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Molecular Requirements for Peroxisomal Targeting of Alanine-Glyoxylate Aminotransferase as an Essential Determinant in Primary Hyperoxaluria Type 1

机译:丙氨酸-乙醛酸氨基转移酶过氧化物酶体靶向的分子要求作为主要的原发性高草酸尿症类型1的决定因素。

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摘要

Alanine-glyoxylate aminotransferase is a peroxisomal enzyme, of which various missense mutations lead to irreversible kidney damage via primary hyperoxaluria type 1, in part caused by improper peroxisomal targeting. To unravel the molecular mechanism of its recognition by the peroxisomal receptor Pex5p, we have determined the crystal structure of the respective cargo–receptor complex. It shows an extensive protein/protein interface, with contributions from residues of the peroxisomal targeting signal 1 and additional loops of the C-terminal domain of the cargo. Sequence segments that are crucial for receptor recognition and hydrophobic core interactions within alanine-glyoxylate aminotransferase are overlapping, explaining why receptor recognition highly depends on a properly folded protein. We subsequently characterized several enzyme variants in vitro and in vivo and show that even minor protein fold perturbations are sufficient to impair Pex5p receptor recognition. We discuss how the knowledge of the molecular parameters for alanine-glyoxylate aminotransferase required for peroxisomal translocation could become useful for improved hyperoxaluria type 1 treatment.
机译:丙氨酸-乙醛酸氨基转移酶是一种过氧化物酶体酶,其中的各种错义突变都会通过1型原发性高草酸尿症导致不可逆的肾脏损害,部分原因是过氧化物酶体靶向不正确。为了揭示过氧化物酶体受体Pex5p识别其的分子机制,我们确定了各自的货物-受体复合物的晶体结构。它显示了广泛的蛋白质/蛋白质界面,来自过氧化物酶体靶向信号1的残基和货物C末端结构域的其他环。对受体识别和丙氨酸-乙醛酸氨基转移酶内的疏水核心相互作用至关重要的序列段重叠,这解释了为什么受体识别高度依赖正确折叠的蛋白质的原因。随后,我们在体外和体内对几种酶变体进行了表征,并表明即使是很小的蛋白质折叠扰动也足以损害Pex5p受体的识别。我们讨论过氧化物酶体易位所需的丙氨酸-乙醛酸氨基转移酶的分子参数的知识如何对改进的1型高草酸尿症治疗有用。

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