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寡霉素敏感性赋予蛋白与线粒体腺苷三磷酸酶复合体F0区段之间的相互作用:F1区段的协同效应。

Interaction between the oligomycin sensitivity conferring protein and the F0 sector of the mitochondrial adenosinetriphosphatase complex: cooperative effect of the F1 sector.

作者信息

Dupuis A, Vignais P V

出版信息

Biochemistry. 1987 Jan 27;26(2):410-8. doi: 10.1021/bi00376a011.

Abstract

Beef heart mitchondrial oligomycin sensitivity conferring protein (OSCP) labeled with [14C]-N-ethylmaleimide ([14C]OSCP) at the only cysteine residue, Cys-118, present in the sequence [Ovchinnikov, Y. A., Modyanov, N. N., Grinkevich, V. A., Aldanova, N. A., Trubetskaya, O. E., Nazimov, I.V., Hundal, T., & Ernster, L. (1984) FEBS Lett. 166, 19-22] exhibits full biological activity in a reconstituted F0-F1 system [Dupuis, A., Issartel, J. P., Lunardi, J., Satre, M., & Vignais, P. V. (1985) Biochemistry 24, 728-733]. The binding parameters of [14C]OSCP with respect to the F0 sector of submitochondrial particles largely depleted of F1 and OSCP (AUA particles) have been explored. In the absence of added F1, a limited number of high-affinity OSCP binding sites were detected in the AUA particles (20-40 pmol/mg of particles); under these conditions, the low-affinity binding sites for OSCP were essentially not saturable. Addition of F1 to the particles promoted high-affinity binding for OSCP, with an apparent Kd of 5 nM, a value 16 times lower than the Kd relative to the binding of OSCP to F1 in the absence of particles. Saturation of the F1 and OSCP binding sites of AUA particles was attained with about 200 pmol of both F1 and OSCP added per milligram of particles. The oligomycin-dependent inhibition of F1-ATPase bound to AUA particles was assayed as a function of bound OSCP. At subsaturating concentrations of F1, the dose-effect curves were rectilinear until inhibition of ATPase activity by oligomycin was virtually complete, and maximal inhibition was obtained for an OSCP to F1 ratio of 1 (mol/mol).(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

牛心线粒体寡霉素敏感性赋予蛋白(OSCP)在其序列中唯一的半胱氨酸残基Cys - 118处用[¹⁴C] - N - 乙基马来酰亚胺([¹⁴C]OSCP)标记后[奥夫钦尼科夫,Y. A.,莫迪亚诺夫,N. N.,格林凯维奇,V. A.,阿尔达诺娃,N. A.,特鲁别茨卡娅,O. E.,纳齐莫夫,I. V.,洪达尔,T.,& 厄恩斯特,L.(1984年)《欧洲生物化学学会联合会快报》166,19 - 22],在重构的F₀ - F₁系统中表现出完全的生物活性[迪皮伊,A.,伊萨尔特尔,J. P.,卢纳尔迪,J.,萨特雷,M.,& 维尼亚伊斯,P. V.(1985年)《生物化学》24,728 - 733]。已经研究了[¹⁴C]OSCP与大量缺乏F₁和OSCP的亚线粒体颗粒(AUA颗粒)的F₀部分的结合参数。在不添加F₁的情况下,在AUA颗粒中检测到有限数量的高亲和力OSCP结合位点(20 - 40 pmol/mg颗粒);在这些条件下,OSCP的低亲和力结合位点基本上不饱和。向颗粒中添加F₁促进了对OSCP的高亲和力结合,表观解离常数(Kd)为5 nM,该值比在没有颗粒的情况下OSCP与F₁结合的Kd低16倍。每毫克颗粒添加约200 pmol的F₁和OSCP时,AUA颗粒的F₁和OSCP结合位点达到饱和。测定了与AUA颗粒结合的F₁ - ATP酶的寡霉素依赖性抑制作用与结合的OSCP的关系。在F₁亚饱和浓度下,剂量 - 效应曲线是直线的,直到寡霉素对ATP酶活性的抑制几乎完全,并且当OSCP与F₁的摩尔比为1(mol/mol)时获得最大抑制。(摘要截短于250字)

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