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支持细胞调节成年雄性小鼠睾丸血管网络的发育、结构和功能,以影响循环睾酮浓度。

Sertoli Cells Modulate Testicular Vascular Network Development, Structure, and Function to Influence Circulating Testosterone Concentrations in Adult Male Mice.

作者信息

Rebourcet Diane, Wu Junxi, Cruickshanks Lyndsey, Smith Sarah E, Milne Laura, Fernando Anuruddika, Wallace Robert J, Gray Calum D, Hadoke Patrick W F, Mitchell Rod T, O'Shaughnessy Peter J, Smith Lee B

机构信息

Medical Research Council Centre for Reproductive Health (D.R., J.W., L.C., S.E.S., L.M., A.F., R.T.M., L.B.S.), University/BHF Centre for Cardiovascular Science (J.W., P.W.F.H.), and Clinical Research Imaging Centre (C.D.G.), University of Edinburgh, The Queen's Medical Research Institute, Edinburgh EH16 4TJ, United Kingdom; Department of Orthopaedics (R.J.W.), University of Edinburgh, Edinburgh Eh16 4SB, United Kingdom; and Institute of Biodiversity, Animal Health, and Comparative Medicine (P.J.O.), University of Glasgow, Garscube Campus, Glasgow G61 1QH, United Kingdom.

出版信息

Endocrinology. 2016 Jun;157(6):2479-88. doi: 10.1210/en.2016-1156. Epub 2016 May 4.

Abstract

The testicular vasculature forms a complex network, providing oxygenation, micronutrients, and waste clearance from the testis. The vasculature is also instrumental to testis function because it is both the route by which gonadotropins are delivered to the testis and by which T is transported away to target organs. Whether Sertoli cells play a role in regulating the testicular vasculature in postnatal life has never been unequivocally demonstrated. In this study we used models of acute Sertoli cell ablation and acute germ cell ablation to address whether Sertoli cells actively influence vascular structure and function in the adult testis. Our findings suggest that Sertoli cells play a key role in supporting the structure of the testicular vasculature. Ablating Sertoli cells (and germ cells) or germ cells alone results in a similar reduction in testis size, yet only the specific loss of Sertoli cells leads to a reduction in total intratesticular vascular volume, the number of vascular branches, and the numbers of small microvessels; loss of germ cells alone has no effect on the testicular vasculature. These perturbations to the testicular vasculature leads to a reduction in fluid exchange between the vasculature and testicular interstitium, which reduces gonadotropin-stimulated circulating T concentrations, indicative of reduced Leydig cell stimulation and/or reduced secretion of T into the vasculature. These findings describe a new paradigm by which the transport of hormones and other factors into and out of the testis may be influenced by Sertoli cells and highlights these cells as potential targets for enhancing this endocrine relationship.

摘要

睾丸血管系统形成一个复杂的网络,为睾丸提供氧合、微量营养素并清除废物。该血管系统对睾丸功能也至关重要,因为它既是促性腺激素输送到睾丸的途径,也是睾酮运输到靶器官的途径。支持细胞在出生后是否参与调节睾丸血管系统,从未得到明确证实。在本研究中,我们使用急性支持细胞消融模型和急性生殖细胞消融模型,来探讨支持细胞是否积极影响成年睾丸的血管结构和功能。我们的研究结果表明,支持细胞在维持睾丸血管系统结构方面发挥关键作用。消融支持细胞(和生殖细胞)或仅消融生殖细胞,都会导致睾丸大小出现类似程度的减小,但只有支持细胞的特异性缺失会导致睾丸内血管总体积、血管分支数量和小微血管数量减少;仅生殖细胞缺失对睾丸血管系统没有影响。这些对睾丸血管系统的干扰导致血管与睾丸间质之间的液体交换减少,从而降低促性腺激素刺激的循环睾酮浓度,这表明睾丸间质细胞刺激减少和/或睾酮分泌到血管中的量减少。这些发现描述了一种新的模式,即支持细胞可能影响激素和其他因子进出睾丸的运输,并突出了这些细胞作为增强这种内分泌关系潜在靶点的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2f89/4891787/16c7455579db/zee0061685070001.jpg

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