In Silico Screening and Binding Characterization of Small Molecules toward a G-Quadruplex Structure Formed in the Promoter Region of c-MYC Oncogene

被引:11
作者
Bhat, Jyotsna [1 ]
Mondal, Soma [1 ]
Sengupta, Pallabi [1 ]
Chatterjee, Subhrangsu [1 ]
机构
[1] Bose Inst, Dept Biophys, P-1-12 CIT Scheme VIIM, Kolkata 700054, WB, India
关键词
ESSENTIAL DYNAMICS; CONTINUUM SOLVENT; DOWN-REGULATION; HUMAN TELOMERE; DNA; PROTEIN; CANCER; DERIVATIVES; LIGANDS; ELEMENT;
D O I
10.1021/acsomega.6b00531
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
Overexpression of c-MYC oncogene is associated with cancer pathology. Expression of c-MYC is regulated by the G-quadruplex structure formed in the G-rich segment of nuclease hypersensitive element (NHE III1), that is, "Pu27", which is localized in the promoter region. Ligand-induced stabilization of the Pu27 structure has been identified as a novel target for cancer therapeutics. Here, we have explored the library of synthetic compounds against the predefined binding site of Pu27. Three compounds were selected based on the docking analyses; they were further scrutinized using all atom molecular dynamics simulations in an explicit water model. Simulated trajectories were scrutinized for conformational stability and ligand binding free energy estimation; essential dynamic behavior was determined using principal component analysis. One of the molecules, "TPP (1-(3-(4-(1,2,3-thiadiazol-4-yl) phenoxy)-2-hydroxypropyl)- 4-carbamoylpiperidinium)", with the best results was considered for further evaluation. The theoretical observations are supported well by biophysical analysis using circular dichroism, isothermal titration calorimetry, and high-resolution NMR spectroscopy indicating association of TPP with Pu27. The in vitro studies were then translated into c-MYC overexpression in the T47D breast cancer cell line. Biological evaluation through the MTT assay, flow cytometric assay, RT-PCR, and reporter luciferase assay suggests that TPP downregulates the expression of c-MYC oncogene by arresting its promoter region. In silico and in vitro observations cumulatively suggest that the novel skeleton of TPP could be a potential anticancer agent by stabilizing the G-quadruplex formed in the Pu27 and consequently downregulating the expression of c-MYC oncogene. Derivation of new molecules on its skeleton may confer anticancer therapeutics for the next generation.
引用
收藏
页码:4382 / 4397
页数:16
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