Circulating monocytes associated with anti-PD-1 resistance in human biliary cancer induce T cell paralysis

与人类胆道癌抗PD-1耐药相关的循环单核细胞可诱导T细胞麻痹

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作者:Bridget P Keenan ,Elizabeth E McCarthy ,Arielle Ilano ,Hai Yang ,Li Zhang ,Kathryn Allaire ,Zenghua Fan ,Tony Li ,David S Lee ,Yang Sun ,Alexander Cheung ,Diamond Luong ,Hewitt Chang ,Brandon Chen ,Jaqueline Marquez ,Brenna Sheldon ,Robin K Kelley ,Chun Jimmie Ye ,Lawrence Fong

Abstract

Suppressive myeloid cells can contribute to immunotherapy resistance, but their role in response to checkpoint inhibition (CPI) in anti-PD-1 refractory cancers, such as biliary tract cancer (BTC), remains elusive. We use multiplexed single-cell transcriptomic and epitope sequencing to profile greater than 200,000 peripheral blood mononuclear cells from advanced BTC patients (n = 9) and matched healthy donors (n = 8). Following anti-PD-1 treatment, CD14+ monocytes expressing high levels of immunosuppressive cytokines and chemotactic molecules (CD14CTX) increase in the circulation of patients with BTC tumors that are CPI resistant. CD14CTX can directly suppress CD4+ T cells and induce SOCS3 expression in CD4+ T cells, rendering them functionally unresponsive. The CD14CTX gene signature associates with worse survival in patients with BTC as well as in other anti-PD-1 refractory cancers. These results demonstrate that monocytes arising after anti-PD-1 treatment can induce T cell paralysis as a distinct mode of tumor-mediated immunosuppression leading to CPI resistance. Trial registration: ClinicalTrials.gov NCT02703714.

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