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骨工程中的骨髓基质细胞(BMSCs):局限性与最新进展

Bone marrow stromal cells (BMSCs) in bone engineering: limitations and recent advances.

作者信息

Derubeis Anna R, Cancedda Ranieri

机构信息

Istituto Nazionale per la Ricerca sul Cancro, Genova, Italy.

出版信息

Ann Biomed Eng. 2004 Jan;32(1):160-5. doi: 10.1023/b:abme.0000007800.89194.95.

Abstract

Bone marrow stromal cells (BMSCs) have been isolated for the first time by Friedenstein et al. and since then have been considered the progenitor cells for the skeletal tissues. Indeed BMSCs are clonogenic, fibroblastic in shape, and can differentiate along multiple lineages such as osteoblasts, chondrocytes, adipocytes, and hematopoiesis-supportive stroma. When implanted in vivo on a three-dimensional bioceramic scaffold into immunocompromised mice, BMSCs form bone and hematopoiesis-supportive stroma. The ease of harvest from a donor bone marrow together with the ability to form bone in vivo make BMSCs ideal for clinical applications. Thus, ex vivo expanded BMSCs have been employed, first in large animal models, then in human clinical trials, to repair large bone segmental defects. Further investigation of the expanded BMSC population led to the observation that in vitro expansion appears a limiting passage: cells tend to senesce and lose their multidifferentiation potential with time in culture. To overcome these limitations, two approaches have been proposed: (1) identification of the appropriate culture conditions to prevent senescence by possibly selecting a subpopulation with stem cell characteristics, and (2) engineering of the cells by transfection with the telomerase gene to prevent cells from telomere shortening and consequent aging.

摘要

骨髓基质细胞(BMSCs)最早由弗里德斯坦等人分离出来,自那时起就被视为骨骼组织的祖细胞。实际上,BMSCs具有克隆性,呈成纤维细胞形态,并且能够沿着多个谱系分化,如成骨细胞、软骨细胞、脂肪细胞以及支持造血的基质细胞。当将其体内植入免疫缺陷小鼠的三维生物陶瓷支架中时,BMSCs会形成骨骼和支持造血的基质。从供体骨髓中易于获取以及在体内形成骨骼的能力,使得BMSCs成为临床应用的理想选择。因此,体外扩增的BMSCs首先被应用于大型动物模型,随后用于人体临床试验,以修复大段骨缺损。对扩增后的BMSC群体的进一步研究发现,体外扩增似乎存在一个限制传代次数:随着培养时间的推移,细胞往往会衰老并丧失其多分化潜能。为了克服这些限制,人们提出了两种方法:(1)通过可能选择具有干细胞特征的亚群来确定合适的培养条件以防止衰老,(2)通过用端粒酶基因转染对细胞进行工程改造,以防止细胞端粒缩短及随之而来的衰老。

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