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Immune signatures of checkpoint inhibitor-induced autoimmunity—A focus on neurotoxicity

医学 免疫系统 免疫学 细胞毒性T细胞 CD8型 颗粒酶B 内科学 免疫球蛋白D 肿瘤科 胃肠病学 抗体 B细胞 生物 生物化学 体外
作者
Leonie Müller‐Jensen,Axel Schulz,Henrik E. Mei,Raphael Mohr,Claas Ulrich,Philipp Knape,Nikolaj Frost,Stefan Frischbutter,Désirée Kunkel,Christian Schinke,Lorena Ginesta Roque,Smilla K. Maierhof,Florian T Nickel,Lucie Heinzerling,Matthias Endres,Wolfgang Boehmerle,Petra Huehnchen,Samuel Knauß
出处
期刊:Neuro-oncology [Oxford University Press]
卷期号:26 (2): 279-294 被引量:17
标识
DOI:10.1093/neuonc/noad198
摘要

Abstract Background Neurologic immune-related adverse events (irAE-n) are rare but severe toxicities of immune checkpoint inhibitor (ICI) treatment. To overcome diagnostic and therapeutic challenges, a better mechanistic understanding of irAE-n is paramount. Methods In this observational cohort study, we collected serum and peripheral blood samples from 34 consecutive cancer patients with irAE-n (during acute illness) and 49 cancer control patients without irAE-n (pre- and on-ICI treatment, n = 44 without high-grade irAEs, n = 5 with high-grade nonneurologic irAEs). Patients received either anti-programmed cell death protein (PD)-1 or anti-PD ligand-1 monotherapy or anti-PD-1/anti-cytotoxic T-lymphocyte-associated protein-4 combination therapy. Most common cancers were melanoma, lung cancer, and hepatocellular carcinoma. Peripheral blood immune profiling was performed using 48-marker single-cell mass cytometry and a multiplex cytokine assay. Results During acute illness, patients with irAE-n presented higher frequencies of cluster of differentiation (CD)8+ effector memory type (EM-)1 and central memory (CM) T cells compared to controls without irAEs. Multiorgan immunotoxicities (neurologic + nonneurologic) were associated with higher CD8+ EM1 T cell counts. While there were no B cell changes in the overall cohort, we detected a marked decrease of IgD− CD11c+ CD21low and IgD− CD24+ CD21high B cells in a subgroup of patients with autoantibody-positive irAE-n. We further identified signatures indicative of enhanced chemotaxis and inflammation in irAE-n patients and discovered C-X-C motif chemokine ligand (CXCL)10 as a promising marker to diagnose high-grade immunotoxicities such as irAE-n. Conclusions We demonstrate profound and partly subgroup-specific immune cell dysregulation in irAE-n patients, which may guide future biomarker development and targeted treatment approaches.
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