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增生体外模型中的克隆选择、衰减与分化

Clonal selection, attenuation and differentiation in an in vitro model of hyperplasia.

作者信息

Martin G M, Sprague C A, Norwood T H, Pendergrass W R

出版信息

Am J Pathol. 1974 Jan;74(1):137-54.

Abstract

Observations of the growth kinetics and morphologies of clones and subclones of diploid human skin fibroblast cultures lead to the working hypothesis that these cells, presumably like their counterparts in healing wounds, constitute a differentiating system. There is attenuation of the growth of serial clones, with continual selection for more vigorous stem cells. The latter segregate daughter cells of varying growth potential, including a class of cells which may be regarded as terminally differentiating; we propose that such cells may be histiocytes or macrophages. These studies a) demonstrate extensive epigenetic heterogeneity in fibroblast cultures, b) suggest that hyperplastic foci may be monoclonal or oligoclonal, c) rule out a simple biologic clock mechanism as an explanation of clonal senescence, d) suggest a new approach to the analysis of various inborn errors of metabolism, such as Werner's Syndrome.

摘要

对二倍体人皮肤成纤维细胞培养物的克隆及亚克隆的生长动力学和形态学观察,得出了一个可行的假说:这些细胞,大概类似于愈合伤口中的对应细胞,构成了一个分化系统。连续克隆的生长会减弱,同时持续选择更具活力的干细胞。后者分离出具有不同生长潜能的子细胞,包括一类可被视为终末分化的细胞;我们提出这类细胞可能是组织细胞或巨噬细胞。这些研究:a)证明了成纤维细胞培养物中存在广泛的表观遗传异质性;b)表明增生性病灶可能是单克隆或寡克隆的;c)排除了简单的生物钟机制作为克隆衰老的解释;d)提出了一种分析各种先天性代谢缺陷(如沃纳综合征)的新方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8e11/1910722/5b37b84ad353/amjpathol00477-0154-a.jpg

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