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通过吖啶橙诱变产生具有生物活性的抗新型隐球菌IgG、IgE和IgA同种型转换变体抗体。

Generation of biologically active anti-Cryptococcus neoformans IgG, IgE and IgA isotype switch variant antibodies by acridine orange mutagenesis.

作者信息

Spira G, Paizi M, Mazar S, Nussbaum G, Mukherjee S, Casadevall A

机构信息

Bruce Rappaport Faculty of Medicine, Haifa, Israel.

出版信息

Clin Exp Immunol. 1996 Sep;105(3):436-42. doi: 10.1046/j.1365-2249.1996.d01-786.x.

Abstract

Administration of MoAbs to Cryptococcus neoformans capsular glucuronoxylomannan (GXM) can alter the course of infection in mouse models. However, the effectiveness of these antibodies appears to depend on isotype and specificity. Comparison of isotype protection efficacy requires families of MoAbs with identical fine specificity and different constant region domain. The generation of such families by hybridoma technology is not always possible because the immune response produces MoAbs of limited classes or subclasses. In these instances isotype switch variants can be isolated in vitro. Unfortunately, standard methods of recovering spontaneous switch variants are often unsuccessful, mainly because of the low frequency of switching. In this study we demonstrate that acridine orange stimulation of an IgG3 anti-C. neoformans-producing hybridoma can be used to recover the entire set of isotype switch variants: IgGl, IgG2b, IgG2a, IgE and IgA. All isotype switch variants bind to GXM; fine specificity mapping, using an 11 amino acid peptide polysaccharide mimetope, revealed conservation of binding site specificity. Furthermore, all isotype switch variants reacted with an anti-idiotopic MoAb. The functional activity of this set of MoAbs was demonstrated by their ability to enhance phagocytosis and antifungal efficacy of human macrophage-like THP-1 cells, with IgG3 being the most effective and IgE being the least effective.

摘要

向新型隐球菌荚膜葡糖醛酸木聚糖甘露聚糖(GXM)施用单克隆抗体(MoAbs)可改变小鼠模型中的感染进程。然而,这些抗体的有效性似乎取决于同种型和特异性。比较同种型保护效力需要具有相同精细特异性和不同恒定区结构域的单克隆抗体家族。通过杂交瘤技术产生这样的家族并不总是可行的,因为免疫反应产生的单克隆抗体类别或亚类有限。在这些情况下,可以在体外分离同种型转换变体。不幸的是,恢复自发转换变体的标准方法通常不成功,主要是因为转换频率低。在本研究中,我们证明吖啶橙刺激产生IgG3抗新型隐球菌的杂交瘤可用于恢复整个同种型转换变体集:IgG1、IgG2b、IgG2a、IgE和IgA。所有同种型转换变体均与GXM结合;使用11个氨基酸的肽多糖模拟表位进行精细特异性图谱分析,揭示了结合位点特异性的保守性。此外,所有同种型转换变体均与抗独特型单克隆抗体反应。这组单克隆抗体的功能活性通过其增强人巨噬细胞样THP-1细胞吞噬作用和抗真菌效力的能力得以证明,其中IgG3最有效,IgE最无效。

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