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带电生物聚合物上的蛋白质扩散:DNA 与微管。

Protein Diffusion on Charged Biopolymers: DNA versus Microtubule.

机构信息

Department of Structural Biology, Weizmann Institute of Science, Rehovot, Israel.

Department of Structural Biology, Weizmann Institute of Science, Rehovot, Israel.

出版信息

Biophys J. 2020 Jun 16;118(12):3008-3018. doi: 10.1016/j.bpj.2020.05.004. Epub 2020 May 19.

Abstract

Protein diffusion in lower-dimensional spaces is used for various cellular functions. For example, sliding on DNA is essential for proteins searching for their target sites, and protein diffusion on microtubules is important for proper cell division and neuronal development. On the one hand, these linear diffusion processes are mediated by long-range electrostatic interactions between positively charged proteins and negatively charged biopolymers and have similar characteristic diffusion coefficients. On the other hand, DNA and microtubules have different structural properties. Here, using computational approaches, we studied the mechanism of protein diffusion along DNA and microtubules by exploring the diffusion of both protein types on both biopolymers. We found that DNA-binding and microtubule-binding proteins can diffuse on each other's substrates; however, the adopted diffusion mechanism depends on the molecular properties of the diffusing proteins and the biopolymers. On the protein side, only DNA-binding proteins can perform rotation-coupled diffusion along DNA, with this being due to their higher net charge and its spatial organization at the DNA recognition helix. By contrast, the lower net charge on microtubule-binding proteins enables them to diffuse more quickly than DNA-binding proteins on both biopolymers. On the biopolymer side, microtubules possess intrinsically disordered, negatively charged C-terminal tails that interact with microtubule-binding proteins, thus supporting their diffusion. Thus, although both DNA-binding and microtubule-binding proteins can diffuse on the negatively charged biopolymers, the unique molecular features of the biopolymers and of their natural substrates are essential for function.

摘要

蛋白质在低维空间中的扩散被用于各种细胞功能。例如,在 DNA 上滑动对于蛋白质寻找其靶位点至关重要,而蛋白质在微管上的扩散对于细胞的正常分裂和神经元的发育也很重要。一方面,这些线性扩散过程是由带正电荷的蛋白质与带负电荷的生物聚合物之间的长程静电相互作用介导的,并且具有相似的特征扩散系数。另一方面,DNA 和微管具有不同的结构特性。在这里,我们使用计算方法,通过探索两种蛋白质类型在两种生物聚合物上的扩散,研究了蛋白质沿 DNA 和微管扩散的机制。我们发现,DNA 结合蛋白和微管结合蛋白可以在彼此的基质上扩散;然而,所采用的扩散机制取决于扩散蛋白质和生物聚合物的分子特性。在蛋白质方面,只有 DNA 结合蛋白可以沿 DNA 进行旋转偶联扩散,这是由于它们的净电荷更高,并且其在 DNA 识别螺旋中的空间组织。相比之下,微管结合蛋白的净电荷较低,使其在两种生物聚合物上的扩散速度比 DNA 结合蛋白更快。在生物聚合物方面,微管具有内在无序的带负电荷的 C 末端尾巴,与微管结合蛋白相互作用,从而支持其扩散。因此,尽管 DNA 结合蛋白和微管结合蛋白都可以在带负电荷的生物聚合物上扩散,但生物聚合物及其天然基质的独特分子特征对于功能是必不可少的。

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本文引用的文献

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Tubulin tails and their modifications regulate protein diffusion on microtubules.微管上的微管蛋白尾部及其修饰调节蛋白质扩散。
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Sliding Mechanism at a Coiled-Coil Interface.卷曲螺旋界面的滑动机制。
Biophys J. 2019 Apr 2;116(7):1228-1238. doi: 10.1016/j.bpj.2019.02.026. Epub 2019 Mar 7.
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Near-atomic model of microtubule-tau interactions.微管-tau 相互作用的近原子模型。
Science. 2018 Jun 15;360(6394):1242-1246. doi: 10.1126/science.aat1780. Epub 2018 May 10.

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