Transgenic antigen-specific, HLA-A*02:01-allo-restricted cytotoxic T cells recognize tumor-associated target antigen STEAP1 with high specificity

Schirmer David; Gruenewald Thomas G. P.; Klar Richard; Schmidt Oxana; Wohlleber Dirk; Rubio Rebeca Alba; Uckert Wolfgang; Thiel Uwe; Bohne Felix; Busch Dirk H.; Krackhardt Angela M.; Burdach Stefan; Richter Guenther H. S.

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Transgenic antigen-specific, HLA-A*02:01-allo-restricted cytotoxic T cells recognize tumor-associated target antigen STEAP1 with high specificity

机译：特异性转基因抗原特异性，HLA-A * 02：01- allo限制细胞毒性T细胞具有高特异性的肿瘤相关靶抗原STEAP1

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Pediatric cancers, including Ewing sarcoma (ES), are only weakly immunogenic and the tumor-patients' immune system often is devoid of effector T cells for tumor elimination. Based on expression profiling technology, targetable tumor-associated antigens (TAA) are identified and exploited for engineered T-cell therapy. Here, the specific recognition and lytic potential of transgenic allo-restricted CD8(+) T cells, directed against the ES-associated antigen 6-transmembrane epithelial antigen of the prostate 1 (STEAP1), was examined. Following repetitive STEAP1(130) peptide-driven stimulations with HLA-A*02:01(+) dendritic cells (DC), allo-restricted HLA-A*02:01(-)CD8(+) T cells were sorted with HLA-A*02:01/peptide multimers and expanded by limiting dilution. After functional analysis of suitable T cell clones via ELISpot, flow cytometry and xCELLigence assay, T cell receptors' (TCR) alpha- and beta-chains were identified, cloned into retroviral vectors, codon optimized, transfected into HLA-A*02:01(-) primary T cell populations and tested again for specificity and lytic capacity in vitro and in a Rag2(-/-) gamma c(-/-) mouse model. Initially generated transgenic T cells specifically recognized STEAP1(130)-pulsed or transfected cells in the context of HLA-A*02:01 with minimal cross-reactivity as determined by specific interferon-g (IFN gamma) release, lysed cells and inhibited growth of HLA-A*02:01(+) ES lines more effectively than HLA-A*02:01(-) ES lines. In vivo tumor growth was inhibited more effectively with transgenic STEAP1(130)-specific T cells than with unspecific T cells. Our results identify TCRs capable of recognizing and inhibiting growth of STEAP1-expressing HLA-A*02:01(+) ES cells in vitro and in vivo in a highly restricted manner. As STEAP1 is overexpressed in a wide variety of cancers, we anticipate these STEAP1-specific TCRs to be potentially useful for immunotherapy of other STEAP1-expressing tumors.

机译：儿科癌症，包括EWING SARCOMA（ES），只是弱免疫原性，并且肿瘤患者的免疫系统通常没有效应T细胞用于肿瘤消除。基于表达分析技术，鉴定和利用可靶向肿瘤相关的抗原（TAA）以进行工程化T细胞疗法。这里，研究了针对前列腺1（STEAP1）的ES相关抗原6-跨膜上皮抗原的转基因血管限制CD8（+）T细胞的特异性识别和裂解电位。在重复的STEAP1（130）与HLA-A * 02：01（+）树枝状细胞（DC），丙倍注的HLA-A * 02：01（ - ）CD8（+）T细胞与HLA分类的肽驱动的刺激-A * 02：01 /肽多方数，通过限制稀释来扩展。通过ELISPOT的合适T细胞克隆功能分析，鉴定流式细胞术和Xcelligence测定，鉴定T细胞受体'（TCR）（TCR）α-和β链，克隆到逆转录病毒载体，密码子优化，转染到HLA-A * 02：01中（ - ）初级T细胞群体再次在体外和RAG2（ - / - ）γc（ - / - ）小鼠模型中进行特异性和裂解能力。最初产生的转基因T细胞在HLA-A * 02：01的上下文中特别识别出STEAP1（130）的胶乳或转染的细胞，其通过特异性干扰素-G（IFNγ）释放，裂解细胞和抑制生长而确定的最小交叉反应性HLA-A * 02：01（+）ES系列比HLA-A * 02：01（ - ）ES线更有效。在Vivo肿瘤中，使用转基因STEAP1（130）特异性T细胞更有效地抑制了比未特异性T细胞更有效的生长。我们的结果鉴定了能够以高度限制的方式在体外和体内识别和抑制STEAP1的HLA-A * 02：01（+）ES细胞的增长的TCR。由于STEAP1在各种癌症中过表达，我们预计这些STEAP1特异性TCR可能对其他STEAP1表达肿瘤的免疫疗法有用。

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来源
《Oncoimmunology.》 |2016年第6期|共11页
作者
Schirmer David; Gruenewald Thomas G. P.; Klar Richard; Schmidt Oxana; Wohlleber Dirk; Rubio Rebeca Alba; Uckert Wolfgang; Thiel Uwe; Bohne Felix; Busch Dirk H.; Krackhardt Angela M.; Burdach Stefan; Richter Guenther H. S.;
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作者单位

