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Interactions between CLIP-170 Tubulin and Microtubules: Implications for the Mechanism of CLIP-170 Plus-End Tracking Behavior

机译:CLIP-170微管蛋白和微管之间的相互作用:对CLIP-170 Plus-End追踪行为机制的影响

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摘要

CLIP-170 belongs to a group of proteins (+TIPs) with the enigmatic ability to dynamically track growing microtubule plus-ends. CLIP-170 regulates microtubule dynamics in vivo and has been implicated in cargo-microtubule interactions in vivo and in vitro. Though plus-end tracking likely has intimate connections to +TIP function, little is known about the mechanism(s) by which this dynamic localization is achieved. Using a combination of biochemistry and live cell imaging, we provide evidence that CLIP-170 tracks microtubule plus-ends by a preassociation, copolymerization, and regulated release mechanism. As part of this analysis, we find that CLIP-170 has a stronger affinity for tubulin dimer than for polymer, and that CLIP-170 can distinguish between GTP- and GDP-like polymer. This work extends the previous analysis of CLIP-170 behavior in vivo and complements the existing fluorescence microscope characterization of CLIP-170 interactions with microtubules in vitro. In particular, these data explain observations that CLIP-170 localizes to newly polymerized microtubules in vitro but cannot track microtubule plus-ends in vitro. These observations have implications for the functions of CLIP-170 in regulating microtubule dynamics.
机译:CLIP-170属于一组蛋白质(+ TIP),具有神秘的能力来动态跟踪生长中的微管正末端。 CLIP-170在体内调节微管动力学,并已参与体内和体外的货物-微管相互作用。尽管正负跟踪可能与+ TIP功能有着密切的联系,但对于实现这种动态定位的机制知之甚少。结合使用生物化学和活细胞成像,我们提供的证据表明,CLIP-170通过预缔合,共聚和调节释放机制追踪微管的末端。作为此分析的一部分,我们发现CLIP-170对微管蛋白二聚体的亲和力强于对聚合物的亲和力,并且CLIP-170可以区分GTP和类GDP聚合物。这项工作扩展了先前CLIP-170体内行为的分析,并补充了现有CLIP-170与微管相互作用的荧光显微镜表征。特别地,这些数据解释了CLIP-170在体外定位于新聚合的微管但在体外无法追踪微管正反的观察结果。这些观察结果对CLIP-170在调节微管动力学中的功能具有影响。

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