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首页> 外文期刊>Journal of Molecular Biology >Allosteric switching by mutually exclusive folding of protein domains.
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Allosteric switching by mutually exclusive folding of protein domains.

机译:通过互斥折叠蛋白质结构域进行变构转换。

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摘要

Many proteins are built from structurally and functionally distinct domains. A major goal is to understand how conformational change transmits information between domains in order to achieve biological activity. A two-domain, bi-functional fusion protein has been designed so that the mechanical stress imposed by the folded structure of one subunit causes the other subunit to unfold, and vice versa. The construct consists of ubiquitin inserted into a surface loop of barnase. The distance between the amino and carboxyl ends of ubiquitin is much greater than the distance between the termini of the barnase loop. This topological constraint causes the two domains to engage in a thermodynamic tug-of-war in which only one can exist in its folded state at any given time. This conformational equilibrium, which is cooperative, reversible, and controllable by ligand binding, serves as a model for the coupled binding and folding mechanism widely used to mediate protein-protein interactions and cellular signaling processes. The position of the equilibrium can be adjusted by temperature or ligand binding and is monitored in vivo by cell death. This design forms the basis for a new class of cytotoxic proteins that can be activated by cell-specific effector molecules, and can thus target particular cell types for destruction.
机译:许多蛋白质是从结构和功能上不同的域构建的。一个主要目标是了解构象变化如何在域之间传递信息以实现生物学活性。已经设计了两个域的双功能融合蛋白,以使一个亚基折叠结构所施加的机械应力导致另一亚基展开,反之亦然。该构建体由遍在barnase表面环中的泛素组成。泛素的氨基末端和羧基末端之间的距离远大于芽孢杆菌蛋白酶环末端之间的距离。这种拓扑约束使两个域参与热力学拔河,在任何时候给定的折叠状态下都只能存在一个。这种构象平衡是可合作的,可逆的并且可通过配体结合控制,是广泛用于介导蛋白质-蛋白质相互作用和细胞信号传导过程的偶联结合和折叠机制的模型。平衡的位置可以通过温度或配体结合进行调节,并通过细胞死亡在体内进行监测。这种设计为一类新型的细胞毒性蛋白奠定了基础,该蛋白可以被细胞特异性效应分子激活,因此可以靶向特定的细胞类型进行破坏。

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