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别构调节在乙酰羟酸合酶(AHASs)中的作用——同一生物体中同工酶的不同结构和动力学行为。

Allosteric regulation in Acetohydroxyacid Synthases (AHASs)--different structures and kinetic behavior in isozymes in the same organisms.

机构信息

Dept. of Life Sciences, Ben-Gurion University of the Negev, Beer-Sheva, Israel.

出版信息

Arch Biochem Biophys. 2012 Mar 15;519(2):167-74. doi: 10.1016/j.abb.2011.11.025. Epub 2011 Dec 16.

Abstract

Acetohydroxyacid Synthases (AHASs) have separate small regulatory subunits which specifically activate the catalytic subunits with which they are associated. The binding sites for the inhibitory amino acid(s) (valine or leucine) are in the interface between two ACT (small ligand binding) domains, and are apparently found in all AHAS regulatory subunits. However, the structures and the kinetic mechanisms of the different enzymes are very heterogeneous. Among the three isozymes encoded in the enterobacteria, the regulatory patterns are different, and their different responses to the inhibitory end product valine can be rationalized, at least in part, on the basis of the regulatory subunit structures and differences in catalytic mechanisms. The regulatory subunits in "typical" single AHASs found in other bacteria are similar to that of Escherichia coli isozyme AHAS III. Eukaryotic AHASs have more complex regulatory mechanisms and larger regulatory subunits. Such AHASs have two separate ACT sequence domains on the same regulatory polypeptide and can simultaneously bind two amino acids with synergistic effects. Yeast and fungal AHASs have ATP-binding sequence inserts in their regulatory subunits and are activated by MgATP in addition to being inhibited by valine.

摘要

乙酰羟酸合酶(AHASs)具有单独的小调节亚基,它们特异性地激活与其相关的催化亚基。抑制氨基酸(缬氨酸或亮氨酸)的结合位点位于两个 ACT(小配体结合)结构域之间的界面上,并且显然存在于所有 AHAS 调节亚基中。然而,不同酶的结构和动力学机制非常不均匀。在肠杆菌中编码的三种同工酶中,调节模式不同,其对抑制终产物缬氨酸的不同反应至少可以部分基于调节亚基结构和催化机制的差异来合理化。“典型”单个 AHAS 中的调节亚基类似于大肠杆菌同工酶 AHAS III。其他细菌中的其他细菌中的调节亚基类似于大肠杆菌同工酶 AHAS III。真核 AHASs 具有更复杂的调节机制和更大的调节亚基。这种 AHASs 在同一调节多肽上具有两个独立的 ACT 序列结构域,并且可以同时结合两个具有协同作用的氨基酸。酵母和真菌 AHASs 在其调节亚基中具有 ATP 结合序列插入,并且除了被缬氨酸抑制之外,还被 MgATP 激活。

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