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目前 SMC 驱动 DNA 环伸出的工作模型。

Current working models of SMC-driven DNA-loop extrusion.

机构信息

Department of Physics and Astronomy, Seoul National University, 1 Gwanak-ro, Gwanak-gu, Seoul 08826, South Korea.

出版信息

Biochem Soc Trans. 2023 Oct 31;51(5):1801-1810. doi: 10.1042/BST20220898.

Abstract

Structural maintenance of chromosome (SMC) proteins play a key roles in the chromosome organization by condensing two meters of DNA into cell-sized structures considered as the SMC protein extrudes DNA loop. Recent sequencing-based high-throughput chromosome conformation capture technique (Hi-C) and single-molecule experiments have provided direct evidence of DNA-loop extrusion. However, the molecular mechanism by which SMCs extrude a DNA loop is still under debate. Here, we review DNA-loop extrusion studies with single-molecule assays and introduce recent structural studies of how the ATP-hydrolysis cycle is coupled to the conformational changes of SMCs for DNA-loop extrusion. In addition, we explain the conservation of the DNA-binding sites that are vital for dynamic DNA-loop extrusion by comparing Cryo-EM structures of SMC complexes. Based on this information, we compare and discuss four compelling working models that explain how the SMC complex extrudes a DNA loop.

摘要

结构维持染色体 (SMC) 蛋白在染色体组织中起着关键作用,通过将两米长的 DNA 浓缩成细胞大小的结构,这些结构被认为是 SMC 蛋白突出的 DNA 环。最近基于测序的高通量染色体构象捕获技术 (Hi-C) 和单分子实验为 DNA 环挤出提供了直接证据。然而,SMC 挤出 DNA 环的分子机制仍存在争议。在这里,我们通过单分子实验综述了 DNA 环挤出的研究,并介绍了最近关于 ATP 水解循环如何与 SMC 的构象变化偶联以进行 DNA 环挤出的结构研究。此外,我们通过比较 SMC 复合物的冷冻电镜结构,解释了对动态 DNA 环挤出至关重要的 DNA 结合位点的保守性。基于这些信息,我们比较和讨论了四个有说服力的工作模型,解释了 SMC 复合物如何挤出 DNA 环。

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