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Comparative immunologic characterization of autoimmune giant cell myocarditis with ipilimumab

机译:具有IPILIMIMAB的自身免疫巨细胞心肌炎的比较免疫表征

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摘要

Autoimmune myocarditis is a rare but often fatal toxicity of checkpoint inhibitor immunotherapy. To improve the understanding of this complication, we performed immune profiling on post-mortem tissue from a patient with metastatic melanoma who had steroid-responsive hepatitis, steroid-refractory myocarditis, and shrinking lung metastases after ipilimumab treatment. Histological analysis of heart tissue demonstrated findings consistent with giant cell myocarditis (GCM). The immune infiltrate in the heart was largely comprised of CD4C T cells, whereas the liver had very few T cells, and CD8C T cells were predominant in the responding lung metastases. TCR sequencing identified high T cell clonality in the lung metastases. The TCR repertoire showed low clonality in the heart and minimal overlap with the liver (1.2%), but some overlap with lung metastases (9.9%). Transcriptional profiling identified several potential mediators of increased inflammation in the heart. These findings provide new insights into the pathogenesis of autoimmune myocarditis with ipilimumab.
机译:自身免疫性心肌炎是一种罕见但经常致命的检查点抑制剂免疫疗法。为了改善对这种并发症的理解,我们在IPILIMIMAB治疗后,从患有类固醇响应性肝炎,类固醇耐火心肌炎和收缩肺转移的患者的患者对验尸组织进行免疫分析。心脏组织的组织学分析证明了与巨细胞心肌炎(GCM)一致的结果。心脏中的免疫浸润主要由CD4C T细胞组成,而肝脏具有很少的T细胞,并且CD8C T细胞在响应肺转移中占主导地位。 TCR测序鉴定肺转移中的高T细胞克隆性。 TCR Repertoire在心脏中显示出低的克隆性,并且用肝脏(1.2%)最小的重叠,但与肺转移有些重叠(9.9%)。转录分析确定了内心炎症增加的几个潜在介质。这些调查结果为具有IPILIMIMAB的自身免疫心肌炎发病机制提供了新的见解。

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