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利用逆转录病毒整合标记单独鉴定的长寿命和短寿命小鼠造血干细胞克隆。

Long- and short-lived murine hematopoietic stem cell clones individually identified with retroviral integration markers.

作者信息

Capel B, Hawley R G, Mintz B

机构信息

Institute for Cancer Research, Fox Chase Cancer Center, Philadelphia, PA 19111.

出版信息

Blood. 1990 Jun 15;75(12):2267-70.

PMID:2350573
Abstract

The proliferative longevity of totipotent hematopoietic stem cells (THSC) is a limiting factor in normal hematopoiesis and in therapy by cell- or gene-replacement, but has not yet been ascertained. We have followed the long-term fate of individual clones of mouse THSC from fetal liver or adult bone marrow, after labeling in culture, followed by engraftment and serial transplantation in unirradiated W/Wv-C57BL/6 hosts. The ancestor cell of each clone and its mitotic progeny were uniquely identifiable retrospectively by the DNA integration pattern experimentally produced by replication-incompetent recombinant murine retroviruses. These viruses provided physiologically neutral markers. The marked clones proved to be derived from THSC, based on their contributions to a wide array of myeloid and lymphoid blood lineages in the hosts. The label also identified the target cells as the population displaying clonal succession. The various labeled stem cell clones proliferated for substantially different periods of time. The longest observed clone endured, after the original cell was marked, for at least 2 1/2 years--the equivalent of a mouse's lifetime. However, the results suggest that THSC clones are not all long-lived and that even the longest-lived ones may not be potentially immortal. Thus, the unpredictable lifespan of any given THSC clone indicates the desirability of introducing multiple clones in therapeutic transplants.

摘要

全能造血干细胞(THSC)的增殖寿命是正常造血以及细胞或基因替代治疗中的一个限制因素,但尚未确定。我们追踪了来自胎肝或成年骨髓的小鼠THSC单个克隆的长期命运,在培养中进行标记后,接着在未受照射的W/Wv-C57BL/6宿主中进行植入和连续移植。每个克隆的祖细胞及其有丝分裂后代可通过无复制能力的重组鼠逆转录病毒实验产生的DNA整合模式进行独特的回顾性鉴定。这些病毒提供了生理中性标记。基于标记克隆对宿主中广泛的髓系和淋巴系血统的贡献,证明它们源自THSC。该标记还将靶细胞鉴定为显示克隆更替的群体。各种标记的干细胞克隆增殖的时间大不相同。观察到的最长寿克隆在原始细胞被标记后存活了至少2年半——相当于小鼠的一生。然而,结果表明THSC克隆并非都长寿,即使是最长寿的克隆也可能没有潜在的永生能力。因此,任何给定THSC克隆不可预测的寿命表明在治疗性移植中引入多个克隆是可取的。

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