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Tumour neoantigen mimicry by microbial species in cancer immunotherapy

Maximilian Boesch, Florent Baty, Sacha I. Rothschild, Michael Tamm, Markus Joerger, Martin Früh, Martin Brutsche

2021British Journal of Cancer52 citationsDOIOpen Access PDF

Abstract

Tumour neoantigens arising from cancer-specific mutations generate a molecular fingerprint that has a definite specificity for cancer. Although this fingerprint perfectly discriminates cancer from healthy somatic and germline cells, and is therefore therapeutically exploitable using immune checkpoint blockade, gut and extra-gut microbial species can independently produce epitopes that resemble tumour neoantigens as part of their natural gene expression programmes. Such tumour molecular mimicry is likely not only to influence the quality and strength of the body's anti-cancer immune response, but could also explain why certain patients show favourable long-term responses to immune checkpoint blockade while others do not benefit at all from this treatment. This article outlines the requirement for tumour neoantigens in successful cancer immunotherapy and draws attention to the emerging role of microbiome-mediated tumour neoantigen mimicry in determining checkpoint immunotherapy outcome, with far-reaching implications for the future of cancer immunotherapy.

Topics & Concepts

ImmunotherapyCancer immunotherapyCancerImmune checkpointBiologyMolecular mimicryImmunologyImmune systemBlockadeEpitopeMimicryMicrobiomeGermline mutationCancer researchMutationAntigenBioinformaticsGeneticsGeneReceptorEcologyCancer Immunotherapy and BiomarkersImmunotherapy and Immune ResponsesCAR-T cell therapy research
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