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小鼠原始生殖细胞发育的调控

Regulation of primordial germ cell development in the mouse.

作者信息

De Felici M

机构信息

Department of Public Health and Cell Biology, University of Rome Tor Vergata, Italy.

出版信息

Int J Dev Biol. 2000;44(6):575-80.

Abstract

Primordial germ cells (PGCs) are the founders of the gametes. They arise at the earliest stages of embryonic development and migrate to the gonadal ridges, where they differentiate into oogonia/oocytes in the ovary, and prospermatogonia in the testis. The present article is a review of the main studies undertaken by the author with the aim of clarifying the mechanisms underlying the development of primordial germ cells. Methods for the isolation and purification of migratory and post-migratory mouse PGCs devised in the author's laboratory are first briefly reviewed. Such methods, together with the primary culture of PGCs onto suitable cell feeder layers, have allowed the analysis of important aspects of the control of their development, concerning in particular survival, proliferation and migration of mouse PGCs. Compounds and growth factors affecting PGC numbers in culture have been identified. These include survival anti-apoptotic factors (SCF, LIF) and positive regulators of proliferation (cAMP, PACAPs, RA). Evidence has been provided that the motility of migrating PGCs relies on integrated signals from extracellular matrix molecules and the surrounding somatic cells. Moreover, homotypic PGC-PGC interaction has been evidenced that might play a role in PGC migration and in regulating their development. Several molecules (i.e. integrins, specific types of oligosaccharides, E-cadherin, the tyrosine kinase receptor c-kit) have been found to be expressed on the surface of PGCs and to mediate adhesive interactions of PGCs with the extracellular matrix, somatic cells and neighbouring PGCs.

摘要

原始生殖细胞(PGCs)是配子的起源细胞。它们在胚胎发育的最早阶段产生,并迁移至性腺嵴,在卵巢中分化为卵原细胞/卵母细胞,在睾丸中分化为精原细胞。本文是作者进行的主要研究的综述,旨在阐明原始生殖细胞发育的潜在机制。首先简要回顾作者实验室设计的分离和纯化迁移期及迁移后期小鼠PGCs的方法。这些方法,连同将PGCs原代培养到合适的细胞饲养层上,使得能够分析其发育控制的重要方面,特别是小鼠PGCs的存活、增殖和迁移。已鉴定出影响培养中PGC数量的化合物和生长因子。这些包括存活抗凋亡因子(SCF、LIF)和增殖正调节因子(cAMP、PACAPs、RA)。有证据表明,迁移中的PGCs的运动性依赖于细胞外基质分子和周围体细胞的整合信号。此外,已证明同型PGC-PGC相互作用可能在PGC迁移和调节其发育中起作用。已发现几种分子(即整合素、特定类型的寡糖、E-钙黏蛋白、酪氨酸激酶受体c-kit)在PGCs表面表达,并介导PGCs与细胞外基质、体细胞和相邻PGCs的黏附相互作用。

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