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Structure-based simulations complemented by conventional all-atom simulations to provide new insights into the folding dynamics of human telomeric G-quadruplex

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ã€Authorã€‘ Yun-Qiang Bian;Feng Song;Zan-Xia Cao;Jia-Feng Yu;Ji-Hua Wang;Shandong Key Laboratory of Biophysics,Institute of Biophysics,Dezhou University;

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ã€æœºæž„ã€‘ Shandong Key Laboratory of Biophysics,Institute of Biophysics,Dezhou Universityï¼›

ã€æ‘˜è¦ã€‘ The hybrid atomistic structure-based model has been validated to be effective in investigation of G-quadruplex folding.In this study, we performed large-scale conventional all-atom simulations to complement the folding mechanism of human telomeric sequence Htel24 revealed by a multi-basin hybrid atomistic structure-based model. Firstly, the real time-scale of folding rate, which cannot be obtained from the structure-based simulations, was estimated directly by constructing a Markov state model. The results show that Htel24 may fold as fast as on the order of milliseconds when only considering the competition between the hybrid-1 and hybrid-2 G-quadruplex conformations. Secondly, in comparison with the results of structure-based simulations, more metastable states were identified to participate in the formation of hybrid-1 and hybrid-2 conformations. These findings suggest that coupling the hybrid atomistic structure-based model and the conventional all-atom model can provide more insights into the folding dynamics of DNA G-quadruplex. As a result, the multiscale computational framework adopted in this study may be useful to study complex processes of biomolecules involving large conformational changes.æ›´å¤š è¿˜åŽŸ

ã€Abstractã€‘ The hybrid atomistic structure-based model has been validated to be effective in investigation of G-quadruplex folding.In this study, we performed large-scale conventional all-atom simulations to complement the folding mechanism of human telomeric sequence Htel24 revealed by a multi-basin hybrid atomistic structure-based model. Firstly, the real time-scale of folding rate, which cannot be obtained from the structure-based simulations, was estimated directly by constructing a Markov state model. The results show that Htel24 may fold as fast as on the order of milliseconds when only considering the competition between the hybrid-1 and hybrid-2 G-quadruplex conformations. Secondly, in comparison with the results of structure-based simulations, more metastable states were identified to participate in the formation of hybrid-1 and hybrid-2 conformations. These findings suggest that coupling the hybrid atomistic structure-based model and the conventional all-atom model can provide more insights into the folding dynamics of DNA G-quadruplex. As a result, the multiscale computational framework adopted in this study may be useful to study complex processes of biomolecules involving large conformational changes.æ›´å¤š è¿˜åŽŸ

ã€å…³é”®è¯ã€‘ molecular dynamics simulationï¼› structure-based modelï¼› all-atom modelï¼› DNA G-quadruplexï¼›
ã€Key wordsã€‘ molecular dynamics simulationï¼› structure-based modelï¼› all-atom modelï¼› DNA G-quadruplexï¼›

ã€åŸºé‡‘ã€‘ Project supported by the National Natural Science Foundation of China (Grant Nos. 11504043, 61671107, 31670727, and 61771093);the Science Foundation of Shandong Province of China (Grant No. ZR2016JL027);the Taishan Young Scholars Program of Shandong Province of China (Grant No. tsqn20161049);the Youth Science and Technology Innovation Plan of Universities in Shandong,China (Grant No. 2019KJE007)

ã€æ–‡çŒ®å‡ºå¤„ã€‘ Chinese Physics B ,ä¸å›½ç‰©ç†B , ç¼–è¾‘éƒ¨é‚®ç®± ,2021å¹´07æœŸ

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