Despite the fact that in living cells DNA molecules are long and highly crowded, they are rarely knotted. DNA knotting interferes with the normal functioning of the DNA and, therefore, molecular mechanisms evolved that maintain the knotting and catenation level below that which would be achieved if the DNA segments could pass randomly through each other. Biochemical experiments with torsionally relaxed DNA demonstrated earlier that type II DNA topoisomerases that permit inter- and intramolecular passages between segments of DNA molecules use the energy of ATP hydrolysis to select passages that lead to unknotting rather than to the formation of knots. Using numerical simulations, we identify here another mechanism by which topoisomerases can keep the knotting level low. We observe that DNA supercoiling, such as found in bacterial cells, creates a situation where intramolecular passages leading to knotting are opposed by the free-energy change connected to transitions from unknotted to knotted circular DNA molecules.
机构:
College of Physics, Guizhou UniversityCollege of Physics, Guizhou University
Caiyun Xiong
Xiaolin Nie
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机构:
School of Physics and Electronic Science, Guizhou Normal UniversityCollege of Physics, Guizhou University
Xiaolin Nie
Yixue Peng
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机构:
College of Physics, Guizhou UniversityCollege of Physics, Guizhou University
Yixue Peng
Xun Zhou
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机构:
School of Physics and Electronic Science, Guizhou Normal UniversityCollege of Physics, Guizhou University
Xun Zhou
Yangtao Fan
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机构:
Collaborative Innovation Center for Optoelectronic Semiconductors and Efficient Devices, Pen Tung Sah Institute of Micro-Nano Science and Technology, Xiamen UniversityCollege of Physics, Guizhou University
Yangtao Fan
Hu Chen
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机构:
Research Institute for Biomimetics and Soft Matter, Fujian Provincial Key Lab for Soft Functional Materials Research, Department of Physics, Xiamen UniversityCollege of Physics, Guizhou University