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首页> 外文期刊>Advances and Applications in Bioinformatics and Chemistry >Structural and Molecular Docking Analytical Studies of the Predicted Ligand Binding Sites of Cadherin-1 in Cancer Prognostics
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Structural and Molecular Docking Analytical Studies of the Predicted Ligand Binding Sites of Cadherin-1 in Cancer Prognostics

机译:癌症预测中钙粘蛋白-1预测配体结合位点的结构和分子对接分析研究

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Introduction: Several studies have explored the design of antimicrobial peptides (AMPs) for the development of therapeutic and diagnostic molecules for the treatment and identification of pathogenic diseases as well as cancer. Human cadherin-1 protein has been identified to be involved in adhesion-mediated signalling pathways in normal cells and its loss through genetic and epigenetic alterations can result in an enhanced invasion and metastasis of malignancy in tumours. Therefore, the identification of cadherin during treatment of cancer can be used as prognostic biomarker to establish the responsiveness of patients to treatment regimen. Antimicrobial peptides (AMPs) offer several compensatory advantages in biomedical applications and have been used for treatment of diseases, dietary supplements and diagnosis of diseases. The aim of this research work was to use in silico approaches to analyse retrieved human cadherin-1 as prognostic targets in cancer treatments using modelled putative anticancer AMPs. Methods: The structures of the putative AMPs and cadherin-1 were modelled using I-TASSER server and the protein overall quality was validated using PROCHECK. Thereafter, the protein motifs were predicted and the molecular interaction between the putative anticancer AMPs and protein was carried out using PatchDock. Results: The results revealed that all the AMPs were good prognostic molecules for cancer with BOO1 having the highest binding affinity of 15,874. Conclusion: This study revealed that all the generated AMPs have good prognostic value for monitoring the progress of cancer treatment using human cadherin-1 as receptor. This is the first report where AMPs were used in prognostics of cancer using human cadherin-1.
机译:简介:若干研究探索了抗菌肽(AMPS)的设计,用于制定治疗和诊断分子,用于治疗和鉴定病原疾病以及癌症。已鉴定人钙粘蛋白-1蛋白涉及粘附介导的正常细胞的信号传导途径,其通过遗传和表观遗传改变的损失可能导致肿瘤中恶性肿瘤的增强和转移。因此,在治疗癌症期间的钙粘蛋白可用作预后生物标志物,以确定患者治疗方案的反应性。抗微生物肽(AMPS)在生物医学应用中提供了几种补偿性优势,并用于治疗疾病,膳食补充剂和疾病诊断。本研究工作的目的是在硅方法中使用,分析使用模型推定抗癌安培的癌症治疗中的预后靶标的检测到的人钙粘蛋白-1。方法:使用i-Tasser服务器建模推定的安培和钙粘蛋白-1的结构,使用Procheck验证蛋白质的整体质量。此后,预测蛋白质基序并使用泥质块进行推定的抗癌AMPS和蛋白质之间的分子相互作用。结果:结果表明,所有安培都是良好的癌症预后分子,其中BOO1具有最高的结合亲和力为15,874。结论:本研究表明,所有产生的AMP都具有良好的预后价值,用于监测使用人钙粘蛋白-1作为受体的癌症治疗进展。这是第一个使用人钙粘蛋白-1在癌症的预后使用的AMPS的第一个报告。

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