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利用杂交杂交瘤靶向人类细胞毒性T淋巴细胞。

The use of hybrid hybridomas to target human cytotoxic T lymphocytes.

作者信息

Lanzavecchia A, Scheidegger D

出版信息

Eur J Immunol. 1987 Jan;17(1):105-11. doi: 10.1002/eji.1830170118.

Abstract

This study describes a general strategy to produce hybrid monoclonal antibodies that are capable of targeting human cytotoxic T lymphocytes (CTL) against any cell carrying the appropriate target antigen. This is done by fusing a HAT-sensitive, G418-resistant anti-T3 hybridoma with immune spleen cells (or with other hybridomas) that produce antibodies against the desired target antigen. In the hybrid hybridomas the reassortment of Ig heavy and light chains results in the production of bifunctional antibody molecules. Because of their double specificity, these antibodies are able to bridge human CTL to target cells and trigger cytotoxic function. We have isolated several stable hybrid hybridomas in which one specificity is against T3 and one either against HLA antigens (class II, DC-1, A3), human Ig (IgM, IgE, kappa), Toxoplasma gondii or an ovary carcinoma-associated antigen. In all of these cases we show that culture supernatants can efficiently and specifically target any CTL clone against any target cell that possesses the relevant surface antigen recognized by the antibody. Furthermore, the killing requires as little as 0.1 ng/ml of antibody, occurs at effector to target ratios comparable to those used in conventional cytotoxic assays and does not affect bystander cells. Nonspecific killing of Fc receptor-positive cells can be avoided using F(ab')2 fragments. As an example, we show that it is possible to change the major histocompatibility complex class and allospecificity of a CTL clone and target CTL against non-major histocompatibility complex antigens such as Ig, parasites and tumor-associated antigens.

摘要

本研究描述了一种产生杂交单克隆抗体的通用策略,该抗体能够将人类细胞毒性T淋巴细胞(CTL)靶向携带适当靶抗原的任何细胞。这是通过将对次黄嘌呤氨基蝶呤-氨基蝶呤-胸腺嘧啶核苷(HAT)敏感、对G418耐药的抗T3杂交瘤与产生针对所需靶抗原的抗体的免疫脾细胞(或其他杂交瘤)融合来实现的。在杂交杂交瘤中,免疫球蛋白重链和轻链的重排导致双功能抗体分子的产生。由于其双重特异性,这些抗体能够将人类CTL连接到靶细胞并触发细胞毒性功能。我们已经分离出几种稳定的杂交杂交瘤,其中一种特异性针对T3,另一种针对HLA抗原(II类,DC-1,A3)、人类免疫球蛋白(IgM、IgE、κ)、弓形虫或卵巢癌相关抗原。在所有这些情况下,我们表明培养上清液可以有效地、特异性地将任何CTL克隆靶向任何具有该抗体识别的相关表面抗原的靶细胞。此外,杀伤所需的抗体低至0.1 ng/ml,在效应细胞与靶细胞比例与传统细胞毒性测定中使用的比例相当的情况下发生,并且不影响旁观者细胞。使用F(ab')2片段可以避免对Fc受体阳性细胞的非特异性杀伤。例如,我们表明可以改变CTL克隆的主要组织相容性复合体类别和同种特异性,并将CTL靶向非主要组织相容性复合体抗原,如免疫球蛋白、寄生虫和肿瘤相关抗原。

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