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神经母细胞瘤相关抗原GD2特异性二聚体小免疫蛋白的产生与特性分析

Generation and characterization of dimeric small immunoproteins specific for neuroblastoma associated antigen GD2.

作者信息

Occhino Marzia, Raffaghello Lizzia, Burrone Oscar, Gambini Claudio, Pistoia Vito, Corrias Maria Valeria, Bestagno Marco

机构信息

International Centre for Genetic Engineering and Biotechnology, 34012 Trieste, Italy.

出版信息

Int J Mol Med. 2004 Sep;14(3):383-8.

Abstract

GD2 is a disialoganglioside expressed at high density on the surface of malignant cells of neuroectodermal origin, especially in neuroblastoma (NB) and melanoma. Since its expression in normal tissues is very restricted, GD2 represents an excellent target for neuroectodermal tumor targeting. Mini-antibody technology allows the production of dimeric single-chain antibodies, also called small immunoproteins (SIPs), which are composed of a scFv fused to a dimerizing domain of immunoglobulin heavy chains. Dimerization results in an increase of the total apparent affinity and a slower clearance in vivo than scFvs. These properties make SIPs very attractive molecules for tumor targeting. We isolated the variable regions from an anti-GD2 monoclonal antibody and exploited the SIP technology to generate two novel anti-GD2 SIPs. The first anti-GD2 SIP is a fully murine molecule containing the CH3 domain of mouse IgG1, whereas the second construct is a hybrid mouse-human molecule containing the CH4 domain of human IgE. Both mini-antibodies were successfully produced and shown to retain binding specificity as well as an affinity similar to that of the original antibody.

摘要

GD2是一种双唾液酸神经节苷脂,在神经外胚层来源的恶性细胞表面高密度表达,尤其是在神经母细胞瘤(NB)和黑色素瘤中。由于其在正常组织中的表达非常有限,GD2是神经外胚层肿瘤靶向治疗的理想靶点。微型抗体技术能够生产二聚体单链抗体,也称为小型免疫蛋白(SIP),它由一个与免疫球蛋白重链二聚化结构域融合的单链抗体片段(scFv)组成。二聚化导致总表观亲和力增加,并且在体内的清除速度比单链抗体片段慢。这些特性使SIP成为肿瘤靶向治疗中非常有吸引力的分子。我们从一种抗GD2单克隆抗体中分离出可变区,并利用SIP技术生成了两种新型抗GD2 SIP。第一种抗GD2 SIP是一个完全由小鼠组成的分子,包含小鼠IgG1的CH3结构域,而第二种构建体是一个小鼠-人杂交分子,包含人IgE的CH4结构域。两种微型抗体均成功制备,并显示保留了结合特异性以及与原始抗体相似的亲和力。

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