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药物转运体与血睾屏障功能。

Drug transporters and blood--testis barrier function.

机构信息

The Mary M. Wohlford Laboratory for Male Contraceptive Research, Center for Biomedical Research, Population Council, New York, New York 10065, USA.

出版信息

J Endocrinol. 2011 Jun;209(3):337-51. doi: 10.1530/JOE-10-0474. Epub 2011 Apr 6.

Abstract

The blood--testis barrier (BTB) creates an immunological barrier that segregates the seminiferous epithelium into the basal and apical compartment. Thus, meiosis I/II and post-meiotic germ cell development take place in a specialized microenvironment in the apical compartment behind the BTB and these events are being shielded from the host immune system. If unwanted drugs and/or chemicals enter the apical compartment from the microvessels in the interstitium via the basal compartment, efflux pumps (e.g. P-glycoprotein) located in Sertoli cells and/or spermatids can actively transport these molecules out of the apical compartment. However, the mechanism(s) by which influx pumps regulate the entry of drugs/chemicals into the apical compartment is not known. In this study, a solute carrier (SLC) transporter organic anion transporting polypeptide 3 (Oatp3, Slco1a5) was shown to be an integrated component of the N-cadherin-based adhesion complex at the BTB. However, a knockdown of Oatp3 alone or in combination with three other major Sertoli cell drug influx pumps, namely Slc22a5, Slco6b1, and Slco6c1, by RNAi using corresponding specific siRNA duplexes failed to perturb the Sertoli cell tight junction (TJ) permeability barrier function. Yet, the transport of [(3)H]adjudin, a potential male contraceptive that is considered a toxicant to spermatogenesis, across the BTB was impeded following the knockdown of either Oatp3 or all the four SLC transporters. In short, even though drug transporters (e.g. influx pumps) are integrated components of the adhesion protein complexes at the BTB, they are not involved in regulating the Sertoli cell TJ permeability barrier function, instead they are only involved in the transport of drugs, such as adjudin, across the immunological barrier at the BTB.

摘要

血睾屏障(BTB)形成了一道免疫屏障,将生精上皮分隔成基底和顶部分区。因此,减数分裂 I/II 和减数后精原细胞发育发生在 BTB 后面的顶部分区的特殊微环境中,这些事件受到宿主免疫系统的保护。如果不想要的药物和/或化学物质通过基底室从间质中的微血管进入顶部分区,位于支持细胞和/或精子细胞中的外排泵(例如 P 糖蛋白)可以将这些分子主动从顶部分区运出。然而,流入泵调节药物/化学物质进入顶部分区的机制尚不清楚。在这项研究中,一种溶质载体(SLC)转运蛋白有机阴离子转运多肽 3(Oatp3,Slco1a5)被证明是 BTB 上基于 N-钙粘蛋白的黏附复合物的一个组成部分。然而,通过使用相应的特异性 siRNA 双链体进行 RNAi 单独或组合敲低 Oatp3 以及另外三个主要的支持细胞药物流入泵 Slc22a5、Slco6b1 和 Slco6c1,未能扰乱支持细胞紧密连接(TJ)通透性屏障功能。然而,在用 Oatp3 或所有四个 SLC 转运蛋白敲低后,潜在的雄性避孕药 [3H]adjudin 的转运被阻止穿过 BTB。简而言之,尽管药物转运蛋白(例如流入泵)是 BTB 上黏附蛋白复合物的组成部分,但它们不参与调节支持细胞 TJ 通透性屏障功能,而是仅参与药物(如 adjudin)穿过 BTB 的免疫屏障的转运。

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