Anzai Naohiko, Jutabha Promsuk, Enomoto Atsushi, Yokoyama Hirokazu, Nonoguchi Hiroshi, Hirata Taku, Shiraya Katsuko, He Xin, Cha Seok Ho, Takeda Michio, Miyazaki Hiroki, Sakata Takeshi, Tomita Kimio, Igarashi Takashi, Kanai Yoshikatsu, Endou Hitoshi
Department of Pharmacology and Toxicology, Kyorin University School of Medicine, Mitaka-shi, Tokyo, Japan.
J Pharmacol Exp Ther. 2005 Nov;315(2):534-44. doi: 10.1124/jpet.105.088583. Epub 2005 Aug 3.
A novel member of the organic anion transporter (OAT) family, Oat5 (Slc22a19), has been reported to transport a naturally occurring mycotoxin, ochratoxin A (OTA). However, neither its endogenous substrate and driving force nor physiological functions have been determined. Herein, we report the functional characterization of rat Oat5 (rOat5), as well as its intrarenal distribution and membrane localization. When expressed in Xenopus laevis oocytes, rOat5 mediated the transport of sulfate conjugates of steroids such as estrone-3-sulfate (E(1)S; K(m) = 18.9 +/- 3.9 microM) and dehydroepiandrosterone sulfate (K(m) = 2.3 +/- 0.2 microM) in a sodium-independent manner, in addition to OTA. The rOat5-mediated E(1)S transport was strongly inhibited by four-carbon (C4) dicarboxylate succinate and longer dicarboxylates (C7-C9). The uptake of [(3)H]E(1)S via rOat5 was significantly trans-stimulated by succinate, and the efflux of [(14)C]succinate was significantly trans-stimulated by E(1)S. A similar trans-stimulatory effect of preloaded succinate on E(1)S uptake was also detected in cells stably expressing rOat5 (S(2) rOat5). rOat5 interacted with chemically heterogenous anionic compounds. The rOat5-mediated E(1)S transport was inhibited by several sulfate conjugates, such as 4-methylumbelliferyl sulfate and beta-estradiol sulfate, but not by glucuronide conjugates. An immunohistochemical study showed that rOat5 was localized at the apical membrane of renal proximal tubules in the corticomedullary region. rOat5 mRNA was expressed in the late segments (S(2) and S(3)) of proximal tubules. These results indicate that rOat5 is renal organic anion/dicarboxylates exchanger and, under physiological conditions, may function as an apical reabsorptive pathway for organic anions in proximal tubules driven by an outward gradient of dicarboxylates.
据报道,有机阴离子转运体(OAT)家族的一个新成员Oat5(Slc22a19)可转运天然存在的霉菌毒素——赭曲霉毒素A(OTA)。然而,其内源性底物、驱动力及生理功能均未明确。在此,我们报道大鼠Oat5(rOat5)的功能特性、肾内分布及膜定位。当在非洲爪蟾卵母细胞中表达时,rOat5除介导OTA转运外,还以不依赖钠的方式介导类固醇硫酸酯(如硫酸雌酮(E(1)S;Km = 18.9±3.9 μM)和硫酸脱氢表雄酮(Km = 2.3±0.2 μM))的转运。rOat5介导的E(1)S转运受到四碳(C4)二羧酸琥珀酸及更长链二羧酸(C7 - C9)的强烈抑制。通过rOat5对[(3)H]E(1)S的摄取受到琥珀酸的显著反刺激,而[(14)C]琥珀酸的流出受到E(1)S的显著反刺激。在稳定表达rOat5的细胞(S(2) rOat5)中也检测到预先加载的琥珀酸对E(1)S摄取具有类似的反刺激作用。rOat5与化学性质不同的阴离子化合物相互作用。rOat5介导的E(1)S转运受到几种硫酸酯(如4 - 甲基伞形酮基硫酸酯和β - 雌二醇硫酸酯)的抑制,但不受葡萄糖醛酸酯的抑制。免疫组织化学研究表明,rOat5定位于肾皮质髓质区近端肾小管的顶端膜。rOat5 mRNA在近端肾小管的晚期节段(S(2)和S(3))表达。这些结果表明,rOat5是肾脏有机阴离子/二羧酸交换体,在生理条件下,可能作为近端肾小管中由二羧酸外向梯度驱动的有机阴离子顶端重吸收途径发挥作用。
