| Literature DB >> 33649592 |
Chris J Frangieh1,2, Johannes C Melms3,4, Pratiksha I Thakore1, Kathryn R Geiger-Schuller1,5, Patricia Ho3,4, Adrienne M Luoma6, Brian Cleary1, Livnat Jerby-Arnon1,7,8, Shruti Malu9,10, Michael S Cuoco1, Maryann Zhao1, Casey R Ager3, Meri Rogava3,4, Lila Hovey1, Asaf Rotem9,11,12, Chantale Bernatchez13, Kai W Wucherpfennig6, Bruce E Johnson9,11, Orit Rozenblatt-Rosen1,5, Dirk Schadendorf14, Aviv Regev15,16,17,18, Benjamin Izar19,20,21.
Abstract
Resistance to immune checkpoint inhibitors (ICIs) is a key challenge in cancer therapy. To elucidate underlying mechanisms, we developed Perturb-CITE-sequencing (Perturb-CITE-seq), enabling pooled clustered regularly interspaced short palindromic repeat (CRISPR)-Cas9 perturbations with single-cell transcriptome and protein readouts. In patient-derived melanoma cells and autologous tumor-infiltrating lymphocyte (TIL) co-cultures, we profiled transcriptomes and 20 proteins in ~218,000 cells under ~750 perturbations associated with cancer cell-intrinsic ICI resistance (ICR). We recover known mechanisms of resistance, including defects in the interferon-γ (IFN-γ)-JAK/STAT and antigen-presentation pathways in RNA, protein and perturbation space, and new ones, including loss/downregulation of CD58. Loss of CD58 conferred immune evasion in multiple co-culture models and was downregulated in tumors of melanoma patients with ICR. CD58 protein expression was not induced by IFN-γ signaling, and CD58 loss conferred immune evasion without compromising major histocompatibility complex (MHC) expression, suggesting that it acts orthogonally to known mechanisms of ICR. This work provides a framework for the deciphering of complex mechanisms by large-scale perturbation screens with multimodal, single-cell readouts, and discovers potentially clinically relevant mechanisms of immune evasion.Entities:
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Year: 2021 PMID: 33649592 PMCID: PMC8376399 DOI: 10.1038/s41588-021-00779-1
Source DB: PubMed Journal: Nat Genet ISSN: 1061-4036 Impact factor: 38.330