Joseph Sia , Criselle D’Souza , Rebecca Castle , Yu-Kuan Huang , Han Xian Aw Yeang , Rejhan Idrizi , Metta Jana , Shankar Siva , Claire Phillips , Paul Neeson
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引用次数: 0
Abstract
Background
Stereotactic radiosurgery (SRS) is highly effective as focal treatment for brain metastases (BrMs), but whether it can promote anti-tumour immune responses that synergise with immunotherapy remains unclear. We investigated this by examining blood samples from a clinical trial for HER2-amplified breast cancer (HER2-BC) BrMs, matched with longitudinal HER2-BC BrM samples resected from the same location in the same patient.
Methods
Blood samples from 10 patients taken pre- and 7–14 days post-SRS were analysed by mass and flow cytometry. One patient received pre-operative SRS for a BrM that recurred 7 months after resection, followed by planned re-resection 8 days post-SRS. Pre- and post-SRS tumours from this patient were analysed by bulk RNAseq, multiplex immunohistochemistry (mIHC), and TCR sequencing.
Results
Monocytes, central memory CD8+ T and regulatory T cells were enriched in blood post-SRS, together with increased MHC-II expression on monocytes, conventional DCs, and monocytic MDSCs. In tumour, SRS upregulated antigen presentation, T cell proliferation and T cell co-stimulation signatures, alongside an influx of tumour-associated macrophages (TAMs) and CD4+ T cells. Specifically, TAMs and CD4+ T cells, but not CD8+ T cells, demonstrated spatial co-localisation post-SRS. These TAMs were lowly PD-L1 expressing, but CD4+ T cells showed increased PD-1 expression. A sizeable proportion of T cell clonotypes were retained post-SRS, and four clones demonstrated significant, non-stochastic expansion.
Conclusion
Systemic and local immunological changes in this homogenous patient cohort suggest that SRS may facilitate MHC-II-restricted T cell priming responses involving the monocyte-macrophage lineage and CD4+ T cells, which should be further explored.
背景立体定向放射手术(SRS)作为脑转移瘤(BrMs)的病灶治疗非常有效,但它是否能促进与免疫疗法协同作用的抗肿瘤免疫反应仍不清楚。我们通过研究来自HER2-扩增乳腺癌(HER2-BC)脑转移灶临床试验的血液样本,以及从同一患者同一部位切除的纵向HER2-BC脑转移灶样本,对此进行了调查。方法通过质谱和流式细胞术分析了10名患者在SRS术前和术后7-14天采集的血液样本。其中一名患者在术前接受了SRS治疗,该肿瘤在切除术后7个月复发,在SRS术后8天按计划进行了再次切除。结果SRS术后血液中的单核细胞、中心记忆CD8+ T细胞和调节性T细胞富集,单核细胞、传统DC和单核MDSCs上的MHC-II表达增加。在肿瘤中,SRS 上调了抗原呈递、T 细胞增殖和 T 细胞协同刺激特征,同时肿瘤相关巨噬细胞(TAMs)和 CD4+ T 细胞也大量涌入。具体来说,TAMs 和 CD4+ T 细胞(而非 CD8+ T 细胞)在 SRS 后表现出空间共定位。这些TAM的PD-L1表达量很低,但CD4+ T细胞的PD-1表达量却很高。结论这组同质患者的系统和局部免疫学变化表明,SRS 可促进涉及单核-巨噬细胞系和 CD4+ T 细胞的 MHC-II 限制性 T 细胞引物反应,这一点应进一步探讨。