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天冬氨酸和谷氨酸对在大鼠心脏线粒体和反向亚线粒体小泡中研究的氧代戊二酸载体的影响。

Effect of aspartate and glutamate on the oxoglutarate carrier investigated in rat heart mitochondria and inverted submitochondrial vesicles.

作者信息

Hautecler J J, Sluse-Goffart C M, Evens A, Duyckaerts C, Sluse F E

机构信息

Laboratoire de Bioénergétique, Université de Liège, Belgium.

出版信息

Biochim Biophys Acta. 1994 Apr 28;1185(2):153-9. doi: 10.1016/0005-2728(94)90205-4.

Abstract

Interaction of glutamate and aspartate with the oxoglutarate carrier was investigated in rat heart mitochondria or inverted submitochondrial particles. With mitochondria, glutamate and aspartate had no effect on the initial rate of oxoglutarate or malate uptake. With inverted submitochondrial vesicles, binding experiments indicated that aspartate bound to the oxoglutarate carrier on its matricial face and increased the affinity of the substrate binding site for malate but did not change the affinity for oxoglutarate. Glutamate had no effect on both substrate bindings. The dissociation constants of the binary substrate-carrier complexes on the matricial side were determined (1.28 +/- 0.15 mM for oxoglutarate and 2.22 +/- 0.26 mM for malate). These values, compared with those obtained previously on the cytosolic side of intact mitochondria, confirmed the asymmetry of the carrier in the native membrane (higher affinities on the cytosolic face). It is concluded that (1) aspartate and glutamate are not cytosolic effectors of the oxoglutarate carrier, (2) matricial aspartate is a positive effector of the binding of malate on the matricial side of the oxoglutarate carrier, and (3) such a characteristic may play a role in the regulation of the oxoglutarate carrier. Thus, it may be emphasized that (1) this observation is the first clear evidence of a well-defined 'sophisticated regulation' (allosteric) of a mitochondrial metabolite carrier, and (2) this regulation of the oxoglutarate carrier may have important consequences on the efficiency of reducing equivalent import in the matrix space by the malate-aspartate shuttle.

摘要

在大鼠心脏线粒体或反向亚线粒体颗粒中研究了谷氨酸和天冬氨酸与草酰戊二酸载体的相互作用。对于线粒体,谷氨酸和天冬氨酸对草酰戊二酸或苹果酸的初始摄取速率没有影响。对于反向亚线粒体囊泡,结合实验表明天冬氨酸在其基质面与草酰戊二酸载体结合,并增加了底物结合位点对苹果酸的亲和力,但未改变对草酰戊二酸的亲和力。谷氨酸对两种底物结合均无影响。测定了基质侧二元底物 - 载体复合物的解离常数(草酰戊二酸为1.28±0.15 mM,苹果酸为2.22±0.26 mM)。将这些值与先前在完整线粒体胞质侧获得的值进行比较,证实了天然膜中载体的不对称性(胞质面亲和力更高)。得出以下结论:(1)谷氨酸和天冬氨酸不是草酰戊二酸载体的胞质效应物;(2)基质天冬氨酸是草酰戊二酸载体基质侧苹果酸结合的正效应物;(3)这种特性可能在草酰戊二酸载体的调节中起作用。因此,可以强调的是:(1)这一观察结果是线粒体代谢物载体明确的“精细调节”(变构)的首个明确证据;(2)草酰戊二酸载体的这种调节可能对苹果酸 - 天冬氨酸穿梭在基质空间中还原当量输入的效率产生重要影响。

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