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Conjugation of phenylalanine hydroxylase with polyubiquitin chains catalysed by rat liver enzymes

机译:大鼠肝酶催化苯丙氨酸羟化酶与多聚泛素链的结合

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摘要

Phenylalanine hydroxylase (PAH, EC 1.14. 16.1) is a highly regulated liver enzyme which catalyses the conversion of L-phenylalanine to L-tyrosine, the rate-limiting step in the catabolic pathway of this amino acid. Among the approx. 400 different mutations of human (h) PAH, frequently associated with the metabolic disease phenylketonuria, a low stability is a characteristic property when expressed in eucaryotic cells. In this study, the pathway of hPAH degradation is addressed with focus on its conjugation with polyubiquitin chains catalysed by the ubiquitin-conjugating enzyme system (E1, E2, E3) isolated from rat liver by covalent affinity chromatography on ubiquitin-Sepharose. In the reconstituted in vitro ubiquitination assay, the enzyme system catalysed both the formation of free polyubiquitin chains and the polyubiquitination of wild-type (wt) hPAH and its 'catalytic domain' (△N102/△C24-hPAH) as visualized by two-dimensional electrophoresis. The ubiquitination of wt-PAH may play a role in the degradation of this liver enzyme notably of its many unstable disease-associated mutant forms. The present approach may also have a more general application in the study of liver proteins as possible targets for ubiquitination.
机译:苯丙氨酸羟化酶(PAH,EC 1.14。16.1)是一种高度调节的肝脏酶,它催化L-苯丙氨酸向L-酪氨酸的转化,这是该氨基酸分解代谢途径中的限速步骤。其中约。人(h)PAH的400种不同突变,通常与代谢性疾病苯丙酮尿症有关,当在真核细胞中表达时,低稳定性是其特征。在这项研究中,hPAH降解的途径着眼于其与多泛素链的缀合,该泛素链是通过在泛素-琼脂糖上的共价亲和色谱法从大鼠肝脏分离的泛素-缀合酶系统(E1,E2,E3)催化的。在重组的体外泛素化测定中,该酶系统既催化了游离多聚泛素链的形成,又催化了野生型(wt)hPAH及其“催化结构域”(△N102 /△C24-hPAH)的多聚泛素化作用,如图2所示。电泳。 wt-PAH的泛素化可能在这种肝酶的降解中发挥作用,尤其是其许多与疾病相关的不稳定突变体形式。本方法在肝蛋白作为泛素化的可能靶标的研究中也可能具有更普遍的应用。

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