A neutrophil response linked to tumor control in immunotherapy

免疫疗法中与肿瘤控制相关的嗜中性粒细胞反应

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作者:Jeremy Gungabeesoon ,Nicolas A Gort-Freitas ,Máté Kiss ,Evangelia Bolli ,Marius Messemaker ,Marie Siwicki ,Mehdi Hicham ,Ruben Bill ,Peter Koch ,Chiara Cianciaruso ,Florent Duval ,Christina Pfirschke ,Michael Mazzola ,Solange Peters ,Krisztian Homicsko ,Christopher Garris ,Ralph Weissleder ,Allon M Klein ,Mikael J Pittet

Abstract

Neutrophils accumulate in solid tumors, and their abundance correlates with poor prognosis. Neutrophils are not homogeneous, however, and could play different roles in cancer therapy. Here, we investigate the role of neutrophils in immunotherapy, leading to tumor control. We show that successful therapies acutely expanded tumor neutrophil numbers. This expansion could be attributed to a Sellhi state rather than to other neutrophils that accelerate tumor progression. Therapy-elicited neutrophils acquired an interferon gene signature, also seen in human patients, and appeared essential for successful therapy, as loss of the interferon-responsive transcription factor IRF1 in neutrophils led to failure of immunotherapy. The neutrophil response depended on key components of anti-tumor immunity, including BATF3-dependent DCs, IL-12, and IFNγ. In addition, we found that a therapy-elicited systemic neutrophil response positively correlated with disease outcome in lung cancer patients. Thus, we establish a crucial role of a neutrophil state in mediating effective cancer therapy.

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