Nagesh Narayana, Sharma Varun K, Ganesh Kumar A, Lewis Edwin A
Department of Biophysics, Center for Cellular and Molecular Biology, Hyderabad-500 007, India.
J Nucleic Acids. 2010;2010. doi: 10.4061/2010/146418. Epub 2009 Oct 18.
C-myc and Bcl2 are well characterized oncogenes that are capable of forming G-quadruplex structures. Promoter regions of C-myc and Bcl2 forming G-quadruplex structures are chemically synthesized and G-quadruplex structure is formed in presence of 100 mM potassium ion. Three different porphyrin drugs, namely TMPyP2, TMPyP3, and TMPyP4 are allowed to interact with quadruplex DNA complex and the site and nature of interaction are studied. Drug interactions with quadruplex DNA were carried out in different potassium ionic strengths using fluorescence spectroscopy. It is found that fluorescence hypochromicity decreases with an increase in ionic strength in the case of TMPyP4, TMPyP3, and TMPyP2. Fluorescence titration studies and Job plots indicate that four molecules of TMPyP4, two molecules of TMPyP3 and TMPyP2 are interacting with one molecule of quadruplex DNA.
C-myc和Bcl2是已被充分表征的致癌基因,它们能够形成G-四链体结构。化学合成了C-myc和Bcl2形成G-四链体结构的启动子区域,并在100 mM钾离子存在的情况下形成G-四链体结构。使三种不同的卟啉药物,即TMPyP2、TMPyP3和TMPyP4与四链体DNA复合物相互作用,并研究相互作用的位点和性质。使用荧光光谱法在不同的钾离子强度下进行药物与四链体DNA的相互作用。结果发现,在TMPyP4、TMPyP3和TMPyP2的情况下,荧光减色随着离子强度的增加而降低。荧光滴定研究和乔布图表明,四个TMPyP4分子、两个TMPyP3分子和TMPyP2分子与一个四链体DNA分子相互作用。