首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Specific activation and targeting of cytotoxic lymphocytes through chimeric single chains consisting of antibody-binding domains and the gamma or zeta subunits of the immunoglobulin and T-cell receptors.
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Specific activation and targeting of cytotoxic lymphocytes through chimeric single chains consisting of antibody-binding domains and the gamma or zeta subunits of the immunoglobulin and T-cell receptors.

机译:通过由抗体结合结构域以及免疫球蛋白和T细胞受体的γ或zeta亚基组成的嵌合单链特异性激活和靶向细胞毒性淋巴细胞。

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摘要

The generation of tumor-specific lymphocytes and their use in adoptive immunotherapy is limited to a few malignancies because most spontaneous tumors are very weak or not at all immunogenic. On the other hand, many anti-tumor antibodies have been described which bind tumor-associated antigens shared among tumors of the same histology. Combining the variable regions (Fv) of an antibody with the constant regions of the T-cell receptor (TCR) chains results in chimeric genes endowing T lymphocytes with antibody-type specificity, potentially allowing cellular adoptive immunotherapy against types of tumors not previously possible. To generalize and extend this approach to additional lymphocyte-activating molecules, we designed and constructed chimeric genes composed of a single-chain Fv domain (scFv) of an antibody linked with gamma or zeta chains, the common signal-transducing subunits of the immunoglobulin receptor and the TCR. Such chimeric genes containing the Fv region of an anti-trinitophenyl antibody could be expressed as functional surface receptors in a cytolytic T-cell hybridoma. They triggered interleukin 2 secretion upon encountering antigen and mediated non-major-histocompatibility-complex-restricted hapten-specific target cell lysis. Such chimeric receptors can be exploited to provide T cells and other effector lymphocytes, such as natural killer cells, with antibody-type recognition directly coupled to cellular activation.
机译:肿瘤特异性淋巴细胞的产生及其在过继免疫疗法中的应用仅限于少数恶性肿瘤,因为大多数自发性肿瘤非常脆弱或完全没有免疫原性。另一方面,已经描述了许多抗肿瘤抗体,其结合相同组织学的肿瘤之间共享的肿瘤相关抗原。将抗体的可变区(Fv)与T细胞受体(TCR)链的恒定区结合在一起,会产生赋予T淋巴细胞以抗体类型特异性的嵌合基因,从而有可能允许针对以前不可能的肿瘤进行细胞过继免疫治疗。为了将这种方法推广并扩展到其他淋巴细胞激活分子,我们设计和构建了由与免疫球蛋白受体的常见信号传导亚基γ或ζ链连接的抗体的单链Fv结构域(scFv)组成的嵌合基因和TCR。此类包含抗三苯甲基苯基抗体的Fv区的嵌合基因可以在溶细胞性T细胞杂交瘤中表达为功能性表面受体。他们遇到抗原并介导非主要组织相容性复合物限制的半抗原特异性靶细胞裂解后触发白介素2分泌。可以利用这种嵌合受体为T细胞和其他效应淋巴细胞(例如自然杀伤细胞)提供直接与细胞活化偶联的抗体类型识别。

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