Abstract

SummaryTransmissible cancers are malignant cells that can spread between individuals of a population, akin to both a parasite and a mobile graft. The survival of the Tasmanian devil, the largest remaining marsupial carnivore, is threatened by the remarkable emergence of two independent lineages of transmissible cancer, devil facial tumour (DFT) 1 and devil facial tumour 2 (DFT2). To aid the development of a vaccine and to interrogate how histocompatibility barriers can be overcome, we analysed the peptides bound to major histocompatibility complex class I (MHC‐I) molecules from Tasmanian devil cells and representative cell lines of each transmissible cancer. Here, we show that DFT1 + IFN‐γ and DFT2 cell lines express a restricted repertoire of MHC‐I allotypes compared with fibroblast cells, potentially reducing the breadth of peptide presentation. Comparison of the peptidomes from DFT1 + IFNγ, DFT2 and host fibroblast cells demonstrates a dominant motif, despite differences in MHC‐I allotypes between the cell lines, with preference for a hydrophobic leucine residue at position 3 and position Ω of peptides. DFT1 and DFT2 both present peptides derived from neural proteins, which reflects a shared cellular origin that could be exploited for vaccine design. These results suggest that polymorphisms in MHC‐I molecules between tumours and host can be ‘hidden’ by a common peptide motif, providing the potential for permissive passage of infectious cells and demonstrating complexity in mammalian histocompatibility barriers.

Highlights

  • Transmissible cancers are clonal cell lines that can spread within a population through the passage of live cells between individuals

  • Immunology published by John Wiley & Sons Ltd., Immunology

  • The fibroblast cell line has the greatest diversity of cell surface major histocompatibility complex (MHC)-I molecules with six allotypes in total (SahaI*27/27-1, SahaI*35, SahaI*90, SahaI*49/82, SahaI*32(UD) and SahaI*UK); devil facial tumour 1 (DFT1) + IFN-c cells have the lowest diversity with three (SahaI*35, SahaI*90 and SahaI*32(UD), while devil facial tumour 2 (DFT2) cells have five variants (SahaI*27/27-1, SahaI*74/88, SahaI*35, SahaI*90 and SahaI*32(UD))

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Summary

Introduction

Transmissible cancers are clonal cell lines that can spread within a population through the passage of live cells between individuals. Tasmanian devils are the largest surviving carnivorous marsupials found only on the Australian island of Tasmania, but since the emergence of DFT1,5 their number has declined significantly.[6] The discovery in 2014 of a second independent transmissible cancer, termed DFT2, has the potential to dramatically increase the pressure on Abbreviations: DFT1, devil facial tumour 1; DFT2, devil facial tumour 2; ER, endoplasmic reticulum; IFN-c, interferon-gamma; LC-MS/MS, liquid chromatography–mass spectrometry/mass spectrometry; MHC, major histocompatibility complex; PBR, peptide binding region; PBS, phosphate-buffered saline; RP-HPLC, reversed-phase high-performance liquid chromatography; b2m, b2-microglobulin a 2021 The Authors.

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