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人类微管相关蛋白tau调节微管中原纤维的数量:一项同步加速器X射线散射研究。

Human microtubule-associated-protein tau regulates the number of protofilaments in microtubules: a synchrotron x-ray scattering study.

作者信息

Choi M C, Raviv U, Miller H P, Gaylord M R, Kiris E, Ventimiglia D, Needleman D J, Kim M W, Wilson L, Feinstein S C, Safinya C R

机构信息

Materials Department, University of California, Santa Barbara, California 93106, USA.

出版信息

Biophys J. 2009 Jul 22;97(2):519-27. doi: 10.1016/j.bpj.2009.04.047.

Abstract

Microtubules (MTs), a major component of the eukaryotic cytoskeleton, are 25 nm protein nanotubes with walls comprised of assembled protofilaments built from alphabeta heterodimeric tubulin. In neural cells, different isoforms of the microtubule-associated-protein (MAP) tau regulate tubulin assembly and MT stability. Using synchrotron small angle x-ray scattering (SAXS), we have examined the effects of all six naturally occurring central nervous system tau isoforms on the assembly structure of taxol-stabilized MTs. Most notably, we found that tau regulates the distribution of protofilament numbers in MTs as reflected in the observed increase in the average radius R(MT) of MTs with increasing Phi, the tau/tubulin-dimer molar ratio. Within experimental scatter, the change in R(MT) seems to be isoform independent. Significantly, R(MT) was observed to rapidly increase for 0 < Phi < 0.2 and saturate for Phi between 0.2-0.5. Thus, a local shape distortion of the tubulin dimer on tau binding, at coverages much less than a monolayer, is spread collectively over many dimers on the scale of protofilaments. This implies that tau regulates the shape of protofilaments and thus the spontaneous curvature C(o)(MT) of MTs leading to changes in the curvature C(MT) (=1/R(MT)). An important biological implication of these findings is a possible allosteric role for tau where the tau-induced shape changes of the MT surface may effect the MT binding activity of other MAPs present in neurons. Furthermore, the results, which provide insight into the regulation of the elastic properties of MTs by tau, may also impact biomaterials applications requiring radial size-controlled nanotubes.

摘要

微管(MTs)是真核细胞骨架的主要组成部分,是直径为25纳米的蛋白质纳米管,其管壁由αβ异二聚体微管蛋白组装而成的原纤维组成。在神经细胞中,微管相关蛋白(MAP)tau的不同亚型调节微管蛋白组装和微管稳定性。利用同步加速器小角X射线散射(SAXS),我们研究了所有六种天然存在的中枢神经系统tau亚型对紫杉醇稳定微管组装结构的影响。最值得注意的是,我们发现tau调节微管中原纤维数量的分布,这反映在随着tau/微管蛋白二聚体摩尔比Phi的增加,微管平均半径R(MT)的增加。在实验误差范围内,R(MT)的变化似乎与亚型无关。值得注意的是,当0 < Phi < 0.2时,R(MT)迅速增加,当Phi在0.2 - 0.5之间时达到饱和。因此,在覆盖率远低于单层的情况下,tau结合时微管蛋白二聚体的局部形状畸变在原纤维尺度上共同扩散到许多二聚体上。这意味着tau调节原纤维的形状,从而调节微管的自发曲率C(o)(MT),导致曲率C(MT)(=1/R(MT))发生变化。这些发现的一个重要生物学意义是tau可能具有变构作用,其中tau诱导的微管表面形状变化可能影响神经元中存在的其他MAP的微管结合活性。此外,这些结果为tau对微管弹性特性的调节提供了见解,也可能影响需要径向尺寸可控纳米管的生物材料应用。

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