Assessment of Phage-Displayed Peptides Targeting Cancer Cell Surface Proteins: A Comprehensive Molecular Docking Study

IF 1.8 4区 生物学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY Journal of Peptide Science Pub Date : 2025-02-04 DOI:10.1002/psc.70004
Verónica Quilumba-Dutan, Clara Carreón-Álvarez, Víctor Sanabria-Ayala, Sergio Hidalgo-Figueroa, Swaroop Chakraborty, Eugenia Valsami-Jones, Rubén López-Revilla, José Luis Rodríguez-López
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Abstract

Peptides binding overexpressed breast and cervical cancer cell surface proteins can be isolated by phage display technology, and their affinity to their potential receptors can be assessed by molecular docking. We isolated 44 phage clones displaying dodecapeptides with high affinity to HeLa cervical cancer and MDA-MB-231 (MDA) breast cancer cells by repeated biopanning of an MK13 phage library and explored their affinity to specific proteins by molecular docking. Six peptides appeared repeatedly during biopanning: two with affinity to HeLa (H5/H21), and four with affinity to MDA cells (M3/M7/M15/M17). Peptide pairs M3/H5 and H1/M17 had affinity to both cell lines. A systematic review identified Annexin A2, EGFR, CD44, CD146, and Integrin alpha V as potential protein targets in HeLa cells, and Vimentin, Galectin-1, and Annexins A1 and A5 in MDA cells. Via virtual screening, we selected six peptides with the highest total docking scores: H1 (−916.32), H6 (−979.21), H19 (−1093.24), M6 (−732.21), M16 (−745.5), and M19 (−739.64), and identified that docking scores were strengthened by the protein type, the interacting amino acid side chains, and the polarity of peptides. This approach facilitates the selection of relevant peptides that could be further explored for active targeting in cancer diagnosis and treatment.

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靶向癌细胞表面蛋白的噬菌体显示肽的评估:一项全面的分子对接研究
通过噬菌体展示技术可以分离出结合过表达乳腺癌和宫颈癌细胞表面蛋白的多肽,并通过分子对接评估其与潜在受体的亲和力。通过对MK13噬菌体文库的重复生物筛选,分离出44个对HeLa宫颈癌和MDA- mb -231 (MDA)乳腺癌细胞具有高亲和力的十二肽噬菌体克隆,并通过分子对接探索其对特定蛋白的亲和力。6个多肽在生物筛选过程中反复出现:2个与HeLa (H5/H21)有亲和力,4个与MDA细胞有亲和力(M3/M7/M15/M17)。肽对M3/H5和H1/M17对两种细胞系均有亲和力。一项系统综述发现,在HeLa细胞中,膜联蛋白A2、EGFR、CD44、CD146和整合素V是潜在的蛋白靶点;在MDA细胞中,Vimentin、半乳糖凝集素1和膜联蛋白A1和A5是潜在的蛋白靶点。通过虚拟筛选,我们选择了总对接分数最高的6个肽段:H1(−916.32)、H6(−979.21)、H19(−1093.24)、M6(−732.21)、M16(−745.5)和M19(−739.64),并发现对接分数与蛋白质类型、相互作用氨基酸侧链和肽极性有关。这种方法有助于选择相关肽,进一步探索在癌症诊断和治疗中的主动靶向。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Journal of Peptide Science
Journal of Peptide Science 生物-分析化学
CiteScore
3.40
自引率
4.80%
发文量
83
审稿时长
1.7 months
期刊介绍: The official Journal of the European Peptide Society EPS The Journal of Peptide Science is a cooperative venture of John Wiley & Sons, Ltd and the European Peptide Society, undertaken for the advancement of international peptide science by the publication of original research results and reviews. The Journal of Peptide Science publishes three types of articles: Research Articles, Rapid Communications and Reviews. The scope of the Journal embraces the whole range of peptide chemistry and biology: the isolation, characterisation, synthesis properties (chemical, physical, conformational, pharmacological, endocrine and immunological) and applications of natural peptides; studies of their analogues, including peptidomimetics; peptide antibiotics and other peptide-derived complex natural products; peptide and peptide-related drug design and development; peptide materials and nanomaterials science; combinatorial peptide research; the chemical synthesis of proteins; and methodological advances in all these areas. The spectrum of interests is well illustrated by the published proceedings of the regular international Symposia of the European, American, Japanese, Australian, Chinese and Indian Peptide Societies.
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