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从不同人体组织分离出的间充质基质细胞的腺苷代谢。

Adenosine metabolism by mesenchymal stromal cells isolated from different human tissues.

作者信息

Galgaro Bruna Campos, Beckenkamp Liziane Raquel, Naasani Liliana I Sous, Wink Márcia Rosângela

机构信息

Laboratório de Biologia Celular, Universidade Federal de Ciências da Saúde de Porto Alegre, UFCSPA, Rua Sarmento Leite, 245, Porto Alegre, RS, CEP 90050-170, Brazil.

出版信息

Hum Cell. 2023 Nov;36(6):2247-2258. doi: 10.1007/s13577-023-00957-9. Epub 2023 Aug 3.

Abstract

Mesenchymal stromal cells (MSCs) have unique biological properties and play important functions, which make them attractive tools for cell-based therapies. The basic mechanisms of these cells are not fully understood. However, the adenosinergic pathway contributes to the main effects attributed to MSCs. Adenosine is a highly immunosuppressive molecule and exerts a central role in inflammation by neutralizing the proinflammatory ATP influence. This nucleoside is produced by purinergic signaling, an important physiological pathway for MSCs, which involves proliferation, migration, differentiation, and apoptosis. Therefore, in this study, we analyzed the extracellular AMP hydrolysis and consequent adenosine production, as well as the expression of CD73 and adenosine receptors on the cell surface of MSCs isolated from different human tissues: dermis (D-MSCs), adipose tissue (AD-MSCs), and umbilical cord (UC-MSCs). All cells confirmed their multipotent capacity by adipogenic, osteogenic, and chondrogenic differentiation, as well as the expression of cell surface markers including CD44 + , CD105 + , and CD90 + . All MSCs expressed similar levels of CD73 and CD26 without a statistical difference among the different tissues, whereas ADA expression was lower in AD-MSCs. In addition, A1R and A3R mRNA levels were higher in D-MSCs and AD-MSCs, respectively. Enzymatic assay showed that AD-MSCs have the highest hydrolysis rate of AMP, leading to increased amount of adenosine production. Moreover, despite all MSCs completely hydrolyze extracellular AMP generating adenosine, the pattern of nucleosides metabolism was different. Therefore, although MSCs share certain characteristics as the multilineage potential and immunophenotype, they show different adenosinergic profiles according to tissue origin.

摘要

间充质基质细胞(MSCs)具有独特的生物学特性并发挥着重要功能,这使其成为基于细胞治疗的有吸引力的工具。这些细胞的基本机制尚未完全了解。然而,腺苷能途径有助于MSCs产生主要效应。腺苷是一种高度免疫抑制分子,通过中和促炎ATP的影响在炎症中发挥核心作用。这种核苷由嘌呤能信号产生,这是MSCs的一条重要生理途径,涉及增殖、迁移、分化和凋亡。因此,在本研究中,我们分析了细胞外AMP水解及随后的腺苷产生,以及从不同人类组织分离的MSCs细胞表面CD73和腺苷受体的表达:真皮(D-MSCs)、脂肪组织(AD-MSCs)和脐带(UC-MSCs)。所有细胞通过脂肪生成、成骨和成软骨分化以及包括CD44 +、CD105 +和CD90 +在内的细胞表面标志物的表达证实了其多能能力。所有MSCs表达相似水平的CD73和CD26,不同组织之间无统计学差异,而ADA表达在AD-MSCs中较低。此外,A1R和A3R mRNA水平分别在D-MSCs和AD-MSCs中较高。酶活性测定表明,AD-MSCs具有最高的AMP水解速率,导致腺苷产生量增加。此外,尽管所有MSCs都能完全水解细胞外AMP生成腺苷,但核苷代谢模式不同。因此,尽管MSCs具有多谱系潜能和免疫表型等某些共同特征,但它们根据组织来源显示出不同的腺苷能谱。

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