ID2007 In vitro selection of macrocyclic peptides against THG-1 for Esophagus Squamous Cell Carcinomas therapeutic lead compounds

Authors

  • Dung Thi-Phuong Tran Human Biology program, School of Integrative and Global Major and Department of Experimental Pathology, University of Tsukuba

DOI:

https://doi.org/10.15419/bmrat.v4iS.250

Keywords:

cancer, Esophagus, macrocyclic peptide, RaPID system, squamous carcinoma, therapeutic, THG-1, TBLR1

Abstract

Ineffective current treatments for esophagus squamous cell carcinoma (ESCC) is one of the main reasons for its low 5-year survival (20%). Transforming growth factor beta-1 stimulated clone 22 - isoform 4 (Tsc22D4/THG-1) is overexpressed in 92.6% of ESCC specimens while strictly resided in mitotically active basal layer of normal squamous epithelial tissue. Knockout of THG-1 caused reduction in cancer cells growth, invasion and tumorigenesis. Experimentally, protein-protein interactions (PPIs) were identified as THG-1 mechanism to promote cancer progression. Well-known cellular regulators', Keap1, PHD2, TBLR1 and NRBP1, functional interactions are disrupted in the present of THG-1. To develop THG-1 PPIs antagonist, Random non-standard Peptide Integrated Discovery (RaPID) system was employed. In this system, D-stereochemistry, unusual side chains and N- methylation containing macrocyclic peptides was generated and screened against THG-1. High-specificity, flat-surface binding ability, rigidity make those peptides to be more advantageous for PPIs blocking compare to small molecules and antibodies. Herein, I discuss the process to identify potential lead compounds for ESCC therapeutic by blocking THG-1 PPIs.

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Published

2017-09-05

How to Cite

ID2007 In vitro selection of macrocyclic peptides against THG-1 for Esophagus Squamous Cell Carcinomas therapeutic lead compounds. (2017). Biomedical Research and Therapy, 4(S), S40. https://doi.org/10.15419/bmrat.v4iS.250

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