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用于靶向癌细胞侵袭的合理肽设计

Rational peptide design for targeting cancer cell invasion.

作者信息

Gomari Mohammad Mahmoudi, Arab Seyed Shahriar, Balalaie Saeed, Ramezanpour Sorour, Hosseini Arshad, Dokholyan Nikolay V, Tarighi Parastoo

机构信息

Department of Medical Biotechnology, Faculty of Allied Medicine, Iran University of Medical Sciences, Tehran, Iran.

Department of Biophysics, Faculty of Biological Sciences, Tarbiat Modares University, Tehran, Iran.

出版信息

Proteins. 2024 Jan;92(1):76-95. doi: 10.1002/prot.26580. Epub 2023 Aug 30.

Abstract

Cell invasion is an important process in cancer progression and recurrence. Invasion and implantation of cancer cells from their original place to other tissues, by disabling vital organs, challenges the treatment of cancer patients. Given the importance of the matter, many molecular treatments have been developed to inhibit cancer cell invasion. Because of their low production cost and ease of production, peptides are valuable therapeutic molecules for inhibiting cancer cell invasion. In recent years, advances in the field of computational biology have facilitated the design of anti-cancer peptides. In our investigation, using computational biology approaches such as evolutionary analysis, residue scanning, protein-peptide interaction analysis, molecular dynamics, and free energy analysis, our team designed a peptide library with about 100 000 candidates based on A6 (acetyl-KPSSPPEE-amino) sequence which is an anti-invasion peptide. During computational studies, two of the designed peptides that give the highest scores and showed the greatest sequence similarity to A6 were entered into the experimental analysis workflow for further analysis. In experimental analysis steps, the anti-metastatic potency and other therapeutic effects of designed peptides were evaluated using MTT assay, RT-qPCR, zymography analysis, and invasion assay. Our study disclosed that the IK1 (acetyl-RPSFPPEE-amino) peptide, like A6, has great potency to inhibit the invasion of cancer cells.

摘要

细胞侵袭是癌症进展和复发中的一个重要过程。癌细胞从其原发部位侵袭并植入其他组织,通过破坏重要器官,对癌症患者的治疗构成挑战。鉴于此事的重要性,已经开发了许多分子疗法来抑制癌细胞侵袭。由于其生产成本低且易于生产,肽是抑制癌细胞侵袭的有价值的治疗分子。近年来,计算生物学领域的进展促进了抗癌肽的设计。在我们的研究中,我们的团队使用进化分析、残基扫描、蛋白质-肽相互作用分析、分子动力学和自由能分析等计算生物学方法,基于A6(乙酰基-KPSSPPEE-氨基)序列设计了一个包含约100000个候选物的肽库,A6是一种抗侵袭肽。在计算研究过程中,将得分最高且与A6序列相似性最高的两种设计肽纳入实验分析流程进行进一步分析。在实验分析步骤中,使用MTT法、RT-qPCR、酶谱分析和侵袭试验评估设计肽的抗转移效力和其他治疗效果。我们的研究表明,IK1(乙酰基-RPSFPPEE-氨基)肽与A6一样,具有很强的抑制癌细胞侵袭的能力。

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