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胆酸盐预处理的肾刷状缘膜囊泡中反转取向的H(+) -ATP酶的特性研究

Characterization of inside-out oriented H(+)-ATPases in cholate-pretreated renal brush-border membrane vesicles.

作者信息

Simon B J, Burckhardt G

机构信息

Max-Planck-Institut für Biophysik, Frankfurt/Main, Federal Republic of Germany.

出版信息

J Membr Biol. 1990 Aug;117(2):141-51. doi: 10.1007/BF01868681.

Abstract

Exposure of porcine renal brush-border membrane vesicles to 1.2% cholate and subsequent detergent removal by dialysis reorients almost all N-ethylmaleimide (NEM)-sensitive ATPases from the vesicle inside to the outside. ATP addition to cholate-pretreated, but not to intact, vesicles causes H+ uptake as visualized by the delta pH indicator, acridine orange. The reoriented H(+)-pump is electrogenic because permeant extravesicular anions or intravesicular K+ plus valinomycin enhance H+ transport. ATP stimulates H+ uptake with an apparent Km of 93 microM. Support of H+ uptake and Pi liberation by ATP greater than GTP approximately ITP greater than UTP indicates a preference for ATP and utilization of other nucleotides at lower efficiency. ADP is a potent, competitive inhibitor of ATP-driven H+ uptake (Ki, 24 microM), Mg2+ and Mn2+ support ATP-driven H+ uptake, but Ca2+, Ba2+, and Zn2+ do not, 1 mM Zn2+ inhibits MgATP-driven H+ transport completely. NEM-sensitive Pi liberation is stimulated by Mg2+ and Mg2+ and, unlike H+ uptake, also by Ca2+ suggesting Ca2(+)-dependent ATP hydrolysis unrelated to H+ transport. The inside-out oriented H(+)-pump is relatively insensitive toward oligomycin, azide, N,N'-dicyclohexylcarbodiimide (DCCD) and vanadate, but efficiently inhibited by NEM (apparent Ki, 0.77 microM), and 4-chloro-7-nitro-benzoxa-1,3-diazole (NBD-Cl; apparent Ki, 0.39 microM). Taken together, the H(+)-ATPase of proximal tubular brush-border membranes exhibits characteristics very similar to those of "vacuolar type" (V-type) H(+)-ATPases. Hence, V-type H(+)-ATPases occur not only in intracellular organelles but also in specialized plasma membrane areas.

摘要

将猪肾刷状缘膜囊泡暴露于1.2%的胆酸盐中,随后通过透析去除去污剂,几乎可使所有对N - 乙基马来酰亚胺(NEM)敏感的ATP酶从囊泡内部重新定向到外部。向经胆酸盐预处理而非完整的囊泡中添加ATP会导致H⁺摄取,这可通过δpH指示剂吖啶橙观察到。重新定向的H⁺泵是生电的,因为可渗透的囊泡外阴离子或囊泡内K⁺加缬氨霉素会增强H⁺运输。ATP刺激H⁺摄取,其表观Km为93μM。ATP对H⁺摄取和Pi释放的支持作用大于GTP,约大于ITP大于UTP,表明对ATP有偏好,对其他核苷酸的利用效率较低。ADP是ATP驱动的H⁺摄取的强效竞争性抑制剂(Ki,24μM),Mg²⁺和Mn²⁺支持ATP驱动的H⁺摄取,但Ca²⁺、Ba²⁺和Zn²⁺则不然,1 mM Zn²⁺完全抑制MgATP驱动的H⁺运输。Mg²⁺和Mg²⁺刺激对NEM敏感的Pi释放,与H⁺摄取不同的是,Ca²⁺也能刺激,这表明存在与H⁺运输无关的Ca²⁺依赖性ATP水解。外翻取向的H⁺泵对寡霉素、叠氮化物、N,N'-二环己基碳二亚胺(DCCD)和钒酸盐相对不敏感,但能被NEM(表观Ki,0.77μM)和4 - 氯 - 7 - 硝基 - 苯并恶唑 - 1,3 - 二唑(NBD - Cl;表观Ki,0.39μM)有效抑制。综上所述,近端肾小管刷状缘膜的H⁺ - ATP酶表现出与“液泡型”(V型)H⁺ - ATP酶非常相似的特性。因此,V型H⁺ - ATP酶不仅存在于细胞内细胞器中,也存在于特殊的质膜区域。

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