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结直肠黏膜下 PDGFRα 细胞的转录组谱分析揭示了几种细胞选择性标记物。

Transcriptome profiling of subepithelial PDGFRα cells in colonic mucosa reveals several cell-selective markers.

机构信息

Department of Physiology and Cell Biology, University of Nevada School of Medicine, Reno, Nevada, United States of America.

Department of Internal Medicine, Division of Gastroenterology and Hepatology, University of Lowa, Lowa City, Lowa, United States of America.

出版信息

PLoS One. 2022 May 13;17(5):e0261743. doi: 10.1371/journal.pone.0261743. eCollection 2022.

Abstract

Subepithelial platelet-derived growth factor receptor alpha (PDGFRα)+ cells found in the colonic mucosal tissue come in close contact with epithelial cells, immune cells, neurons, capillaries, and lymphatic networks. Mucosal subepithelial PDGFRα+ cells (MuPαC) are important regulators in various intestinal diseases including fibrosis and inflammation. However, the transcriptome of MuPαC has not yet been elucidated. Using Pdgfra-eGFP mice and flow cytometry, we isolated colonic MuPαC and obtained their transcriptome data. In analyzing the transcriptome, we identified three novel, and selectively expressed, markers (Adamdec1, Fin1, and Col6a4) found in MuPαC. In addition, we identified a unique set of MuPαC-enriched genetic signatures including groups of growth factors, transcription factors, gap junction proteins, extracellular proteins, receptors, cytokines, protein kinases, phosphatases, and peptidases. These selective groups of genetic signatures are linked to the unique cellular identity and function of MuPαC. Furthermore, we have added this MuPαC transcriptome data to our Smooth Muscle Genome Browser that contains the transcriptome data of jejunal and colonic smooth muscle cells (SMC), interstitial cells of Cajal (ICC), and smooth muscle resident PDGFRα+ cells: (https://med.unr.edu/physio/transcriptome). This online resource provides a comprehensive reference of all currently known genetic transcripts expressed in primary MuPαC in the colon along with smooth muscle resident PDGFRα cells, SMC, and ICC in the murine colon and jejunum.

摘要

在结肠黏膜组织中发现的黏膜下血小板衍生生长因子受体 alpha(PDGFRα)+细胞与上皮细胞、免疫细胞、神经元、毛细血管和淋巴网络密切接触。黏膜下 PDGFRα+细胞(MuPαC)是各种肠道疾病(包括纤维化和炎症)的重要调节因子。然而,MuPαC 的转录组尚未阐明。使用 Pdgfra-eGFP 小鼠和流式细胞术,我们分离了结肠 MuPαC 并获得了它们的转录组数据。在分析转录组时,我们鉴定了三个在 MuPαC 中选择性表达的新标记物(Adamdec1、Fin1 和 Col6a4)。此外,我们鉴定了一组独特的 MuPαC 富集的遗传特征,包括生长因子、转录因子、间隙连接蛋白、细胞外蛋白、受体、细胞因子、蛋白激酶、磷酸酶和肽酶。这些选择性的遗传特征群与 MuPαC 的独特细胞身份和功能有关。此外,我们已将此 MuPαC 转录组数据添加到我们的平滑肌基因组浏览器中,该浏览器包含空肠和结肠平滑肌细胞(SMC)、Cajal 间质细胞(ICC)和平滑肌驻留 PDGFRα+细胞的转录组数据:(https://med.unr.edu/physio/transcriptome)。这个在线资源为在结肠中发现的原代 MuPαC 以及在鼠结肠和空肠中发现的平滑肌驻留 PDGFRα 细胞、SMC 和 ICC 中表达的所有当前已知遗传转录物提供了全面的参考。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c4ed/9106222/a6bb45a382f6/pone.0261743.g001.jpg

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