作者
Aurélien Laguerre, Loic Stefan, Manuel Larrouy, David Genest, Jana Novotna, Marc Pirrotta, David Monchaud
发表日期
2014/9/3
期刊
Journal of the American Chemical Society
卷号
136
期号
35
页码范围
12406-12414
出版商
American Chemical Society
简介
Recent and unambiguous evidences of the formation of DNA and RNA G-quadruplexes in cells has provided solid support for these structures to be considered as valuable targets in oncology. Beyond this, they have lent further credence to the anticancer strategies relying on small molecules that selectively target these higher-order DNA/RNA architectures, referred to as G-quadruplex ligands. They have also shed bright light on the necessity of designing multitasking ligands, displaying not only enticing quadruplex interacting properties (affinity, structural selectivity) but also additional features that make them usable for detecting quadruplexes in living cells, notably for determining whether, when, and where these structures fold and unfold during the cell cycle and also for better assessing the consequences of their stabilization by external agents. Herein, we report a brand new design of such multitasking ligands …
引用总数
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学术搜索中的文章
A Laguerre, L Stefan, M Larrouy, D Genest, J Novotna… - Journal of the American Chemical Society, 2014