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睾丸中细胞与细胞外基质之间的动态相互作用。

Dynamic cross-talk between cells and the extracellular matrix in the testis.

作者信息

Siu Michelle K Y, Cheng C Yan

机构信息

Population Council, Center for Biomedical Research, New York, New York 10021, USA.

出版信息

Bioessays. 2004 Sep;26(9):978-92. doi: 10.1002/bies.20099.

Abstract

In the seminiferous tubule of the mammalian testis, one type A1 spermatogonium (diploid, 2n) divides and differentiates into 256 spermatozoa (haploid, n) during spermatogenesis. To complete spermatogenesis and produce approximately 150 x 10(6) spermatozoa each day in a healthy man, germ cells must migrate progressively across the seminiferous epithelium yet remain attach to the nourishing Sertoli cells. This active cell migration process involves precisely controlled restructuring events at the tight (TJ) and anchoring junctions at the cell-cell interface. While the hormonal events that regulate spermatogenesis by follicle-stimulating hormone and testosterone from the pituitary gland and Leydig cells, respectively, are known, less is known about the mechanism(s) that regulates junction restructuring during germ cell movement in the seminiferous epithelium. The relative position of tight (TJs) and anchoring junctions in the testis is of interest. Sertoli cell TJs that constitute the blood-testis barrier (BTB) are present side by side with anchoring junctions and are adjacent to the basement membrane. This intimate physical association with the TJs, the anchoring junctions and the basement membrane (a modified form of extracellular matrix, ECM) suggests a role for the ECM in the junction dynamics of the testis. Indeed, evidence is accumulating that ECM proteins are crucial to Sertoli cell TJ dynamics. In this review, we discuss the pivotal role of tumor necrosis factor alpha (TNFalpha) on BTB dynamics via its effects on the homeostasis of ECM proteins. In addition, discussion will also be focused on the novel findings regarding the role of non-basement-membrane-associated ECM proteins and components of focal adhesion (a cell-matrix anchoring junction type) in the regulation of junction dynamics in the testis.

摘要

在哺乳动物睾丸的生精小管中,一个A1型精原细胞(二倍体,2n)在精子发生过程中分裂并分化为256个精子(单倍体,n)。为了完成精子发生并使健康男性每天产生约1.5×10⁶个精子,生殖细胞必须逐渐穿过生精上皮,但仍要附着于滋养的支持细胞。这种活跃的细胞迁移过程涉及细胞 - 细胞界面处紧密连接(TJ)和锚定连接的精确控制的重组事件。虽然已知分别由垂体和睾丸间质细胞分泌的促卵泡激素和睾酮调节精子发生的激素事件,但对于调节生精上皮中生殖细胞运动期间连接重组的机制了解较少。睾丸中紧密连接(TJs)和锚定连接的相对位置备受关注。构成血睾屏障(BTB)的支持细胞TJ与锚定连接并排存在,且与基底膜相邻。这种与TJ、锚定连接和基底膜(细胞外基质,ECM的一种修饰形式)的紧密物理关联表明ECM在睾丸连接动力学中发挥作用。事实上,越来越多的证据表明ECM蛋白对支持细胞TJ动力学至关重要。在本综述中,我们讨论肿瘤坏死因子α(TNFα)通过其对ECM蛋白稳态的影响在BTB动力学中的关键作用。此外,讨论还将聚焦于关于非基底膜相关ECM蛋白和粘着斑(一种细胞 - 基质锚定连接类型)成分在调节睾丸连接动力学中作用的新发现。

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