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脂联素多聚化依赖于胶原结构域中保守的赖氨酸:翻译后修饰改变对多聚化调控的证据

Adiponectin multimerization is dependent on conserved lysines in the collagenous domain: evidence for regulation of multimerization by alterations in posttranslational modifications.

作者信息

Richards Ayanthi A, Stephens Tim, Charlton Hayley K, Jones Alun, Macdonald Graeme A, Prins Johannes B, Whitehead Jonathan P

机构信息

Centre for Diabetes and Endocrine Research, University of Queensland, Princess Alexandra Hospital, Brisbane, Queensland 4102, Australia.

出版信息

Mol Endocrinol. 2006 Jul;20(7):1673-87. doi: 10.1210/me.2005-0390. Epub 2006 Feb 23.

Abstract

Adiponectin is a secreted, multimeric protein with insulin-sensitizing, antiatherogenic, and antiinflammatory properties. Serum adiponectin consists of trimer, hexamer, and larger high-molecular-weight (HMW) multimers, and these HMW multimers appear to be the more bioactive forms. Multimer composition of adiponectin appears to be regulated; however, the molecular mechanisms involved are unknown. We hypothesize that regulation of adiponectin multimerization and secretion occurs via changes in posttranslational modifications (PTMs). Although a structural role for intertrimer disulfide bonds in the formation of hexamers and HMW multimers is established, the role of other PTMs is unknown. PTMs identified in murine and bovine adiponectin include hydroxylation of multiple conserved proline and lysine residues and glycosylation of hydroxylysines. By mass spectrometry, we confirmed the presence of these PTMs in human adiponectin and identified three additional hydroxylations on Pro71, Pro76, and Pro95. We also investigated the role of the five modified lysines in multimer formation and secretion of recombinant human adiponectin expressed in mammalian cell lines. Mutation of modified lysines in the collagenous domain prevented formation of HMW multimers, whereas a pharmacological inhibitor of prolyl- and lysyl-hydroxylases, 2,2'-dipyridyl, inhibited formation of hexamers and HMW multimers. Bacterially expressed human adiponectin displayed a complete lack of differentially modified isoforms and failed to form bona fide trimers and larger multimers. Finally, glucose-induced increases in HMW multimer production from human adipose explants correlated with changes in the two-dimensional electrophoresis profile of adiponectin isoforms. Collectively, these data suggest that adiponectin multimer composition is affected by changes in PTM in response to physiological factors.

摘要

脂联素是一种具有胰岛素增敏、抗动脉粥样硬化和抗炎特性的分泌型多聚体蛋白。血清脂联素由三聚体、六聚体和更大的高分子量(HMW)多聚体组成,这些HMW多聚体似乎是生物活性更强的形式。脂联素的多聚体组成似乎受到调控;然而,其中涉及的分子机制尚不清楚。我们推测脂联素多聚化和分泌的调控是通过翻译后修饰(PTM)的变化来实现的。尽管三聚体间二硫键在六聚体和HMW多聚体形成中的结构作用已得到证实,但其他PTM的作用尚不清楚。在小鼠和牛脂联素中鉴定出的PTM包括多个保守脯氨酸和赖氨酸残基的羟基化以及羟赖氨酸的糖基化。通过质谱分析,我们证实了这些PTM在人脂联素中的存在,并鉴定出Pro71、Pro76和Pro95上的另外三处羟基化。我们还研究了五个修饰赖氨酸在哺乳动物细胞系中表达的重组人脂联素多聚体形成和分泌中的作用。胶原结构域中修饰赖氨酸的突变阻止了HMW多聚体的形成,而脯氨酰和赖氨酰羟化酶的药理抑制剂2,2'-联吡啶抑制了六聚体和HMW多聚体的形成。细菌表达的人脂联素完全缺乏差异修饰的异构体,无法形成真正的三聚体和更大的多聚体。最后,葡萄糖诱导人脂肪外植体中HMW多聚体产量的增加与脂联素异构体二维电泳图谱的变化相关。总体而言,这些数据表明脂联素多聚体组成受PTM变化的影响,以响应生理因素。

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