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Efficient glycoengineering of GM3 on melanoma cell and monoclonal antibody-mediated selective killing of the glycoengineered cancer cell

机译：GM3在黑素瘤细胞上的高效糖工程化和单克隆抗体介导的糖工程化癌细胞的选择性杀伤

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摘要

To verify the principal of a new immunotherapeutic strategy for cancer, a monoclonal antibody 2H3 against N-phenylacetyl GM3, an unnatural form of the tumor-associated antigen GM3, was prepared and employed to demonstrate that murine melanoma cell B16F0 could be effectively glycoengineered by N-phenylacetyl-d-mannosamine to express N-phenylacetyl GM3 and that 2H3 was highly cytotoxic to the glycoengineered B16F0 cell in the presence of complements. It was further demonstrated that B16F0 cell could be glycoengineered 4-5 times more effectively than 3T3 A31 cell, a normal murine embryo fibroblast cell, and that the antibody and complement mediated cytotoxicity was at least 200 times more potent to the glycoengineered B16F0 cell than to the N-phenylacetyl-d-mannosamine-treated 3T3 A31 cell. These results show the promise for developing useful melanoma immunotherapies based on vaccination against N-phenylacetyl GM3 followed by treatment with N-phenylacetyl-d-mannosamine.

机译：为了验证一种新的癌症免疫治疗策略的原理，制备了一种针对N-苯基乙酰基GM3（一种与肿瘤相关的抗原GM3的非天然形式）的单克隆抗体2H3，并用于证明小鼠黑素瘤细胞B16F0可以被N有效地糖工程化-苯基乙酰基-d-甘露糖胺表达N-苯基乙酰基GM3，并且在存在补体的情况下2H3对糖工程B16F0细胞具有高度的细胞毒性。进一步证明，B16F0细胞的糖工程改造能力比正常鼠胚胎成纤维细胞3T3 A31细胞高4-5倍，而且抗体和补体介导的细胞毒性对糖改造B16F0细胞的功效至少是200倍。 N-苯基乙酰基-d-甘露糖胺处理的3T3 A31细胞。这些结果表明，基于针对N-苯基乙酰基GM3的疫苗接种，然后用N-苯基乙酰基-d-甘露糖胺治疗，可以开发有用的黑色素瘤免疫疗法。

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期刊名称 other
作者
Qianli Wang; Junping Zhang; Zhongwu Guo;
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作者单位

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年(卷),期 -1(15),24
年度 -1
页码 7561–7567
总页数 13
原文格式 PDF
正文语种
中图分类
关键词
cancer immunotherapy cell glycoengineering GM3 melanoma;

机译：癌症免疫疗法;细胞糖工程;GM3;黑色素瘤;

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专利

1. Efficient glycoengineering of GM3 on melanoma cell and monoclonal antibody-mediated selective killing of the glycoengineered cancer cell [J] . Qianli Wang, Junping Zhang, Zhongwu Guo Bioorganic and Medicinal Chemistry . 2007,第24期

机译：GM3在黑素瘤细胞上的高效糖工程化和单克隆抗体介导的糖工程化癌细胞的选择性杀伤
2. Labeling glycans on living cells by a chemoenzymatic glycoengineering approach Labeling glycans on living cells by a chemoenzymatic glycoengineering approach Labeling glycans on living cells by a chemoenzymatic glycoengineering approach [J] . Ruben T. Almaraz, Yanhong Li Biology Open . 2017,第6期

机译：用化学酶糖工程方法标记活细胞上的聚糖通过化学酶糖工程方法标记活细胞上的聚糖通过化学酶糖工程方法标记活细胞上的聚糖
3. Glycoengineered monoclonal antibodies using a chemoenzymatic approach and their affinities for Fc gamma RIIIa and variable antibody-dependent cellular cytotoxicities [J] . Shirai Takashi, Kurogochi Masaki, Mori Masako, Glycobiology. . 2015,第11期

机译：使用化学酶法的糖工程单克隆抗体及其对FcγRIIIa的亲和力和可变抗体依赖性细胞毒性
4. GLYCOENGINEERING OF CHO CELLS FOR PRODUCTION OF RECOMBINANT THERAPEUTICS WITH ENHANCED EFFICACY [C] . Zhiwei Song Cell culture engineering conference . 2018

机译：CHO细胞的糖工程化以生产具有增强功效的重组疗法
5. Functionalized nanoparticles for the selective killing of cancer cells. [D] . Thevenot, Paul Todd. 2007

机译：用于选择性杀死癌细胞的功能化纳米粒子。
6. γδ T-cell killing of primary follicular lymphoma cells is dramatically potentiated by GA101 a type II glycoengineered anti-CD20 monoclonal antibody [O] . Mounia Sabrina Braza, Bernard Klein, Geneviève Fiol, 2011

机译：II型糖工程化抗CD20单克隆抗体GA101大大增强了原发性滤泡性淋巴瘤细胞的γδT细胞杀伤
7. Efficient glycoengineering of GM3 on melanoma cell and monoclonal antibody-mediated selective killing of the glycoengineered cancer cell [O] . Qianli Wang, Junping Zhang, Zhongwu Guo 2007

机译：GM3对黑色素瘤细胞和单克隆抗体介导的甘油癌细胞选择性杀死GM3的高效甘油

Efficient glycoengineering of GM3 on melanoma cell and monoclonal antibody-mediated selective killing of the glycoengineered cancer cell

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