• 主题
高级搜索  >
历史搜索 清空历史
首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Molecular defects of the glycine 41 variants of alanine glyoxylate aminotransferase associated with primary hyperoxaluria type I
【24h】

Molecular defects of the glycine 41 variants of alanine glyoxylate aminotransferase associated with primary hyperoxaluria type I

机译:与I型原发性高草酸尿症相关的丙氨酸乙醛酸转氨酶的甘氨酸41变体的分子缺陷

获取原文
获取原文并翻译 | 示例
       
页面导航
  • 摘要
  • 著录项
  • 相似文献
  • 相关主题

摘要

G41 is an interfacial residue located within the α-helix 34-42 of alaninelglyoxylate aminotransferase (AGT). Its mutations on the major (AGT-Ma) or the minor (AGT-Mi) allele give rise to the variants G41R-Ma, G41R-Mi, and G41V-Ma causing hyperoxaluria type 1. Impairment of dimerization in these variants has been suggested to be responsible for immunoreactivity deficiency, intraper-oxisomal aggregation, and sensitivity to proteasomal degradation. However, no experimental evidence supports this view. Here we report that G41 mutations, besides increasing the dimer-monomer equilibrium dissociation constant, affect the protein conformation and stability, and perturb its active site. As compared to AGT-Ma or AGT-Mi, G41 variants display different near-UV CD and intrinsic emission fluorescence spectra, larger exposure of hydrophobic surfaces, sensitivity to Met53-Tyr54 peptide bond cleavage by pro-teinase K, decreased thermostability, reduced coenzyme binding affinity, and catalytic efficiency. Additionally, unlike AGT-Ma and AGT-Mi, G41 variants under physiological conditions form insoluble inactive high-order aggregates (~5,000 nm) through intermolecu-lar electrostatic interactions. A comparative molecular dynamics study of the putative structures of AGT-Mi and G41R-Mi predicts that G41 → R mutation causes a partial unwinding of the 34-42 α-helix and a displacement of the first 44 N-terminal residues including the active site loop 24-32. These simulations help us to envisage the possible structural basis of AGT dysfunction associated with G41 mutations. The detailed insight into how G41 mutations act on the structure-function of AGT may contribute to achieve the ultimate goal of correcting the effects of these mutations.
机译:G41是位于丙二醛基乙氧基化物氨基转移酶(AGT)的α-螺旋34-42内的界面残基。其在主要(AGT-Ma)或次要(AGT-Mi)等位基因上的突变会引起变体G41R-Ma,G41R-Mi和G41V-Ma,从而引起1型高草酸尿症。已经提出了这些变体中二聚化的损害。造成免疫反应性不足,过氧化物酶体内部聚集以及对蛋白酶体降解的敏感性。但是,没有实验证据支持这种观点。在这里我们报告说,G41突变除了增加二聚体单体平衡解离常数外,还影响蛋白质的构象和稳定性,并扰乱其活性位点。与AGT-Ma或AGT-Mi相比,G41变体显示出不同的近紫外CD和内在发射荧光光谱,疏水性表面的暴露量更大,蛋白蛋白酶K对Met53-Tyr54肽键裂解的敏感性,热稳定性降低,辅酶降低结合亲和力和催化效率。此外,与AGT-Ma和AGT-Mi不同,在生理条件下,G41变体通过分子间的静电相互作用形成不溶的非活性高阶聚集体(约5,000 nm)。对AGT-Mi和G41R-Mi的假定结构进行的比较分子动力学研究预测,G41→R突变会导致34-42α-螺旋部分解开并导致包括活性位点的前44个N末端残基发生位移循环24-32。这些模拟有助于我们设想与G41突变相关的AGT功能障碍的可能结构基础。对G41突变如何作用于AGT的结构功能的详细了解可能有助于实现纠正这些突变影响的最终目标。

著录项

  • 来源
  • 作者

    Barbara Cellini; Riccardo Montioli; Alessandro Paiardini; Antonio Lorenzetto; Fabio Maset; Tiziana Bellini; Elisa Oppici; Carla Borri Voltattorni;

  • 作者单位

    Dipartimento di Scienze Morfologico-Biomediche, Sezione di Chimica Biologica, Facolta di Medicina e Chirurgia, Universita degli Studi di Verona, Strada Le Grazie, 8, 37134 Verona, Italy;

    rnDipartimento di Scienze Morfologico-Biomediche, Sezione di Chimica Biologica, Facolta di Medicina e Chirurgia, Universita degli Studi di Verona, Strada Le Grazie, 8, 37134 Verona, Italy;

    rnDipartimento di Scienze Biochimiche 'A. Rossi Fanelli' and Centra di Biologia Molecolare del Consiglio Nazionale delle Ricerche, Universita 'La Sapienza', 00185 Rome, Italy;

    rnDipartimento di Scienze Morfologico-Biomediche, Sezione di Chimica Biologica, Facolta di Medicina e Chirurgia, Universita degli Studi di Verona, Strada Le Grazie, 8, 37134 Verona, Italy;

    rnDipartimento di Scienze Farmaceutiche, Universita di Padua, via Marzolo 5, 35131 Padua, Italy;

    Dipartimento di Biochimica e Biologia Molecolare, Universita di Ferrara, via Borsari 46, 44100 Ferrara, Italy;

    rnDipartimento di Scienze Morfologico-Biomediche, Sezione di Chimica Biologica, Facolta di Medicina e Chirurgia, Universita degli Studi di Verona, Strada Le Grazie, 8, 37134 Verona, Italy;

    rnDipartimento di Scienze Morfologico-Biomediche, Sezione di Chimica Biologica, Facolta di Medicina e Chirurgia, Universita degli Studi di Verona, Strada Le Grazie, 8, 37134 Verona, Italy;

  • 收录信息 美国《科学引文索引》(SCI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

    dimer interface; pathogenic variant; protein aggregation; pyridoxal 5'-phosphate;

    机译:二聚体介面;致病变异蛋白质聚集;吡ido醛5'-磷酸;
  • 入库时间 2022-08-18 00:41:17

相似文献

  • 外文文献
  • 中文文献
  • 专利
获取原文

客服邮箱:kefu@zhangqiaokeyan.com

京公网安备:11010802029741号 ICP备案号:京ICP备15016152号-6 六维联合信息科技 (北京) 有限公司©版权所有

  • 客服微信

  • 服务号