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Melting down protein stability: PAPS synthase 2 in patients and in a cellular environment

机译:降低蛋白质稳定性:患者和细胞环境中的PAPS合酶2

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Within the crowded and complex environment of the cell, a protein experiences stabilizing excluded-volume effects and destabilizing quinary interactions with other proteins. Which of these prevail, needs to be determined on a case-by-case basis. PAPS synthases are dimeric and bifunctional enzymes, providing activated sulfate in the form of 3’-phospho-adenosine-5’-phosphosulfate (PAPS) for sulfation reactions. The human PAPS synthases PAPSS1 and PAPSS2 differ significantly in their protein stability as PAPSS2 is a naturally fragile protein. PAPS synthases bind a series of nucleotide ligands and some of them markedly stabilize these proteins. PAPS synthases are of biomedical relevance as destabilizing point mutations give rise to several pathologies. Genetic defects in PAPSS2 have been linked to bone and cartilage malformations as well as a steroid sulfation defect. All this makes PAPS synthases ideal to study protein unfolding, ligand binding and the stabilizing and destabilizing factors in their cellular environment. This review provides an overview on current concepts of protein folding and stability and links this with our current understanding of the different disease mechanisms of PAPSS2-related pathologies with perspectives for future research and application.
机译:在细胞拥挤而复杂的环境中,一种蛋白质会经历稳定的排除体积效应,并破坏与其他蛋白质的五元相互作用。需要根据具体情况确定哪种优先。 PAPS合成酶是二聚体和双功能酶,以3'-磷酸-腺苷-5'-磷酸硫酸盐(PAPS)的形式提供活化的硫酸盐,用于硫酸盐化反应。人PAPS合成酶PAPSS1和PAPSS2的蛋白质稳定性存在显着差异,因为PAPSS2是天然易碎的蛋白质。 PAPS合成酶结合了一系列核苷酸配体,其中一些显着稳定了这些蛋白质。 PAPS合成酶具有生物医学相关性,因为不稳定点突变会引起多种病理。 PAPSS2的遗传缺陷与骨骼和软骨畸形以及类固醇硫酸化缺陷有关。所有这些使PAPS合成酶成为研究蛋白质解折叠,配体结合以及其细胞环境中稳定和不稳定因素的理想选择。这篇综述提供了有关蛋白质折叠和稳定性的当前概念的概述,并将其与我们对PAPSS2相关病理的不同疾病机制的当前理解以及未来的研究和应用前景联系在一起。

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