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Molecular comparison of Neanderthal and Modern Human adenylosuccinate lyase

机译:穴居人与现代人腺苷琥珀酸裂合酶的分子比较

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The availability of genomic data from extinct homini such as Neanderthals has caused a revolution in palaeontology allowing the identification of modern human-specific protein substitutions. Currently, little is known as to how these substitutions alter the proteins on a molecular level. Here, we investigate adenylosuccinate lyase, a conserved enzyme involved in purine metabolism for which several substitutions in the modern human protein (hADSL) have been described to affect intelligence and behaviour. During evolution, modern humans acquired a specific substitution (Ala429Val) in ADSL distinguishing it from the ancestral variant present in Neanderthals (nADSL). We show here that despite this conservative substitution being solvent exposed and located distant from the active site, there is a difference in thermal stability, but not enzymology or ligand binding between nADSL and hADSL. Substitutions near residue 429 which do not profoundly affect enzymology were previously reported to cause neurological symptoms in humans. This study also reveals that ADSL undergoes conformational changes during catalysis which, together with the crystal structure of a hitherto undetermined product bound conformation, explains the molecular origin of disease for several modern human ADSL mutants.
机译:来自灭绝的人类(如尼安德特人)的基因组数据的可用性引起了古生物学的一场革命,从而可以鉴定出现代人类特异性蛋白质替代物。目前,关于这些取代如何在分子水平上改变蛋白质的知之甚少。在这里,我们研究腺嘌呤琥珀酸裂合酶,一种参与嘌呤代谢的保守酶,现代人类蛋白质(hADSL)中的几种取代已被描述为影响智力和行为。在进化过程中,现代人类在ADSL中获得了特定的替代(Ala429Val),使其与尼安德特人(nADSL)中存在的祖先变种区分开来。我们在这里表明,尽管这种保守的取代是暴露在溶剂中并且位于远离活性位点的位置,但是在热稳定性方面存在差异,但nADSL和hADSL之间没有酶学或配体结合。先前已经报道了残基429附近的取代基不会对酶学产生深远影响,该取代基在人类中引起神经系统症状。这项研究还表明,ADSL在催化过程中发生构象变化,再加上迄今尚未确定的产物结合构象的晶体结构,解释了几种现代人类ADSL突变体的疾病分子起源。

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