Loss of the intracellular enzyme QPCTL limits chemokine function and reshapes myeloid infiltration to augment tumor immunity.
Rosa Barreira da SilvaRicardo M LeitaoXimo Pechuan-JorgeScott WernekeJason OehVincent JavinalYingyun WangWilson PhungChristine EverettJim NonomiyaDavid ArnottCheng LuYi-Chun HsiaoJames T KoerberIsidro HötzelJames ZiaiZora ModrusanThomas H PillowMerone Roose-GirmaJill M SchartnerMark MerchantSascha RutzCéline EidenschenkIra MellmanMatthew L AlbertPublished in: Nature immunology (2022)
Tumor-associated macrophages are composed of distinct populations arising from monocytes or tissue macrophages, with a poorly understood link to disease pathogenesis. Here, we demonstrate that mouse monocyte migration was supported by glutaminyl-peptide cyclotransferase-like (QPCTL), an intracellular enzyme that mediates N-terminal modification of several substrates, including the monocyte chemoattractants CCL2 and CCL7, protecting them from proteolytic inactivation. Knockout of Qpctl disrupted monocyte homeostasis, attenuated tumor growth and reshaped myeloid cell infiltration, with loss of monocyte-derived populations with immunosuppressive and pro-angiogenic profiles. Antibody targeting of the receptor CSF1R, which more broadly eliminates tumor-associated macrophages, reversed tumor growth inhibition in Qpctl -/- mice and prevented lymphocyte infiltration. Modulation of QPCTL synergized with anti-PD-L1 to expand CD8 + T cells and limit tumor growth. QPCTL inhibition constitutes an effective approach for myeloid cell-targeted cancer immunotherapy.
Keyphrases
- dendritic cells
- peripheral blood
- immune response
- single cell
- cell therapy
- endothelial cells
- acute myeloid leukemia
- bone marrow
- cancer therapy
- liver injury
- liver fibrosis
- drug induced
- stem cells
- metabolic syndrome
- skeletal muscle
- adipose tissue
- anti inflammatory
- insulin resistance
- functional connectivity
- mesenchymal stem cells
- wild type