溶酶体相关膜糖蛋白1可预测针对肿瘤相关抗原的T细胞受体转基因CD8 + T细胞之间的自相残杀。
Lysosome-associated membrane glycoprotein 1 predicts fratricide amongst T cell receptor transgenic CD8+ T cells directed against tumor-associated antigens.
作者信息
Kirschner Andreas, Thiede Melanie, Blaeschke Franziska, Richter Günther H S, Gerke Julia S, Baldauf Michaela C, Grünewald Thomas G P, Busch Dirk H, Burdach Stefan, Thiel Uwe
机构信息
Laboratory for Functional Genomics and Transplantation Biology, Departments of Pediatrics and Children's Cancer Research Center, Klinikum rechts der Isar, Technische Universität München, Munich, Germany.
Laboratory for Immunotherapy, Dr. von Hauner Children's Hospital, Medical center of the LMU Munich, Munich, Germany.
出版信息
Oncotarget. 2016 Aug 30;7(35):56584-56597. doi: 10.18632/oncotarget.10647.
AIM
Autologous as well as allogeneic CD8+ T cells transduced with tumor antigen specific T cell receptors (TCR) may cause significant tumor lysis upon adoptive transfer. Besides unpredictable life-threatening off-target effects, these TCRs may unexpectedly commit fratricide. We hypothesized lysosome-associated membrane glycoprotein 1 (LAMP1, CD107a) to be a marker for fratricide in TCR transgenic CD8+ T cells.
METHODS
We identified HLA-A02:01/peptide-restricted T cells directed against ADRB3295. After TCR identification, we generated HLA-A02:01/peptide restricted TCR transgenic T cells by retroviral transduction and tested T cell expansion rates as well as A*02:01/peptide recognition and ES killing in ELISpot and xCELLigence assays. Expansion arrest was analyzed via Annexin and CD107a staining. Results were compared to CHM1319-TCR transgenic T cells.
RESULTS
Beta-3-adrenergic receptor (ADRB3) as well as chondromodulin-1 (CHM1) are over-expressed in Ewing Sarcoma (ES) but not on T cells. TCR transgenic T cells demonstrated HLA-A02:01/ADRB3295 mediated ES recognition and killing in ELISpot and xCELLigence assays. 24h after TCR transduction, CD107a expression correlated with low expansion rates due to apoptosis of ADRB3 specific T cells in contrast to CHM1 specific transgenic T cells. Amino-acid exchange scans clearly indicated the cross-reactive potential of HLA-A02:01/ADRB3295- and HLA-A*02:01/CHM1319-TCR transgenic T cells. Comparison of peptide motive binding affinities revealed extended fratricide among ADRB3295 specific TCR transgenic T cells in contrast to CHM1319.
CONCLUSION
Amino-acid exchange scans alone predict TCR cross-reactivity with little specificity and thus require additional assessment of potentially cross-reactive HLA-A*02:01 binding candidates. CD107a positivity is a marker for fratricide of CD8+ TCR transgenic T cells.
目的
用肿瘤抗原特异性T细胞受体(TCR)转导的自体及异体CD8 + T细胞在过继转移后可能会导致显著的肿瘤溶解。除了不可预测的危及生命的脱靶效应外,这些TCR可能会意外地发生自相残杀。我们假设溶酶体相关膜糖蛋白1(LAMP1,CD107a)是TCR转基因CD8 + T细胞中自相残杀的标志物。
方法
我们鉴定了针对ADRB3295的HLA - A02:01/肽限制性T细胞。在鉴定TCR后,我们通过逆转录病毒转导产生了HLA - A02:01/肽限制性TCR转基因T细胞,并在ELISpot和xCELLigence检测中测试了T细胞扩增率以及A*02:01/肽识别和杀伤尤文肉瘤(ES)的能力。通过膜联蛋白和CD107a染色分析扩增停滞情况。将结果与CHM1319 - TCR转基因T细胞进行比较。
结果
β - 3 - 肾上腺素能受体(ADRB3)以及软骨调节素 - 1(CHM1)在尤文肉瘤(ES)中过表达,但在T细胞上不表达。TCR转基因T细胞在ELISpot和xCELLigence检测中表现出HLA - A02:01/ADRB3295介导的ES识别和杀伤能力。与CHM1特异性转基因T细胞相比,TCR转导24小时后,由于ADRB3特异性T细胞凋亡,CD107a表达与低扩增率相关。氨基酸交换扫描清楚地表明了HLA - A02:01/ADRB3295 - 和HLA - A*02:01/CHM1319 - TCR转基因T细胞的交叉反应潜力。肽基序结合亲和力的比较显示,与CHM1319相比,ADRB3295特异性TCR转基因T细胞中存在更广泛的自相残杀现象。
结论
仅氨基酸交换扫描预测TCR交叉反应性的特异性较差,因此需要对潜在的交叉反应性HLA - A*02:01结合候选物进行额外评估。CD107a阳性是CD8 + TCR转基因T细胞自相残杀的标志物。
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