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Identification of Novel Inhibitors Against HPV16/18-E7 for Cancer Therapy

机译:鉴定抗HPV16 / 18-E7的新型癌症治疗抑制剂

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Cervical cancer contributes most to cancer mortality in women worldwide. Human Papilloma Virus (HPV) is majorly involved in progression of cervical cancer through E7 oncoprotein directed inhibition of Retinoblastoma tumour suppressor protein (pRB). Studies reported E7 proteins of HPV16/18 (HPV16/18-E7) as potential targets for identification of lead compounds. Generally, HPV16/18-E7 participates in the process of cell proliferation and metastasis of cancer, indicates its functional similarity with human cellular kinases. Despite of various efforts, until there is no establish inhibitor reported for HPV16/18-E7 target. Current study examine the inhibition proficiency of well-known kinase inhibitors for the control of HPV16/18-E7 function through molecular modelling, virtual screening. Top six inhibitors for both strains HPV16/18-E7 examined and CID9549298 inhibitor showing highest inhibition efficiency against both strains can be referred as multi-target inhibitor. However, CID5329102, CID5749625, CID6818961 and CID641974 also shows good inhibition efficacy to HPV16-E7 and HPV18-E7. Furthermore, the effects of these inhibitors in various proteins involved in different biological process and metabolic pathways responsible for cell proliferation were explored. We do believe that findings can be further helpful towards inhibition of cervical cancer growth through in-vitro and in-vivo experiments.
机译:宫颈癌是全世界女性癌症死亡率最高的原因。人乳头瘤病毒(HPV)主要通过E7癌蛋白定向抑制视网膜母细胞瘤肿瘤抑制蛋白(pRB)参与宫颈癌的进展。研究报告HPV16 / 18的E7蛋白(HPV16 / 18-E7)作为鉴定先导化合物的潜在靶标。通常,HPV16 / 18-E7参与癌症的细胞增殖和转移过程,表明其与人细胞激酶的功能相似性。尽管进行了各种努力,直到没有针对HPV16 / 18-E7靶标的抑制剂报道。当前的研究通过分子模拟和虚拟筛选研究了著名的激酶抑制剂对HPV16 / 18-E7功能的控制能力。所检测到的两种菌株HPV16 / 18-E7的前六种抑制剂和对两种菌株均显示出最高抑制效率的CID9549298抑制剂可称为多靶标抑制剂。但是,CID5329102,CID5749625,CID6818961和CID641974也显示出对HPV16-E7和HPV18-E7的良好抑制效果。此外,探索了这些抑制剂对参与不同生物过程和负责细胞增殖的代谢途径的各种蛋白质的作用。我们确实相信,这些发现可以通过体外和体内实验进一步抑制宫颈癌的生长。

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