{"title":"Motor domain of condensin and step formation in extruding loop of DNA","authors":"Ya-chang Chou","doi":"10.1007/s10867-024-09661-7","DOIUrl":null,"url":null,"abstract":"<div><p>During the asymmetric loop extrusion of DNA by a condensin complex, one domain of the complex stably anchors to the DNA molecule, and another domain reels in the DNA strand into a loop. The DNA strand in the loop is fully relaxed, or there is no tension in the loop. Just outside of the loop, there is a tension that resists the extrusion of DNA. To maintain the extrusion of the DNA loop, the condensin complex must have a domain capable of generating a force to overcome the tension outside of the loop. This study proposes that the groove-shaped HEAT repeat domain Ycg1 plays the role of a molecular motor. A DNA molecule may bind to the groove electrostatically, and the weak binding force facilitates the random thermal motion of DNA molecules. A mechanical model that random collisions between DNA and the nonparallel inner surfaces of the groove may generate a directional force which is required for the loop extrusion to sustain. The hinge domain binds to the DNA molecule and acts as an anchor during asymmetric DNA loop extrusion. When the effects of ATP hydrolysis and the viscous drag of the fluid environment are considered, the motor–anchor model for the condensin complex and the mechanical model might explain the asymmetric loop extrusion, the formation of steps, the step size distribution in the loop extrusion, the tension-dependent extrusion speed, the interaction between coexisting loops on the DNA strand, and untying the knots during extrusion. This model can also explain the observed formation of the Z-loop.</p></div>","PeriodicalId":612,"journal":{"name":"Journal of Biological Physics","volume":"50 3-4","pages":"307 - 325"},"PeriodicalIF":1.8000,"publicationDate":"2024-07-30","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":null,"platform":"Semanticscholar","paperid":null,"PeriodicalName":"Journal of Biological Physics","FirstCategoryId":"99","ListUrlMain":"https://link.springer.com/article/10.1007/s10867-024-09661-7","RegionNum":4,"RegionCategory":"生物学","ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"","PubModel":"","JCR":"Q3","JCRName":"BIOPHYSICS","Score":null,"Total":0}
引用次数: 0
Abstract
During the asymmetric loop extrusion of DNA by a condensin complex, one domain of the complex stably anchors to the DNA molecule, and another domain reels in the DNA strand into a loop. The DNA strand in the loop is fully relaxed, or there is no tension in the loop. Just outside of the loop, there is a tension that resists the extrusion of DNA. To maintain the extrusion of the DNA loop, the condensin complex must have a domain capable of generating a force to overcome the tension outside of the loop. This study proposes that the groove-shaped HEAT repeat domain Ycg1 plays the role of a molecular motor. A DNA molecule may bind to the groove electrostatically, and the weak binding force facilitates the random thermal motion of DNA molecules. A mechanical model that random collisions between DNA and the nonparallel inner surfaces of the groove may generate a directional force which is required for the loop extrusion to sustain. The hinge domain binds to the DNA molecule and acts as an anchor during asymmetric DNA loop extrusion. When the effects of ATP hydrolysis and the viscous drag of the fluid environment are considered, the motor–anchor model for the condensin complex and the mechanical model might explain the asymmetric loop extrusion, the formation of steps, the step size distribution in the loop extrusion, the tension-dependent extrusion speed, the interaction between coexisting loops on the DNA strand, and untying the knots during extrusion. This model can also explain the observed formation of the Z-loop.
在冷凝蛋白复合物对 DNA 进行不对称环状挤压的过程中,复合物的一个结构域稳定地固定在 DNA 分子上,另一个结构域将 DNA 链卷绕成环。环路中的 DNA 链完全松弛,或者说环路中没有张力。在环的外侧,有一种张力阻止 DNA 的挤出。为了保持 DNA 环的挤出,冷凝蛋白复合物必须有一个能够产生力的结构域,以克服环外的张力。本研究提出,沟槽状的 HEAT 重复结构域 Ycg1 扮演着分子马达的角色。DNA 分子可能与凹槽发生静电结合,微弱的结合力促进了 DNA 分子的随机热运动。一种机械模型认为,DNA 与凹槽非平行内表面之间的随机碰撞可能会产生一种定向力,而这种定向力是环挤压持续进行所必需的。铰链结构域与 DNA 分子结合,在不对称 DNA 环挤压过程中起到锚定作用。如果考虑到 ATP 水解和流体环境粘性阻力的影响,冷凝蛋白复合物的马达-锚模型和机械模型可以解释不对称环挤压、阶梯的形成、环挤压中阶梯大小的分布、与张力相关的挤压速度、DNA 链上共存环之间的相互作用以及挤压过程中的解结。该模型还能解释观察到的 Z 环的形成。
期刊介绍:
Many physicists are turning their attention to domains that were not traditionally part of physics and are applying the sophisticated tools of theoretical, computational and experimental physics to investigate biological processes, systems and materials.
The Journal of Biological Physics provides a medium where this growing community of scientists can publish its results and discuss its aims and methods. It welcomes papers which use the tools of physics in an innovative way to study biological problems, as well as research aimed at providing a better understanding of the physical principles underlying biological processes.