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剪接事件和转录组变化对肾结石形成的影响。

Effects of alternative splicing events and transcriptome changes on kidney stone formation.

机构信息

Department of Urology, The First Affiliated Hospital of Anhui Medical University, Hefei, China.

Institute of Urology, Anhui Medical University, Hefei, China.

出版信息

Urolithiasis. 2022 Apr;50(2):131-140. doi: 10.1007/s00240-021-01293-z. Epub 2022 Jan 8.

Abstract

During the development of urinary stone disease, the formation of tiny crystals that adhere to the renal tubular epithelium induces epithelial cell damage. This damage and repair of the epithelium is associated with the establishment of more crystal adhesion sites, which in turn stimulates further crystal adhesion and, eventually, stone formation. Deposited crystals typically cause changes in epithelial cell gene expression, such as transcriptome changes and alternative splicing events. Although considered important for regulating gene expression, alternative splicing has not been reported in studies related to kidney stones. To date, whether alternative splicing events are involved in the regulation of stone formation and whether crystallographic cell interactions are regulated by alternative splicing at the transcriptional level have remained unknown. Therefore, we conducted RNA sequencing and alternative splicing-related bioassays by modeling the in vitro stone environment. Many alternative splicing events were associated with crystallographic cell interactions. Moreover, these events regulated transcription and significantly affected the capacity of crystals to adhere to renal tubular epithelial cells and regulate apoptosis.

摘要

在尿石症的发展过程中,微小晶体的形成黏附在肾小管上皮细胞上,诱导上皮细胞损伤。这种上皮细胞的损伤和修复与更多晶体黏附位点的建立有关,这反过来又刺激了进一步的晶体黏附,并最终导致结石形成。沉积的晶体通常会导致上皮细胞基因表达的变化,如转录组变化和选择性剪接事件。尽管选择性剪接被认为对基因表达的调控很重要,但在与肾结石相关的研究中尚未报道过。迄今为止,选择性剪接事件是否参与结石形成的调控,以及晶体细胞相互作用是否在转录水平上受到选择性剪接的调控仍不清楚。因此,我们通过模拟体外结石环境进行了 RNA 测序和选择性剪接相关的生物分析。许多选择性剪接事件与晶体细胞相互作用有关。此外,这些事件调节转录,显著影响晶体黏附于肾小管上皮细胞的能力,并调节细胞凋亡。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3848/8956516/f8947f449849/240_2021_1293_Fig1_HTML.jpg

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