Tech Univ Munich Klinikum Rechts Isar Childrens Canc Res Ctr Munich Germany;

Ludwig Maximilians Univ Munchen Inst Pathol Lab Pediat Sarcoma Biol Munich Germany;

Dept Med 3 Hematol &

Oncol Munich Germany;

Tech Univ Munich Klinikum Rechts Isar Childrens Canc Res Ctr Munich Germany;

Tech Univ Munich Klinikum Rechts Isar Inst Mol Immunol Expt Oncol Munich Germany;

Ludwig Maximilians Univ Munchen Inst Pathol Lab Pediat Sarcoma Biol Munich Germany;

Max Delbruck Ctr Mol Med Berlin Germany;

Tech Univ Munich Klinikum Rechts Isar Childrens Canc Res Ctr Munich Germany;

Tech Univ Munich Helmholtz Zentrum Munchen Inst Virol Munich Germany;

Tech Univ Munich Inst Med Microbiol Immunol &

Hyg Munich Germany;

Dept Med 3 Hematol &

Oncol Munich Germany;

Tech Univ Munich Klinikum Rechts Isar Childrens Canc Res Ctr Munich Germany;

Tech Univ Munich Klinikum Rechts Isar Childrens Canc Res Ctr Munich Germany;

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原文格式 PDF
正文语种 eng
中图分类肿瘤学;
关键词
Allo-restricted T cells; Ewing sarcoma; STEAP1; TCR-transgenic T cells;

机译：allo-trusted t细胞;ewing sarcoma;steap1;tcr-转基因t细胞;

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专利

1. Transgenic antigen-specific, HLA-A*02:01-allo-restricted cytotoxic T cells recognize tumor-associated target antigen STEAP1 with high specificity [J] . Schirmer David, Gruenewald Thomas G. P., Klar Richard, Oncoimmunology. . 2016,第6期

机译：特异性转基因抗原特异性，HLA-A * 02：01- allo限制细胞毒性T细胞具有高特异性的肿瘤相关靶抗原STEAP1
2. Transgenic antigen-specific, HLA-A*02:01-allo-restricted cytotoxic T cells recognize and kill tumor associated antigen STEAP1+tumour cells in vivo [J] . Schirmer D., Grunewald T., Klar R., European journal of cancer: official journal for European Organization for Research and Treatment of Cancer (EORTC) [and] European Association for Cancer Research (EACR) . 2016,第Null期

机译：转基因抗原特异性HLA-A * 02：01-allo限制性细胞毒性T细胞在体内识别并杀死肿瘤相关抗原STEAP1 +肿瘤细胞
3. Transgenic antigen-specific, HLA-A*02:01-allo-restricted cytotoxic T cells recognize and kill tumor associated antigen STEAP1+tumour cells in vivo [J] . Schirmer D., Grunewald T., Klar R., European journal of cancer: official journal for European Organization for Research and Treatment of Cancer (EORTC) [and] European Association for Cancer Research (EACR) . 2016,第Null期

机译：特异性转基因抗原特异性，HLA-A * 02：01-Allo-Impreted细胞毒性T细胞识别和杀死体内肿瘤相关抗原STEAP1 +肿瘤细胞
4. INDUCTION OF ANTIGEN-SPECIFIC IMMUNE RESPONSES BASED ON CHEMICAL MODIFICATION OF ANTIGEN PROTEINS TARGETING TO ANTIGEN PRESENTATING CELLS [C] . Yasuomi Yamasaki, Tomoko Ikenaga, Yoshinobu Takakura Proceedings of the 29th Annual Meeting of the Controlled Release Society . 2002

机译：基于针对抗原预增敏细胞的抗原蛋白的化学修饰，诱导抗原特异性免疫反应
5. Quantifying biomass changes of single cells during antigen-specific CD8+ T cell mediated cytotoxicity. [D] . Burnes, Daina Laura. 2012

机译：量化抗原特异性CD8 + T细胞介导的细胞毒性过程中单细胞的生物量变化。
6. Transgenic antigen-specific HLA-A*02:01-allo-restricted cytotoxic T cells recognize tumor-associated target antigen STEAP1 with high specificity [O] . David Schirmer, Thomas G. P. Grünewald, Richard Klar, 2016

机译：转基因抗原特异性HLA-A * 02：01-allo限制性细胞毒性T细胞以高特异性识别与肿瘤相关的靶抗原STEAP1
7. Establishment of a stable T lymphoma cell line transduced with HLA-A^^lowast;24:02-restricted WT1-specific TCR genes and its application to antigen-specific immunomonitoring [O] . Kazue Watanabe, Shingo Toji, Junya Ohtake, 2013

机译：建立稳定的T淋巴瘤细胞系与HLA-A ^ ^ ^λ^λ2：02限制的WT1特异性TCR基因及其在抗原特异性免疫监测中的应用

Transgenic antigen-specific, HLA-A*02:01-allo-restricted cytotoxic T cells recognize tumor-associated target antigen STEAP1 with high specificity

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