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  2. Identification of nonsense-mediated decay inhibitors that alter the tumor immune landscape

Identification of nonsense-mediated decay inhibitors that alter the tumor immune landscape

  • bioRxiv. 2023 Dec 29:2023.12.28.573594. doi: 10.1101/2023.12.28.573594.
Ashley L Cook Surojit Sur Laura Dobbyn Evangeline Watson Joshua D Cohen Blair Ptak Bum Seok Lee Suman Paul Emily Hsiue Maria Popoli Bert Vogelstein Nickolas Papadopoulos Chetan Bettegowda Kathy Gabrielson Shibin Zhou Kenneth W Kinzler Nicolas Wyhs
Abstract

Despite exciting developments in Cancer Immunotherapy, its broad application is limited by the paucity of targetable antigens on the tumor cell surface. As an intrinsic cellular pathway, nonsense- mediated decay (NMD) conceals neoantigens through the destruction of the RNA products from genes harboring truncating mutations. We developed and conducted a high throughput screen, based on the ratiometric analysis of transcripts, to identify critical mediators of NMD. This screen revealed disruption of kinase SMG1's phosphorylation of UPF1 as a potent disruptor of NMD. This led us to design a novel SMG1 inhibitor, KVS0001, that elevates the expression of transcripts and proteins resulting from truncating mutations in vivo and in vitro . Most importantly, KVS0001 concomitantly increased the presentation of immune-targetable HLA class I-associated Peptides from NMD-downregulated proteins on the surface of Cancer cells. KVS0001 provides new opportunities for studying NMD and the diseases in which NMD plays a role, including Cancer and inherited diseases.

One sentence summary: Disruption of the nonsense-mediated decay pathway with a newly developed SMG1 inhibitor with in-vivo activity increases the expression of T-cell targetable Cancer neoantigens resulting from truncating mutations.

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