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对缺血性骨骼肌中成纤维细胞转录组的分析。

Analyses of the pericyte transcriptome in ischemic skeletal muscles.

机构信息

Department of Biophysics, Escola Paulista de Medicina, Federal University of São Paulo, Rua Mirassol 207, São Paulo, SP, 04044-010, Brazil.

Department of Zoology, University of São Paulo, São Paulo, Brazil.

出版信息

Stem Cell Res Ther. 2021 Mar 16;12(1):183. doi: 10.1186/s13287-021-02247-3.

Abstract

BACKGROUND

Peripheral arterial disease (PAD) affects millions of people and compromises quality of life. Critical limb ischemia (CLI), which is the most advanced stage of PAD, can cause nonhealing ulcers and strong chronic pain, and it shortens the patients' life expectancy. Cell-based angiogenic therapies are becoming a real therapeutic approach to treat CLI. Pericytes are cells that surround vascular endothelial cells to reinforce vessel integrity and regulate local blood pressure and metabolism. In the past decade, researchers also found that pericytes may function as stem or progenitor cells in the body, showing the potential to differentiate into several cell types. We investigated the gene expression profiles of pericytes during the early stages of limb ischemia, as well as the alterations in pericyte subpopulations to better understand the behavior of pericytes under ischemic conditions.

METHODS

In this study, we used a hindlimb ischemia model to mimic CLI in C57/BL6 mice and explore the role of pericytes in regeneration. To this end, muscle pericytes were isolated at different time points after the induction of ischemia. The phenotypes and transcriptomic profiles of the pericytes isolated at these discrete time points were assessed using flow cytometry and RNA sequencing.

RESULTS

Ischemia triggered proliferation and migration and upregulated the expression of myogenesis-related transcripts in pericytes. Furthermore, the transcriptomic analysis also revealed that pericytes induce or upregulate the expression of a number of cytokines with effects on endothelial cells, leukocyte chemoattraction, or the activation of inflammatory cells.

CONCLUSIONS

Our findings provide a database that will improve our understanding of skeletal muscle pericyte biology under ischemic conditions, which may be useful for the development of novel pericyte-based cell and gene therapies.

摘要

背景

外周动脉疾病(PAD)影响着数百万人的生活,降低了生活质量。严重肢体缺血(CLI)是 PAD 的最严重阶段,可导致难以愈合的溃疡和强烈的慢性疼痛,并缩短患者的预期寿命。基于细胞的血管生成疗法正在成为治疗 CLI 的一种真正的治疗方法。周细胞环绕血管内皮细胞,以增强血管完整性并调节局部血压和代谢,是血管系统中的关键细胞。在过去的十年中,研究人员还发现周细胞可能在体内发挥干细胞或祖细胞的功能,具有分化为多种细胞类型的潜力。我们研究了肢体缺血早期周细胞的基因表达谱,以及周细胞亚群的变化,以更好地了解周细胞在缺血条件下的行为。

方法

在这项研究中,我们使用后肢缺血模型模拟 C57/BL6 小鼠的 CLI,并探索周细胞在再生中的作用。为此,我们在诱导缺血后不同时间点分离肌肉周细胞。使用流式细胞术和 RNA 测序评估在这些离散时间点分离的周细胞的表型和转录组谱。

结果

缺血触发了周细胞的增殖和迁移,并上调了肌生成相关转录物的表达。此外,转录组分析还表明,周细胞诱导或上调了许多细胞因子的表达,这些细胞因子对内皮细胞、白细胞趋化作用或炎症细胞的激活具有影响。

结论

我们的研究结果提供了一个数据库,将有助于我们了解缺血条件下骨骼肌周细胞的生物学特性,这可能对新型周细胞为基础的细胞和基因治疗的发展有用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8768/7962292/9ed54fba7b3b/13287_2021_2247_Fig1_HTML.jpg

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