Departament d'Estructura i Constituents de la Matèria, Facultat de Física, Universitat de Barcelona, Avinguda Diagonal 647, E-08028 Barcelona, Spain.
Phys Rev Lett. 2013 Jul 26;111(4):048103. doi: 10.1103/PhysRevLett.111.048103.
KIF1A is a kinesin motor protein that can work processively in a monomeric (single-headed) form by using a noise-driven ratchet mechanism. Here, we show that the combination of a passive diffusive state and finite-time kinetics of adenosine triphosphate hydrolysis provides a powerful mechanism of cooperative force generation, implying for instance that ∼10 monomeric KIF1As can team up to become ∼100 times stronger than a single one. Consequently, we propose that KIF1A could outperform conventional (double-headed) kinesin collectively and thus explain its specificity in axonal trafficking. We elucidate the cooperativity mechanism with a lattice model that includes multiparticle transitions.
KIF1A 是一种驱动蛋白马达蛋白,它可以通过使用噪声驱动的棘轮机制以单体(单头)形式进行连续运动。在这里,我们表明,被动扩散状态和三磷酸腺苷水解的有限时间动力学的组合提供了一种强大的协同力产生机制,例如,大约 10 个单体 KIF1As 可以联合起来,使其强度比单个 KIF1A 强约 100 倍。因此,我们提出 KIF1A 可以集体优于传统(双头)驱动蛋白,从而解释其在轴突运输中的特异性。我们使用包含多粒子跃迁的格点模型阐明了协同作用机制。