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Multiple fuzzy interactions in the moonlighting function of thymosin-β4

机译:胸腺素β4的月光功能中的多个模糊相互作用

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摘要

Thymosine β4 (Tß4) is a 43 amino acid long intrinsically disordered protein (IDP), which was initially identified as an actin-binding and sequestering molecule. Later it was described to have multiple other functions, such as regulation of endothelial cell differentiation, blood vessel formation, wound repair, cardiac cell migration, and survival.1 The various functions of Tβ4 are mediated by interactions with distinct and structurally unrelated partners, such as PINCH, ILK, and stabilin-2, besides the originally identified G-actin. Although the cellular readout of these interactions and the formation of these complexes have been thoroughly described, no attempt was made to study these interactions in detail, and to elucidate the thermodynamic, kinetic, and structural underpinning of this range of moonlighting functions. Because Tβ4 is mostly disordered, and its 4 described partners are structurally unrelated (the CTD of stabilin-2 is actually fully disordered), it occurred to us that this system might be ideal to characterize the structural adaptability and ensuing moonlighting functions of IDPs. Unexpectedly, we found that Tβ4 engages in multiple weak, transient, and fuzzy interactions, i.e., it is capable of mediating distinct yet specific interactions without adapting stable folded structures.
机译:胸腺素β4(Tß4)是一个43个氨基酸长的内在无序蛋白(IDP),最初被鉴定为肌动蛋白结合和螯合分子。后来又描述了它具有多种其他功能,例如调节内皮细胞分化,血管形成,伤口修复,心脏细胞迁移和存活。 1 Tβ4的各种功能是通过与除了最初确定的G-肌动蛋白之外,还存在其他与结构无关的伙伴,例如PINCH,ILK和stabilin-2。尽管已经详细描述了这些相互作用的细胞读数和这些复合物的形成,但并未尝试详细研究这些相互作用以及阐明该月光功能范围的热力学,动力学和结构基础。由于Tβ4大部分是无序的,并且它描述的4个伙伴在结构上不相关(stabilin-2的CTD实际上是完全无序的),因此我们发现该系统可能是表征IDPs的结构适应性和随后的月光照功能的理想选择。出乎意料的是,我们发现Tβ4参与了多种弱的,短暂的和模糊的相互作用,即它能够介导截然不同但又特定的相互作用,而无需适应稳定的折叠结构。

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