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端粒功能障碍环境导致静止状态的丧失和造血干细胞功能的固有损伤。

Telomere dysfunctional environment induces loss of quiescence and inherent impairments of hematopoietic stem cell function.

机构信息

Institute of Molecular Medicine and Max-Planck-Research Group on Stem Cell Aging, University of Ulm, 89081 Ulm, Germany.

出版信息

Aging Cell. 2012 Jun;11(3):449-55. doi: 10.1111/j.1474-9726.2012.00802.x. Epub 2012 Feb 22.

Abstract

Previous studies have shown that telomere dysfunction induces alteration in the systemic (circulatory) environment impairing the differentiation of hematopoietic stem cells (HSCs) but these defects can be reverted by re-exposing HSCs to an environment with functional telomeres. In contrast, HSC intrinsic telomere dysfunction induces permanent and irreversible limitations in the repopulation capacity partially depending on the induction of checkpoints such as cell cycle arrest, differentiation, or apoptosis. It is currently unknown whether telomere dysfunctional environment can induce irreversible, cell intrinsic defects impairing the function of HSCs. Here, we analyzed the functional reserves of murine, wild-type HSCs with intact telomeres that were transiently exposed to a telomere dysfunctional environment (late generation telomerase knockout mice) or to an environment with functional telomeres (wild-type mice). The study shows that the telomere dysfunctional environment leads to irreversible impairments in the repopulation capacity of wild-type HSCs. The telomere dysfunctional environment impaired the maintenance of HSC quiescent. Moreover, the study shows that alterations in the systemic (circulatory) environment rather than the bone stromal niche induce loss of stem cell quiescence and irreversible deficiencies of HSCs exposed to a telomere dysfunctional environment.

摘要

先前的研究表明,端粒功能障碍会导致全身(循环)环境发生改变,从而损害造血干细胞(HSCs)的分化,但这些缺陷可以通过将 HSCs 重新暴露于具有功能端粒的环境中得到逆转。相比之下,HSC 内在的端粒功能障碍会导致其在重建能力方面出现永久性和不可逆转的限制,这部分取决于细胞周期停滞、分化或凋亡等检查点的诱导。目前尚不清楚端粒功能障碍的环境是否会导致不可逆的、细胞内在的缺陷,从而损害 HSCs 的功能。在这里,我们分析了具有完整端粒的野生型小鼠 HSCs 的功能储备,这些 HSCs 短暂暴露于端粒功能障碍的环境(端粒酶敲除鼠的晚期世代)或功能端粒的环境(野生型小鼠)中。研究表明,端粒功能障碍的环境会导致野生型 HSCs 的重建能力出现不可逆转的损伤。端粒功能障碍的环境损害了 HSC 静止的维持。此外,研究还表明,是全身(循环)环境的改变,而不是骨基质龛,导致暴露于端粒功能障碍环境中的静止性干细胞丧失和 HSCs 的不可逆转缺陷。

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