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Sox2(+) 成年干细胞和祖细胞对小鼠的组织再生和存活很重要。

Sox2(+) adult stem and progenitor cells are important for tissue regeneration and survival of mice.

机构信息

Howard Hughes Medical Institute and Department of Stem Cell and Regenerative Biology, Harvard University and Harvard Medical School, Cambridge, MA 02138, USA.

出版信息

Cell Stem Cell. 2011 Oct 4;9(4):317-29. doi: 10.1016/j.stem.2011.09.001.

Abstract

The transcription factor Sox2 maintains the pluripotency of early embryonic cells and regulates the formation of several epithelia during fetal development. Whether Sox2 continues to play a role in adult tissues remains largely unknown. We show here that Sox2 marks adult cells in several epithelial tissues where its expression has not previously been characterized, including the stomach, cervix, anus, testes, lens, and multiple glands. Genetic lineage tracing and transplantation experiments demonstrate that Sox2-expressing cells continuously give rise to mature cell types within these tissues, documenting their self-renewal and differentiation potentials. Consistent with these findings, ablation of Sox2(+) cells in mice results in a disruption of epithelial tissue homeostasis and lethality. Developmental fate mapping reveals that Sox2(+) adult stem cells originate from fetal Sox2(+) tissue progenitors. Thus, our results identify Sox2 expression in numerous adult endodermal and ectodermal stem cell compartments, which are critical for normal tissue regeneration and survival.

摘要

转录因子 Sox2 维持早期胚胎细胞的多能性,并在胎儿发育过程中调节几种上皮组织的形成。Sox2 是否在成人组织中继续发挥作用在很大程度上仍是未知的。我们在这里表明,Sox2 标记了几个上皮组织中的成年细胞,其表达以前没有被描述过,包括胃、宫颈、肛门、睾丸、晶状体和多个腺体。遗传谱系追踪和移植实验表明,Sox2 表达的细胞在这些组织内持续产生成熟的细胞类型,证明了它们的自我更新和分化潜力。与这些发现一致的是,在小鼠中敲除 Sox2(+)细胞会导致上皮组织稳态的破坏和致死。发育命运图谱显示 Sox2(+)成年干细胞源自胎儿 Sox2(+)组织祖细胞。因此,我们的结果表明 Sox2 在许多内胚层和外胚层的成年干细胞区室中表达,这对于正常组织再生和存活至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6dc7/3538360/9f8413a5b76c/nihms328957f1.jpg

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