变。值得注意的是,老年AT1细胞表现出细胞衰老增加和趋化因子基因表达增加,同时上皮特征减少,如细胞连接、内吞作用和肺基质组基因表达降低。基因集分析还表明,老年AT1细胞对凋亡具有抗性,而凋亡是AT1细胞更新和再生的关键机制,从而确保肺泡的完整性和功能。对这些改变进行进一步研究对于充分阐明其对AT1细胞的影响至关重要,并且对于开发有效的疗法以维持肺功能和促进健康衰老不可或缺。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/598c/11361087/7ee561ea9c9e/nihms-2014370-f0001.jpg

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