Computational study for suppression of CD25/IL-2 interaction

(2021) Computational study for suppression of CD25/IL-2 interaction. Biological Chemistry. pp. 167-178. ISSN 1431-6730

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Abstract

Cancer recurrence presents a huge challenge in cancer patient management. Immune escape is a key mechanism of cancer progression and metastatic dissemination. CD25 is expressed in regulatory T (Treg) cells including tumor-infiltrating Treg cells (TI-Tregs). These cells specially activate and reinforce immune escape mechanism of cancers. The suppression of CD25/IL-2 interaction would be useful against Treg cells activation and ultimately immune escape of cancer. Here, software, web servers and databases were used, at which in silico designed small interfering RNAs (siRNAs), de novo designed peptides and virtual screened small molecules against CD25 were introduced for the prospect of eliminating cancer immune escape and obtaining successful treatment. We obtained siRNAs with low off-target effects. Further, small molecules based on the binding homology search in ligand and receptor similarity were introduced. Finally, the critical amino acids on CD25 were targeted by a de novo designed peptide with disulfide bond. Hence we introduced computational-based antagonists to lay a foundation for further in vitro and in vivo studies.

Item Type: Article
Keywords: CD25 de novo designed peptides in silico Off-target effects siRNAs virtual screened small molecules REGULATORY T-CELLS TUMOR-INFILTRATING LYMPHOCYTES BINDING-HOMOLOGY SEARCH DOCK WEB SERVER PROTEIN DOCKING SMALL MOLECULES LIGAND CARCINOMA INTERLEUKIN-2-RECEPTOR EXPRESSION
Page Range: pp. 167-178
Journal or Publication Title: Biological Chemistry
Journal Index: ISI
Volume: 402
Number: 2
Identification Number: https://doi.org/10.1515/hsz-2020-0326
ISSN: 1431-6730
Depositing User: Zahra Otroj
URI: http://eprints.mui.ac.ir/id/eprint/14214

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