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Immune Checkpoint Inhibitors in Tumors Harboring Homologous Recombination Deficiency: Challenges in Attaining Efficacy

Saulo Silva, Carlos W. Wanderley, Leandro M. Colli

2022Frontiers in Immunology17 citationsDOIOpen Access PDF

Abstract

Cancer cells harbor genomic instability due to accumulated DNA damage, one of the cancer hallmarks. At least five major DNA Damage Repair (DDR) pathways are recognized to repair DNA damages during different stages of the cell cycle, comprehending base excision repair (BER), nucleotide excision repair (NER), mismatch repair (MMR), homologous recombination (HR), and non-homologous end joining (NHEJ). The unprecedented benefits achieved with immunological checkpoint inhibitors (ICIs) in tumors with mismatch repair deficiency (dMMR) have prompted efforts to extend this efficacy to tumors with HR deficiency (HRD), which are greatly sensitive to chemotherapy or PARP inhibitors, and also considered highly immunogenic. However, an in-depth understanding of HRD's molecular underpinnings has pointed to essential singularities that might impact ICIs sensitivity. Here we address the main molecular aspects of HRD that underlie a differential profile of efficacy and resistance to the treatment with ICIs compared to other DDR deficiencies.

Topics & Concepts

Homologous recombinationDNA mismatch repairGenome instabilityDNA repairDNA damageCancer researchBase excision repairNucleotide excision repairImmune checkpointCell cycle checkpointBiologyHomologous chromosomeCancerDNAGeneticsCell cycleImmunotherapyGenePARP inhibition in cancer therapyGenetic factors in colorectal cancerDNA Repair Mechanisms