Wei Li

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Organization: Institute of Physics
Department: Beijing National Laboratory for Condensed Matter Physics and Key Laboratory of Soft Matter Physics
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Co-reporter:Wei Li ; Xi-Miao Hou ; Peng-Ye Wang ; Xu-Guang Xi ;Ming Li
Journal of the American Chemical Society 2013 Volume 135(Issue 17) pp:6423-6426
Publication Date(Web):April 17, 2013
DOI:10.1021/ja4019176
Single-stranded guanine-rich sequences fold into compact G-quadruplexes. Although G-triplexes have been proposed and demonstrated as intermediates in the folding of G-quadruplexes, there is still a debate on their folding pathways. In this work, we employed magnetic tweezers to investigate the folding kinetics of single human telomeric G-quadruplexes in 100 mM Na+ buffer. The results are consistent with a model in which the G-triplex is an in-pathway intermediate in the folding of the G-quadruplex. By finely tuning the force exerted on the G-quadruplex, we observed reversible transitions from the G-quadruplex to the G-triplex as well as from the G-triplex to the unfolded coil when the force was increased from 26 to 39 pN. The energy landscape derived from the probability distribution shows clearly that the G-quadruplex goes through an intermediate when it is unfolded, and vice versa.
Co-reporter:Hai-Peng Ju, Yi-Zhou Wang, Jing You, Xi-Miao Hou, Xu-Guang Xi, Shuo-Xing Dou, Wei Li, and Peng-Ye Wang
ACS Omega Volume 1(Issue 2) pp:244-250
Publication Date(Web):August 24, 2016
DOI:10.1021/acsomega.6b00044
G-Quadruplex DNA structure has been proven to be a binding target for small molecular organic compounds and hence regarded as a promising pharmacological target. Cisplatin is a widely used chemotherapy drug that targets duplex DNA and was recently shown to react also with G-quadruplex, implying that cisplatin actually may also target G-quadruplex. In this work, we employed magnetic tweezers to investigate the influence of cisplatin on the folding kinetics of single human telomeric G-quadruplex. It was revealed that cisplatin and G-quadruplex interact in two different and competitive ways that depend on cisplatin concentration.Topics: Conformation; Magnetic materials; Magnetic materials; Molecular association; Molecular modeling; Nucleic acid structure; Pharmacology;
Phenol,2-[[[2,6-bis(1-methylethyl)phenyl]imino]methyl]-6-(1,1-dimethylethyl)-
Phenol, 2-(1,1-dimethylethyl)-6-(diphenylphosphino)-
Caspase-3
Mitogen-activated protein kinase p38
c-Jun N-terminal kinase
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