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哺乳动物干细胞龛中的异细胞分子接触。

Heterocellular molecular contacts in the mammalian stem cell niche.

机构信息

Ultrastructural Pathology Laboratory, 'Victor Babeș' National Institute of Pathology, Bucharest, Romania; Department of Cellular & Molecular Biology and Histology, School of Medicine, 'Carol Davila' University of Medicine and Pharmacy, Bucharest, Romania.

Ultrastructural Pathology Laboratory, 'Victor Babeș' National Institute of Pathology, Bucharest, Romania; Department of Neurology, School of Medicine, 'Carol Davila', University of Medicine and Pharmacy, Bucharest, Romania.

出版信息

Eur J Cell Biol. 2018 Aug;97(6):442-461. doi: 10.1016/j.ejcb.2018.07.001. Epub 2018 Jul 7.

Abstract

Adult tissue homeostasis and repair relies on prompt and appropriate intervention by tissue-specific adult stem cells (SCs). SCs have the ability to self-renew; upon appropriate stimulation, they proliferate and give rise to specialized cells. An array of environmental signals is important for maintenance of the SC pool and SC survival, behavior, and fate. Within this special microenvironment, commonly known as the stem cell niche (SCN), SC behavior and fate are regulated by soluble molecules and direct molecular contacts via adhesion molecules providing connections to local supporting cells and the extracellular matrix. Besides the extensively discussed array of soluble molecules, the expression of adhesion molecules and molecular contacts is another fundamental mechanism regulating niche occupancy and SC mobilization upon activation. Some adhesion molecules are differentially expressed and have tissue-specific consequences, likely reflecting the structural differences in niche composition and design, especially the presence or absence of a stromal counterpart. However, the distribution and identity of intercellular molecular contacts for adhesion and adhesion-mediated signaling within stromal and non-stromal SCN have not been thoroughly studied. This review highlights common details or significant differences in cell-to-cell contacts within representative stromal and non-stromal niches that could unveil new standpoints for stem cell biology and therapy.

摘要

成人组织的稳态和修复依赖于组织特异性成体干细胞(SCs)的快速和适当干预。SCs 具有自我更新的能力;在适当的刺激下,它们会增殖并产生专门的细胞。一系列环境信号对于维持 SC 池和 SC 存活、行为和命运至关重要。在这个特殊的微环境中,通常被称为干细胞龛(SCN),SCs 的行为和命运受到可溶性分子和通过黏附分子的直接分子接触的调节,这些黏附分子提供了与局部支持细胞和细胞外基质的连接。除了广泛讨论的可溶性分子外,黏附分子的表达和分子接触是另一种调节龛位占据和 SC 激活时动员的基本机制。一些黏附分子表达不同,具有组织特异性的后果,可能反映了龛位组成和设计的结构差异,特别是基质对应物的存在或缺失。然而,细胞间黏附分子和黏附介导的信号转导的分子接触在基质和非基质 SCN 中的分布和身份尚未得到深入研究。这篇综述强调了代表性基质和非基质龛位中细胞间接触的共同细节或显著差异,这可能为干细胞生物学和治疗揭示新的观点。

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