| Literature DB >> 34562372 |
Julien Champagne1, Abhijeet Pataskar1, Naomi Blommaert1, Remco Nagel1, Demi Wernaart1, Sofia Ramalho1, Juliana Kenski2, Onno B Bleijerveld3, Esther A Zaal4, Celia R Berkers4, Maarten Altelaar5, Daniel S Peeper2, William J Faller1, Reuven Agami6.
Abstract
mRNA translation is a highly conserved and tightly controlled mechanism for protein synthesis. Despite protein quality control mechanisms, amino acid shortage in melanoma induces aberrant proteins by ribosomal frameshifting. The extent and the underlying mechanisms related to this phenomenon are yet unknown. Here, we show that tryptophan depletion-induced ribosomal frameshifting is a widespread phenomenon in cancer. We termed this event sloppiness and strikingly observed its association with MAPK pathway hyperactivation. Sloppiness is stimulated by RAS activation in primary cells, suppressed by pharmacological inhibition of the oncogenic MAPK pathway in sloppy cells, and restored in cells with acquired resistance to MAPK pathway inhibition. Interestingly, sloppiness causes aberrant peptide presentation at the cell surface, allowing recognition and specific killing of drug-resistant cancer cells by T lymphocytes. Thus, while oncogenes empower cancer progression and aggressiveness, they also expose a vulnerability by provoking the production of aberrant peptides through sloppiness.Entities:
Keywords: MAPK pathway; T cell killing; T cell recognition; aberrant peptides; acquired drug resistance; antigen presentation; cancer; protein synthesis; ribosomal frameshifting
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Year: 2021 PMID: 34562372 DOI: 10.1016/j.molcel.2021.09.002
Source DB: PubMed Journal: Mol Cell ISSN: 1097-2765 Impact factor: 17.970