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活性半胱氨酸的多种功能促进了易于聚集的白细胞介素-31 的独特生物合成过程。

Diverse functions of reactive cysteines facilitate unique biosynthetic processes of aggregate-prone interleukin-31.

机构信息

Department of Protein Science, Amgen Inc, Seattle, WA 98119, USA.

出版信息

Exp Cell Res. 2011 Apr 15;317(7):976-93. doi: 10.1016/j.yexcr.2010.12.012. Epub 2010 Dec 21.

DOI:10.1016/j.yexcr.2010.12.012
PMID:21182835
Abstract

Interleukin-31 (IL-31) is a member of the four helical-bundle gp130/IL-6 cytokine family. Despite its implicated roles in inflammatory diseases, the biosynthetic processes of IL-31 have been poorly investigated. A detailed understanding of IL-31 biosynthesis and the nature of ligand-receptor interactions can provide insights into effective strategies for the design of therapeutic approaches. By using various heterologous protein expression systems, we demonstrated that murine IL-31 was secreted as inter-molecularly disulfide-bonded covalent aggregates. Covalently aggregated IL-31 appeared while trafficking in the secretory pathway, but was not actively retained in the ER. The aggregate formation was not caused by a dysfunctional ER quality control mechanism or an intrinsic limitation in protein folding capacity. Furthermore, secreted IL-31 aggregates were part of a large complex composed of various pleiotropic secretory factors and immune-stimulators. The extent and the heterogeneous nature of aggregates may imply that IL-31 was erroneously folded, but it was capable of signaling through cognate receptors. Mutagenesis revealed the promiscuity of all five cysteines in inter-molecular disulfide formation with components of the hetero-aggregates, but no cysteine was required for IL-31 secretion itself. Our present study not only illustrated various functions that cysteines perform during IL-31 biosynthesis and secretion, but also highlighted their potential roles in cytokine effector functions.

摘要

白细胞介素 31(IL-31)是四螺旋束 gp130/IL-6 细胞因子家族的成员。尽管它在炎症性疾病中具有重要作用,但 IL-31 的生物合成过程尚未得到充分研究。详细了解 IL-31 的生物合成以及配体-受体相互作用的性质,可以为设计治疗方法提供有效的策略。通过使用各种异源蛋白表达系统,我们证明了鼠源 IL-31 是以分子间二硫键共价结合的形式分泌的。在分泌途径中运输时,IL-31 会形成共价聚集物,但不会被 ER 主动保留。聚集物的形成不是由于 ER 质量控制机制功能失调或蛋白质折叠能力的内在限制所致。此外,分泌的 IL-31 聚集物是由各种多效性分泌因子和免疫刺激剂组成的大复合物的一部分。聚集物的程度和异质性可能意味着 IL-31 错误折叠,但它能够通过同源受体发出信号。突变分析揭示了所有五个半胱氨酸在分子间二硫键形成与异质聚集物成分之间的混杂性,但 IL-31 分泌本身不需要半胱氨酸。本研究不仅说明了半胱氨酸在 IL-31 生物合成和分泌过程中的各种功能,还强调了它们在细胞因子效应功能中的潜在作用。

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