P851从血浆外泌体和过继T细胞中鉴定潜在的预测性生物标志物,以区分接受化疗和病毒特异性T细胞治疗的短期和长期转移性鼻咽癌幸存者

T. Shuen, Wang Who-Whong, H. Toh, Janice Lim, Cherlyn Tan, J. Kosasih, R. Cheong
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Methods We isolated exosome from plasma samples by size exclusion chromatography and magnetic-based isolation technology, followed by fluorescence-activated cell sorting (FACS) analysis, Western blot analysis for immune-related checkpoint molecules, or mass spectrometry for exosomal peptide detection. All the generated CTLs were analysed by gene expression microarray as well as a FACS system with the use of T cell-specific 23-antibody panel for comprehensive immunophenotyping. The representative CTL samples were also subject to single-cell (sc) RNA-Seq with DNA barcoded antibodies for comprehensive integrated transcriptomics and immunophenotyping analysis. Results Patients with overall survival longer than 2 years were grouped as long survivors and the remaining patients were grouped as short survivors. Differentially expressed immune-related checkpoint molecules, such as PD1, ICOS, and CD137, were detected in in pre-treatment exosome of long and short survivors. Furthermore, more than 13,000 high confident and unique peptides which belong to 1,500 unique proteins were identified and quantified by mass spectrometry from the purified plasma exosome. Pathway enrichment analysis further showed that plasma exosome of the short survivors had significantly higher innate immune response-activating signal transduction-related peptides detected (p-value = 4.81 x 10-5). The transcriptomic analysis revealed that statistically lower expressions of SELL (CD62L) and LEF1 were found in the EBV CTL of the short survivors, suggesting that the EBV CTL of short survivors were characterized by a lesser central memory T cell phenotype. 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引用次数: 1

摘要

生物标志物的鉴定预测过继性T细胞治疗的更好结果是一个新兴的,仍然是新生的领域。我们之前完成了一项2期临床试验,在吉西他滨+卡铂化疗后,自体过继ebv特异性细胞毒性T淋巴细胞(CTL)免疫治疗作为一线治疗,治疗了35例晚期无法治愈的4c期鼻咽癌(NPC)患者。在这里,我们的目标是1)评估外泌体蛋白对过继T细胞治疗有益的潜在特异性预测性生物标志物,2)研究我们生成的EBV靶向ctl的特定免疫表型是否与生存益处相关。方法采用大小排斥层析和磁分离技术从血浆样品中分离外泌体,然后采用荧光活化细胞分选(FACS)分析、免疫相关检查点分子的Western blot分析或外泌体肽检测的质谱分析。所有生成的ctl通过基因表达微阵列和FACS系统进行分析,并使用T细胞特异性23抗体面板进行综合免疫表型分析。代表性CTL样品也进行单细胞(sc) RNA-Seq与DNA条形码抗体进行综合整合转录组学和免疫表型分析。结果将总生存期大于2年的患者归为长生存者,其余患者归为短生存者。差异表达的免疫相关检查点分子,如PD1, ICOS和CD137,在治疗前的长和短存活者的外泌体中被检测到。此外,通过质谱法从纯化的血浆外泌体中鉴定和定量了属于1500种独特蛋白质的13000多个高自信和独特的肽。途径富集分析进一步表明,短存活者血浆外泌体检测到的先天免疫反应激活信号转导相关肽显著增加(p值= 4.81 x 10-5)。转录组学分析显示,在短存活者的EBV CTL中,SELL (CD62L)和LEF1的表达在统计学上较低,这表明短存活者的EBV CTL具有较低的中枢记忆T细胞表型。我们的数据报告了治疗前特异性血浆外泌体蛋白,以及输注患者之前生成的基线EBV ctl的转录组学特征与患者生存率相关,这表明它们可以一起用作生物标志物来预测接受这种化学免疫治疗联合治疗的晚期鼻咽癌患者的预后。更深入的分析所有ctl的免疫表型和代表性ctl的scRNA-Seq数据将在会议上发表。这项工作得到了新加坡政府资助(国家医学研究委员会(NMRC) -开放基金-大型协作补助金(OF-LCG)和新加坡国家癌症中心整体补助金)以及Tessa Therapeutics有限公司的部分支持。
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P851 Identifying potential predictive biomarkers from plasma exosomes and adoptive T cells that differentiate short and long-term metastatic nasopharyngeal cancer survivors treated with chemotherapy and virus-specific T cells
Background The identification of biomarkers predicting a better outcome to adoptive T cell therapy is an emerging, still nascent field. We previously completed a phase 2 clinical trial of autologous adoptive EBV-specific cytotoxic T lymphocyte (CTL) immunotherapy following gemcitabine + carboplatin chemotherapy as first line treatment in 35 advanced incurable stage 4c nasopharyngeal carcinoma (NPC) patients. Here, we aim 1) to evaluate exosome proteins for potential specific predictive biomarkers of benefit to adoptive T cell therapy and 2) to investigate if a specific immunophenotype of our generated EBV targeting CTLs correlates with survival benefit. Methods We isolated exosome from plasma samples by size exclusion chromatography and magnetic-based isolation technology, followed by fluorescence-activated cell sorting (FACS) analysis, Western blot analysis for immune-related checkpoint molecules, or mass spectrometry for exosomal peptide detection. All the generated CTLs were analysed by gene expression microarray as well as a FACS system with the use of T cell-specific 23-antibody panel for comprehensive immunophenotyping. The representative CTL samples were also subject to single-cell (sc) RNA-Seq with DNA barcoded antibodies for comprehensive integrated transcriptomics and immunophenotyping analysis. Results Patients with overall survival longer than 2 years were grouped as long survivors and the remaining patients were grouped as short survivors. Differentially expressed immune-related checkpoint molecules, such as PD1, ICOS, and CD137, were detected in in pre-treatment exosome of long and short survivors. Furthermore, more than 13,000 high confident and unique peptides which belong to 1,500 unique proteins were identified and quantified by mass spectrometry from the purified plasma exosome. Pathway enrichment analysis further showed that plasma exosome of the short survivors had significantly higher innate immune response-activating signal transduction-related peptides detected (p-value = 4.81 x 10-5). The transcriptomic analysis revealed that statistically lower expressions of SELL (CD62L) and LEF1 were found in the EBV CTL of the short survivors, suggesting that the EBV CTL of short survivors were characterized by a lesser central memory T cell phenotype. Conclusions Our data reports that specific pre-treatment plasma exosome proteins, and separately, transcriptomic profile of the generated baseline EBV CTLs prior to infusion into the patients correlate with patient survival, suggesting that they could be used together as biomarkers to predict outcome in the advanced NPC patients treated with this chemo-immunotherapy combination. More in-depth analysis of the immunophenotyping of all the CTLs and the representative CTLs’ scRNA-Seq data will be presented at the meeting. Acknowledgements This work was supported by Singapore government funding (National Medical Research Council (NMRC) – Open Fund - Large Collaborative Grant (OF-LCG) and National Cancer Centre Singapore Block Grant as well as in part by Tessa Therapeutics Ltd.
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