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ADP-氟铝酸盐复合物在嗜热芽孢杆菌PS3的F1-ATPase野生型和突变型α3β3γ亚复合物的两个催化位点协同形成。

ADP-fluoroaluminate complexes are formed cooperatively at two catalytic sites of wild-type and mutant alpha3beta3gamma subcomplexes of the F1-ATPase from the thermophilic Bacillus PS3.

作者信息

Dou C, Grodsky N B, Matsui T, Yoshida M, Allison W S

机构信息

Department of Chemistry & Biochemistry, School of Medicine, University of California at San Diego, La Jolla 92093, USA.

出版信息

Biochemistry. 1997 Mar 25;36(12):3719-27. doi: 10.1021/bi962353+.

Abstract

Addition of Al3+ and F- to the alpha3beta3gamma subcomplex of the TF1-ATPase containing MgADP in one catalytic site causes slow, complete inactivation as the ADP-fluoroaluminate complex is formed. This conflicts with the "bisite" stochastic model suggested earlier (Issartel, J. P., Dupuis, A., Lunardi, J. & Vignais, P. V. (1991) Biochemistry 30, 4726-4733] on the finding that complete inactivation of the bovine mitochondrial F1-ATPase by Al3+, F-, Mg2+, and excess ADP occurs as ADP-fluoroaluminate complexes form in two catalytic sites. When Al3+ and F- were added to alpha3beta3gamma containing MgADP in two catalytic sites, inactivation accelerated 8-fold, indicating catalytic to catalytic site cooperativity. When added to alpha3beta3gamma containing MgADP bound to one or two catalytic sites prior to addition of Al3+ and F-, phosphate inhibits formation of the ADP-fluoroaluminate complex. When introduced after adding 200 microM ADP plus Mg2+ to alpha3beta3gamma, but before adding Al3+ and F-, phosphate accelerated formation of the ADP-fluoroaluminate complex 3-fold. Sulfite accelerated formation of the ADP-fluoroaluminate complex 9-fold when 200 microM ADP plus Mg2+ was added to alpha3beta3gamma before adding Al3+ and F-. The accelerations induced by phosphate or sulfite in the presence of excess ADP and Mg2+ suggest noncatalytic to catalytic site cooperativity. When Al3+ and F- were added to the (alphaD261N)3beta3gamma subcomplex containing MgADP in a single catalytic site, the ADP-fluoroaluminate complex formed at least 10-fold more slowly than observed with wild-type under the same conditions. Therefore, the catalytic site containing MgADP recognizes the alphaD261N substitution when noncatalytic sites are empty. Cross-linking alpha to gamma or beta to gamma by oxidizing the (alphaA396C)3beta3(gammaA22C) and alpha3(betaD390C)3(gammaS90C) subcomplexes, respectively, abolishes cooperative formation of ADP-fluoroaluminate complexes in two catalytic sites. ADP-fluoroaluminate complex formation is restricted to a single catalytic site in the oxidized double mutants. The alpha3beta3delta subcomplex does not form an inhibitory ADP-fluoroaluminate complex under any of the conditions examined for the alpha3beta3gamma subcomplexes.

摘要

在一个催化位点含有MgADP的TF1 - ATPase的α3β3γ亚复合物中添加Al3 +和F - ,随着ADP - 氟铝酸盐复合物的形成,会导致缓慢、完全失活。这与之前提出的“双位点”随机模型[伊萨尔特尔,J.P.,迪皮伊,A.,卢纳尔迪,J.和维尼亚斯,P.V.(1991年)《生物化学》30,4726 - 4733]相冲突,该模型认为牛线粒体F1 - ATPase在两个催化位点形成ADP - 氟铝酸盐复合物时会被Al3 +、F - 、Mg2 +和过量ADP完全失活。当在两个催化位点向含有MgADP的α3β3γ添加Al3 +和F - 时,失活加速了8倍,表明催化位点之间存在协同作用。在添加Al3 +和F - 之前,当向一个或两个催化位点结合有MgADP的α3β3γ添加磷酸盐时,会抑制ADP - 氟铝酸盐复合物的形成。当在向α3β3γ添加200μM ADP加Mg2 +之后,但在添加Al3 +和F - 之前引入磷酸盐时,磷酸盐使ADP - 氟铝酸盐复合物的形成加速了3倍。当在添加Al3 +和F - 之前向α3β3γ添加200μM ADP加Mg2 +时,亚硫酸盐使ADP - 氟铝酸盐复合物的形成加速了9倍。在过量ADP和Mg2 +存在下磷酸盐或亚硫酸盐诱导的加速表明非催化位点与催化位点之间存在协同作用。当在单个催化位点向含有MgADP的(αD261N)3β3γ亚复合物添加Al3 +和F - 时,在相同条件下,ADP - 氟铝酸盐复合物的形成比野生型慢至少10倍。因此,当非催化位点为空时,含有MgADP的催化位点能识别αD261N取代。分别通过氧化(αA396C)3β3(γA22C)和α3(βD390C)3(γS90C)亚复合物使α与γ或β与γ交联,会消除两个催化位点中ADP - 氟铝酸盐复合物的协同形成。在氧化的双突变体中,ADP - 氟铝酸盐复合物的形成仅限于单个催化位点。在针对α3β3γ亚复合物所研究的任何条件下,α3β3δ亚复合物都不会形成抑制性的ADP - 氟铝酸盐复合物。

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