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Linear ubiquitination in NF-kappaB signaling and inflammation: What we do understand and what we do not.

机译:NF-κB信号传导和炎症中的线性泛素化:我们了解的和不了解的。

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摘要

Despite its small size, ubiquitin is one of the most versatile signaling molecules in the cell and affects distinct cellular processes. It forms the building block of a repertoire of posttranslational modifications of cellular proteins, ranging from the attachment of a single ubiquitin to ubiquitin chains of different linkage. Proteins that contain ubiquitin chain-specific ubiquitin-binding domains recognize different types of ubiquitination and determine the mode of signaling of modified proteins. Polyubiquitin chains were thought to be formed only by the conjugation of the ubiquitin C-terminal Gly to one of the seven internal Lys residues of another ubiquitin. However, the C-terminal Gly was recently shown to also link to the N-terminus of another ubiquitin to form head-to-tail polyubiquitin chains, which is referred to as linear ubiquitination. These linear linkages can be assembled and conjugated to another protein by an E3 ligase complex known as LUBAC, and are recognized by a particular ubiquitin-binding domain known as UBAN. Both have been implicated in the regulation of TNF-induced NF-kappaB signaling, which induces the expression of a wide range of proteins that mediate many biological processes including inflammation and cell survival. We discuss the molecular players and mechanisms that determine the specificity and outcome of linear ubiquitination in NF-kappaB signaling, as well as future directions and challenges ahead.
机译:尽管泛素小,但泛素是细胞中功能最广泛的信号分子之一,并影响独特的细胞过程。它构成了细胞蛋白翻译后修饰库的组成部分,范围从单个泛素的附着到具有不同连接的泛素链。包含泛素链特异性泛素结合结构域的蛋白质识别不同类型的泛素化,并确定修饰蛋白质的信号传导方式。认为多聚泛素链仅通过将泛素C末端Gly与另一个泛素的七个内部Lys残基之一缀合而形成。但是,最近显示C末端的Gly也连接到另一个泛素的N末端,形成头对尾的多泛素链,这被称为线性泛素化。这些线性连接可以被称为LUBAC的E3连接酶复合物组装并偶联至另一种蛋白质,并被称为UBAN的特定泛素结合结构域识别。两者都参与了TNF诱导的NF-κB信号传导的调节,该信号传导诱导介导许多生物过程(包括炎症和细胞存活)的多种蛋白质的表达。我们讨论了确定线性泛素化在NF-κB信号传导中的特异性和结果的分子参与者和机制,以及未来的方向和未来的挑战。

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