Litcius/Paper detail

Interplay between the DNA Damage Response and Immunotherapy Response in Cancer

Elizabeth Chun Yong Lee, Jessica Sook Ting Kok, Bin Tean Teh, Kah Suan Lim

2022International Journal of Molecular Sciences19 citationsDOIOpen Access PDF

Abstract

Genome instability and immune evasion are both defining hallmarks of cancer. Tumorigenesis is frequently initiated when there is DNA damage to a proto-oncogene or tumor suppressor gene and DNA repair mechanisms are lost or insufficient to correct the damage; immune evasion then prevents the host immune system from recognizing these transformed cells. Therapies targeting genomic instability and immune evasion have been effectively used to treat cancer. Genotoxic therapies such as chemoradiation have been employed in cancer treatments for several decades, while immunotherapy is a relatively new class of cancer therapy that has led to disease regression even in patients with advanced cancer. Several recent studies have shown synergy between both classes of therapy targeting these two defining hallmarks of cancer, and different mechanisms are proposed to be involved. Here, we review the different classes of DNA damage, their links to cancer, and their contribution to immunotherapy responses, as well as the different models that are currently being used to study tumor-immune interactions.

Topics & Concepts

Genome instabilityImmune systemImmunotherapyCancerCarcinogenesisDNA damageCancer immunotherapyEvasion (ethics)Cancer researchBiologyDNA repairImmunologyMedicineDNAGeneticsImmune Cell Function and InteractionImmunotherapy and Immune ResponsesCancer Immunotherapy and Biomarkers