Modified Dendritic Cell-based T-cell Expansion Protocol and Single-cell Multi-omics Allow for the Selection of the Most Expanded and -effective Clonotype Via Profiling of Thousands of MAGE-A3-specific T-cells

Overview

Journal Front Immunol

Specialty Allergy & Immunology

Date 2024 Oct 25

PMID 39450161

Authors

Sergey Sennikov

Marina Volynets

Saleh Alrhmoun

Roman Perik-Zavodskii

Olga Perik-Zavodskaia

Marina Fisher

Julia Lopatnikova

Julia Shevchenko

Kirill Nazarov

Julia Philippova

Alaa Alsalloum

Vasily Kurilin

Alexander Silkov

Affiliations

Soon will be listed here.

Abstract

Introduction: Adoptive cell therapy using TCR-engineered T-cells is one of the most effective strategies against tumor cells. The TCR T-cell approach has been well tested against a variety of blood neoplasms but is yet to be deeply tested against solid tumors. Among solid tumors, cancer-testis antigens are the most prominent targets for tumor-specific therapy, as they are usually found on cells that lie behind blood-tissue barriers.

Methods: We have employed a novel efficient protocol for MAGE-A3-specific T-cell clonal expansion, performed single-cell multi-omic analysis of the expanded T-cells via BD Rhapsody, engineered a selected T-cell receptor into a lentiviral construct, and tested it in an LDH-cytotoxicity test.

Results And Discussion: We have observed a 191-fold increase in the MAGE-A3-specific T-cell abundance, obtained a dominant T-cell receptor via single-cell multi-omic BD Rhapsody data analysis in the TCRscape bioinformatics tool, and observed potent cytotoxicity of the dominant-clonotype transduced TCR T-cells against a MAGE-A3-positive tumor. We have demonstrated the efficiency of our T-cell enrichment protocol in obtaining potent anti-tumor T-cells and their T-cell receptors, especially when paired with the modern single-cell analysis methods.

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