Escape From ALL-CARTaz Leukemia Immunoediting in the Age of Chimeric Antigen Receptors

Zheng Sisi; Asnani Mukta; Thomas-Tikhonenko Andrei

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Escape From ALL-CARTaz Leukemia Immunoediting in the Age of Chimeric Antigen Receptors

机译：逃离嵌合抗原受体时代的全卡其出白血病免疫性

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Chimeric antigen receptor (CAR) T-cell therapy has been transformative for the treatment of B-cell malignancies, with CD19- and CD22-directed CARs being prime examples. However, immunoediting and ensuing antigen loss remain the major obstacles to curative therapy in up to 25% of patients. For example, to achieve the CD19-negative phenotype, malignant cells can pick from a broad array of mechanisms, including focal loss-of-function mutations, dysregulated trafficking to the cell surface, alternative splicing, and lineage switching. In other cases, where resistance is mediated by insufficient antigen density, trogocytosis has been proposed as a possible underlying mechanism. To overcome these barriers, compensatory strategies will be needed, which could include using combinatorial CARs, harnessing epitope spreading, and targeting tumor neoantigens.

机译：嵌合抗原受体（汽车）T细胞疗法已转型性用于治疗B细胞恶性肿瘤，CD19-和CD22针对型汽车是素的实例。然而，免疫和随后的抗原损失仍然是治疗疗法的主要障碍，高达25％的患者。例如，为了实现CD19阴性表型，恶性细胞可以从广泛的机制中挑选，包括功能局灶性突变突变，失去了对细胞表面，替代拼接和谱系切换的局灶性突变。在其他情况下，在抗原密度不足的抗原介导的情况下，已经提出了Trogocytiss作为可能的潜在机制。为了克服这些障碍，需要补偿策略，这可能包括使用组合汽车，利用表位扩散和靶向肿瘤新抗原。

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来源
《The cancer journal》 |2019年第3期|共6页
作者
Zheng Sisi; Asnani Mukta; Thomas-Tikhonenko Andrei;
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作者单位

Univ Penn Perelman Sch Med Childrens Hosp Philadelphia Div Oncol Philadelphia PA 19104 USA;

Univ Penn Perelman Sch Med Childrens Hosp Philadelphia Div Canc Pathobiol Philadelphia PA;

Univ Penn Perelman Sch Med Childrens Hosp Philadelphia Div Oncol Philadelphia PA 19104 USA;

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原文格式 PDF
正文语种 eng
中图分类肿瘤学;
关键词
Adoptive T-cell therapy; alternative splicing; antigen escape; chimeric antigen receptors; epitope loss; immunoediting; immunotherapy; leukemia; lymphoma; therapeutic resistance;

机译：采用T细胞疗法;替代剪接;抗原逃生;嵌合抗原受体;表位损失;免疫疗法;免疫疗法;白血病;淋巴瘤;治疗抵抗;

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专利

1. Escape From ALL-CARTaz Leukemia Immunoediting in the Age of Chimeric Antigen Receptors [J] . Zheng Sisi, Asnani Mukta, Thomas-Tikhonenko Andrei The cancer journal . 2019,第3期

机译：逃离嵌合抗原受体时代的全卡其出白血病免疫性
2. Minimizing leukemia escape: implementing a dual anti-CD20- and CD19-scFv-based chimeric antigen receptor (CAR) [J] . Dina Schneider, Ying Xiong, Andre Roy, Journal for ImmunoTherapy of Cancer . 2015,第S2期

机译：最大限度地减少白血病逃逸：实现基于抗CD20和CD19-scFv的双重嵌合抗原受体（CAR）
3. T Cells Expressing CD19/CD20 Bispecific Chimeric Antigen Receptors Prevent Antigen Escape by Malignant B Cells [J] . Zah Eugenia, Lin Meng-Yin, Silva-Benedict Anne, Cancer immunology research. . 2016,第6期

机译：表达CD19 / CD20双特异性嵌合抗原受体的T细胞阻止恶性B细胞逃逸抗原
4. Chimeric-Antigen-Receptor (CAR) T-Cell Therapy, Can We Leverage the Success? [C] . Aviad Pato, Anat Globersin-Levin, Tamar Shiloach, Protein Engineering Summit. . 2018

机译：嵌合抗原受体（汽车）T细胞治疗，我们可以利用成功吗？
5. 4-1BB Costimulation Ameliorates T Cell Exhaustion Induced by Antigen Independent Signaling of Chimeric Antigen Receptors [D] . Long, Adrienne Hart 2015

机译：4-1BB共刺激可改善嵌合抗原受体的抗原独立信号转导所致的T细胞衰竭。
6. Minimizing leukemia escape: implementing a dual anti-CD20- and CD19-scFv-based chimeric antigen receptor (CAR) [O] . Dina Schneider, Ying Xiong, Andre Roy, 2015

机译：最大限度地减少白血病逃逸：实现基于抗CD20和CD19-scFv的双重嵌合抗原受体（CAR）
7. Minimizing leukemia escape: implementing a dual anti-CD20- and CD19-scFv-based chimeric antigen receptor (CAR) [O] . 2015

机译：最大限度地减少白血病逃逸：实现基于抗CD20和CD19-scFv的双重嵌合抗原受体（CAR）

Escape From ALL-CARTaz Leukemia Immunoediting in the Age of Chimeric Antigen Receptors

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