Bioinformatics evaluation of anticancer properties of GP63 protein-derived peptides on MMP2 protein of melanoma cancer

Q2 Medicine
Fatemeh Sharifi , Iraj Sharifi , Zahra Babaei , Sodabeh Alahdin , Ali Afgar
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引用次数: 0

Abstract

Background

GP63, also known as Leishmanolysin, is a multifunctional virulence factor abundant on the surface of Leishmania spp. small peptides with anticancer capabilities that are selective and toxic to cancer cells are known as anticancer peptides. We aimed to demonstrate the activity of GP63 and its anticancer properties on melanoma using a range of in silico tools and screening methods to identify predicted and designed anticancer peptides.

Methods

Various in silico modeling methodologies are used to establish the three-dimensional (3D) structure of GP63. Refinement and re-evaluation of the modeled structures and the built models' quality evaluated using the different docking used to find the interacting amino acids between MMP2 and GP63 and its anticancer peptides. AntiCP2.0 is used for screening anticancer peptides. 2D interaction plots of protein–ligand complexes evaluated by Protein–Ligand Interaction Profiler server. It is for the first time that used anticancer peptides of GP63 and the predicted and designed peptides.

Results

We used 3 peptides of GP63 based on the AntiCP 2.0 server with scores of 0.63, 0.53, and 0.49, and common peptides of GP63/MMP2 (continues peptide: mean the completely selected peptide after docking with non-anticancer effect, predicted with 0.58 score and designed peptides with 0.47 and 0.45 scores by AntiCP 2.0 server).

Conclusions

The antileishmanial and anticancer peptide research topics exemplify the multidisciplinary nature of peptide research. The advancement of therapeutics targeting cancer and/or Leishmania requires an interconnected research strategy shown in this work.

Abstract Image

Abstract Image

Abstract Image

GP63蛋白衍生肽对黑色素瘤MMP2蛋白抗癌特性的生物信息学评价
dgp63,又称利什曼溶素,是利什曼原虫表面大量存在的一种多功能毒力因子,对癌细胞具有选择性和毒性的小肽被称为抗癌肽。我们的目的是利用一系列的计算机工具和筛选方法来鉴定预测和设计的抗癌肽,证明GP63的活性及其对黑色素瘤的抗癌特性。方法采用多种计算机建模方法建立GP63的三维结构。通过对MMP2与GP63及其抗癌肽之间的相互作用氨基酸的不同对接,对模型结构进行改进和重新评估,并对构建的模型质量进行评估。antip2.0用于筛选抗癌肽。利用protein-ligand interaction Profiler server评估蛋白质-配体复合物的二维相互作用图。这是首次使用GP63的抗癌肽以及预测和设计的肽。结果我们选取了基于antip 2.0服务器的GP63的3个多肽,评分分别为0.63、0.53和0.49,以及GP63/MMP2的常用多肽(连续多肽:指对接后完全选择的无抗癌作用的多肽,预测评分为0.58分,设计肽评分为0.47和0.45分)。结论抗利什曼原虫和抗癌肽的研究主题体现了肽研究的多学科性质。针对癌症和/或利什曼原虫的治疗方法的进步需要一种相互关联的研究策略。
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来源期刊
Journal of Pathology Informatics
Journal of Pathology Informatics Medicine-Pathology and Forensic Medicine
CiteScore
3.70
自引率
0.00%
发文量
2
审稿时长
18 weeks
期刊介绍: The Journal of Pathology Informatics (JPI) is an open access peer-reviewed journal dedicated to the advancement of pathology informatics. This is the official journal of the Association for Pathology Informatics (API). The journal aims to publish broadly about pathology informatics and freely disseminate all articles worldwide. This journal is of interest to pathologists, informaticians, academics, researchers, health IT specialists, information officers, IT staff, vendors, and anyone with an interest in informatics. We encourage submissions from anyone with an interest in the field of pathology informatics. We publish all types of papers related to pathology informatics including original research articles, technical notes, reviews, viewpoints, commentaries, editorials, symposia, meeting abstracts, book reviews, and correspondence to the editors. All submissions are subject to rigorous peer review by the well-regarded editorial board and by expert referees in appropriate specialties.
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