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首页> 外文期刊>Biochemistry >THE ALPHA(3)BETA(3)GAMMA COMPLEX OF THE F-1-ATPASE FROM THERMOPHILIC BACILLUS PS3 CONTAINING THE ALPHA-D261N SUBSTITUTION FAILS TO DISSOCIATE INHIBITORY MGADP FROM A CATALYTIC SITE WHEN ATP BINDS TO NONCATALYTIC SITES
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THE ALPHA(3)BETA(3)GAMMA COMPLEX OF THE F-1-ATPASE FROM THERMOPHILIC BACILLUS PS3 CONTAINING THE ALPHA-D261N SUBSTITUTION FAILS TO DISSOCIATE INHIBITORY MGADP FROM A CATALYTIC SITE WHEN ATP BINDS TO NONCATALYTIC SITES

机译:ATP结合到非催化位点时,包含ALPHA-D261N取代基的嗜热芽孢杆菌PS3的F-1-ATPase的ALPHA(3)BETA(3)γ络合物无法从催化位点解离抑制性MGADP

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ATP hydrolyses by the wild-type alpha(3) beta(3) gamma and mutant (alpha D261N)(3) beta(3) gamma subcomplexes of the F-1-ATPase from the thermophilic Bacillus PS3 have been compared. The wild-type complex hydrolyzes 50 mu M ATP in three kinetic phases: a burst decelerates to an intermediate phase, which then gradually accelerates to a final rate, In contrast, the mutant complex hydrolyzes 50 mu M or 2 mM ATP in two kinetic phases, The mutation abolishes acceleration from the intermediate phase to a faster final rate, Both the wild-type and mutant complexes hydrolyze 4TP with a lag after loading a catalytic site with MgADP. The rate of the MgADP-loaded wild-type complex rapidly accelerates and approaches that observed for the wild-type apo-complex. The MgADP-loaded mutant complex hydrolyzes ATP with a more pronounced lag, and the gradually accelerating rate approaches the slow, final rate observed with the mutant ape-complex. Lauryl dimethylamide oxide (LDAO) stimulates hydrolysis of 2 mM ATP catalyzed by wild-type and mutant complexes 4- and 7.5-fold, respectively. The rate of release of [H-3]ADP from the Mg[H-3]ADP-loaded mutant complex during hydrolysis of 40 mu M ATP is slower than observed with the wild-type complex. LDAO increases the rate of release of [H-3]ADP from the preloaded wild-type and mutant complexes during hydrolysis of 40 mu M ATP, Again, release is slower with the mutant complex. When the wild-type and mutant complexes are irradiated in the presence of 2-N-3-[H-3]ADP plus Mg2+ or 2-N-3-[H-3]ATP plus Mg2+ and azide, the same extent of labeling of noncatalytic sites is observed. Whereas ADP and ATP protect noncatalytic sites of the wild-type and mutant complexes about equally from labeling by 2-N-3-[H-3]ADP or 2-N-3-[H-3]ATP, respectively, AMP-PNP provides little protection of noncatalytic sites of the mutant complex. The results suggest that the substitution does not prevent binding of ADP or ATP to noncatalytic sites, but rather that it affects cross-talk between liganded noncatalytic sites and catalytic sites which is necessary to promote dissociation of inhibitory MgADP.
机译:比较了野生型alpha(3)beta(3)γ和来自嗜热芽孢杆菌PS3的F-1-ATPase的突变体(alpha D261N)(3)beta(3)γ亚复合物的ATP水解情况。野生型复合物在三个动力学相中水解50μM ATP:爆发减速到中间相,然后逐渐加速至最终速率。相反,突变复合物在两个动力学相中水解50μM或2 mM ATP。 ,该突变消除了从中间阶段加速到更快的最终速率。在将MgADP装载到催化位点后,野生型和突变体复合物均会延迟水解4TP。加载MgADP的野生型复合物的速率迅速加快,并且接近野生型载脂蛋白复合物所观察到的速度。加载MgADP的突变体复合物水解ATP的滞后更加明显,并且逐渐加速的速率接近突变体猿复合体观察到的缓慢的最终速率。月桂基二甲酰胺氧化物(LDAO)分别刺激野生型和突变型复合物4倍和7.5倍催化的2 mM ATP水解。从40 M M ATP的水解过程中,从装载Mg [H-3] ADP的突变体复合物中释放[H-3] ADP的速率比在野生型复合物中观察到的要慢。 LDAO在水解40μMATP的过程中提高了[H-3] ADP从预加载的野生型和突变体复合物中的释放速率。再次,突变体复合物的释放较慢。当在2-N-3- [H-3] ADP加Mg2 +或2-N-3- [H-3] ATP加Mg2 +和叠氮化物的存在下辐照野生型和突变型复合物时,观察到非催化位点的标记。而ADP和ATP分别保护野生型和突变体复合物的非催化位点,使其分别被2-N-3- [H-3] ADP或2-N-3- [H-3] ATP,AMP- PNP对突变复合物的非催化位点几乎没有提供保护。结果表明该取代不会阻止ADP或ATP与非催化位点结合,而是会影响配体非催化位点与催化位点之间的串扰,这对于促进抑制性MgADP的解离是必不可少的。

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