Biglycan As a Potential Regulator of Tumorgenicity and Immunogenicity in K-RAS-transformed Cells

Overview

Journal Oncoimmunology

Specialty Allergy & Immunology

Date 2022 May 9

PMID 35529675

Authors

Karthikeyan Subbarayan

Chiara Massa

Sandra Leisz

Andre Steven

Daniel Bethmann

Katharina Biehl

Claudia Wickenhauser

Barbara Seliger

Affiliations

Soon will be listed here.

Abstract

The extracellular matrix component biglycan (BGN) plays an essential role in various physiological and pathophysiological processes. A deficient BGN expression associated with reduced immunogenicity was found in HER-2/neu-overexpressing cells. To determine whether BGN is suppressed by oncogene-driven regulatory networks, the expression and function of BGN was analyzed in murine and human BGN/BGN K-RAS-transformed model systems as well as in different patients' datasets of colorectal carcinoma (CRC) lesions. K-RAS-mutated CRC tissues expressed low BGN mRNA and protein levels when compared to normal colon epithelial cells, which was associated with a reduced patients' survival. Transfection of BGN in murine and human BGN K-RAS-expressing cells resulted in a reduced growth and migration of BGN vs BGN K-RAS cells. In addition, increased MHC class I surface antigens as a consequence of an enhanced antigen processing machinery component expression was found upon restoration of BGN, which was confirmed by RNA-sequencing of BGN vs. BGN K-RAS models. Furthermore, a reduced tumor formation of BGN versus BGN K-RAS-transformed fibroblasts associated with an enhanced MHC class I expression and an increased frequency of tumor-infiltrating lymphocytes in tumor lesions was found. Our data provide for the first time an inverse link between BGN and K-RAS expression in murine and human K-RAS-overexpressing models and CRC lesions associated with altered growth properties, reduced immunogenicity and worse patients' outcome. Therefore, reversion of BGN might be a novel therapeutic option for K-RAS-associated malignancies.

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