A single-molecule platform for investigation of interactions between G-quadruplexes and small-molecule ligands

被引:0
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作者
Deepak Koirala
Soma Dhakal
Beth Ashbridge
Yuta Sannohe
Raphaël Rodriguez
Hiroshi Sugiyama
Shankar Balasubramanian
Hanbin Mao
机构
[1] Kent State University,Department of Chemistry and Biochemistry and School of Biomedical Sciences
[2] The University of Cambridge,Department of Chemistry
[3] Graduate School of Science,Department of Chemistry
[4] Kyoto University,undefined
[5] Kitashirakawa-oiwakecho,undefined
[6] Sakyo-ku,undefined
[7] Institute for Integrated Cell Material Sciences (iCeMS),undefined
[8] Kyoto University,undefined
[9] Yoshida-ushinomiyacho,undefined
[10] Sakyo-ku,undefined
[11] CREST,undefined
[12] Japan Science and Technology Corporation (JST),undefined
[13] Sanbancho,undefined
[14] Chiyoda-ku,undefined
[15] Cancer Research UK,undefined
[16] Cambridge Research Institute,undefined
[17] Li Ka Shing Center,undefined
[18] School of Clinical Medicine,undefined
[19] The University of Cambridge,undefined
来源
Nature Chemistry | 2011年 / 3卷
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摘要
Ligands that stabilize the formation of telomeric DNA G-quadruplexes have potential as cancer treatments, because the G-quadruplex structure cannot be extended by telomerase, an enzyme over-expressed in many cancer cells. Understanding the kinetic, thermodynamic and mechanical properties of small-molecule binding to these structures is therefore important, but classical ensemble assays are unable to measure these simultaneously. Here, we have used a laser tweezers method to investigate such interactions. With a force jump approach, we observe that pyridostatin promotes the folding of telomeric G-quadruplexes. The increased mechanical stability of pyridostatin-bound G-quadruplex permits the determination of a dissociation constant Kd of 490 ± 80 nM. The free-energy change of binding obtained from a Hess-like process provides an identical Kd for pyridostatin and a Kd of 42 ± 3 µM for a weaker ligand RR110. We anticipate that this single-molecule platform can provide detailed insights into the mechanical, kinetic and thermodynamic properties of liganded bio-macromolecules, which have biological relevance.
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页码:782 / 787
页数:5
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