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富含血小板的血浆促进人类成肌细胞的扩增,并有利于在更深层次的静止状态下体外生成人类肌肉储备细胞。

Platelet-Rich Plasma Promotes the Expansion of Human Myoblasts and Favors the In Vitro Generation of Human Muscle Reserve Cells in a Deeper State of Quiescence.

机构信息

Department of Orthopedic Surgery, Geneva University Hospitals & Faculty of Medicine, Geneva, Switzerland.

Regen Lab SA, 1052, Le Mont-Sur-Lausanne, Switzerland.

出版信息

Stem Cell Rev Rep. 2024 Oct;20(7):1981-1994. doi: 10.1007/s12015-024-10760-0. Epub 2024 Jul 13.

Abstract

Stem cell therapy holds significant potential for skeletal muscle repair, with in vitro-generated human muscle reserve cells (MuRCs) emerging as a source of quiescent myogenic stem cells that can be injected to enhance muscle regeneration. However, the clinical translation of such therapies is hampered by the need for fetal bovine serum (FBS) during the in vitro generation of human MuRCs. This study aimed to determine whether fresh allogeneic human platelet-rich plasma (PRP) combined or not with hyaluronic acid (PRP-HA) could effectively replace xenogeneic FBS for the ex vivo expansion and differentiation of human primary myoblasts. Cells were cultured in media supplemented with either PRP or PRP-HA and their proliferation rate, cytotoxicity and myogenic differentiation potential were compared with those cultured in media supplemented with FBS. The results showed similar proliferation rates among human myoblasts cultured in PRP, PRP-HA or FBS supplemented media, with no cytotoxic effects. Human myoblasts cultured in PRP or PRP-HA showed reduced fusion ability upon differentiation. Nevertheless, we also observed that human MuRCs generated from PRP or PRP-HA myogenic cultures, exhibited increased Pax7 expression and delayed re-entry into the cell cycle upon reactivation, indicating a deeper quiescent state of human MuRCs. These results suggest that allogeneic human PRP effectively replaces FBS for the ex vivo expansion and differentiation of human myoblasts and favors the in vitro generation of Pax7 human MuRCs, with important implications for the advancement of stem cell-based muscle repair strategies.

摘要

干细胞治疗在骨骼肌修复方面具有重要的潜力,体外生成的人类肌肉储备细胞(MuRCs)作为静止的肌源性干细胞的来源,可通过注射来增强肌肉再生。然而,由于在体外生成人类 MuRCs 时需要胎牛血清(FBS),此类治疗的临床转化受到了阻碍。本研究旨在确定新鲜同种异体富血小板血浆(PRP)是否联合透明质酸(PRP-HA)可有效替代异种 FBS,用于体外扩增和分化人类原代成肌细胞。细胞在添加 PRP 或 PRP-HA 的培养基中培养,将其增殖率、细胞毒性和肌源性分化潜能与添加 FBS 的培养基中培养的细胞进行比较。结果表明,在 PRP、PRP-HA 或 FBS 补充培养基中培养的人类成肌细胞增殖率相似,没有细胞毒性。在分化过程中,在 PRP 或 PRP-HA 中培养的人类成肌细胞融合能力降低。尽管如此,我们还观察到,从 PRP 或 PRP-HA 肌生成培养物中生成的人类 MuRCs,表现出 Pax7 表达增加和再激活后重新进入细胞周期的延迟,表明人类 MuRCs 处于更深的静止状态。这些结果表明,同种异体人类 PRP 可有效替代 FBS,用于体外扩增和分化人类成肌细胞,并有利于 Pax7 人类 MuRCs 的体外生成,这对推进基于干细胞的肌肉修复策略具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5968/11445347/a256bf12ed2a/12015_2024_10760_Fig1_HTML.jpg

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