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抗GD3神经节苷脂小鼠单克隆抗体的同源性结合

Homophilic binding of mouse monoclonal antibodies against GD3 ganglioside.

作者信息

Chapman P B, Yuasa H, Houghton A N

机构信息

Department of Medicine, Memorial Sloan-Kettering Cancer Center, New York, NY 10021.

出版信息

J Immunol. 1990 Aug 1;145(3):891-8.

PMID:1695649
Abstract

R24, a mouse IgG3 mAb against GD3 ganglioside, was shown to bind to itself in a homophilic manner. This was demonstrated by augmented binding of 125I-labeled R24 to the cell surface of GD3+ cells by unlabeled R24 and by direct binding of biotinylated R24 to R24 adsorbed on solid phase. Although homophilic binding was evident when R24 was bound to solid phase, R24-R24 aggregates could not be detected in solution under otherwise identical conditions. R24 bound to four other mAb (two IgG3, one IgG2a, one IgM) directed against GD3 but did not bind to a panel of 21 other mAb including other IgG3 mAb and mAb directed against non-GD3 ganglioside. Evidence implicating the GD3-binding site of R24 in homophilic binding included the following observations: 1) F(ab')2 fragments of R24 could bind to R24, 2) an antiidiotypic mAb against the GD3-binding site of R24 inhibited R24 homophilic binding, 3) an IgM anti-GD3 mAb also demonstrated homophilic binding to R24, and 4) homophilic binding was a function of immunoreactivity and avidity for GD3. R24 variants with 40-fold lower avidity for GD3 demonstrated a similar decrease in homophilic binding. Inasmuch as R24 bound to R24 F(ab')2 fragments and specifically to anti-GD3 mAb, it appeared that the target for homophilic binding was an epitope within the V region of anti-GD3 mAb. It is likely that homophilic interactions result in increased affinity of R24 for GD3 through increased effective valency of antibody-Ag complexes.

摘要

R24是一种抗GD3神经节苷脂的小鼠IgG3单克隆抗体,已证明它能以同源亲和的方式自身结合。未标记的R24增强了125I标记的R24与GD3+细胞表面的结合,以及生物素化的R24与吸附在固相上的R24的直接结合,从而证明了这一点。尽管当R24结合到固相时同源亲和结合很明显,但在其他相同条件下,在溶液中未检测到R24-R24聚集体。R24与另外四种针对GD3的单克隆抗体(两种IgG3、一种IgG2a、一种IgM)结合,但不与包括其他IgG3单克隆抗体和针对非GD3神经节苷脂的单克隆抗体在内的另外21种单克隆抗体结合。涉及R24的GD3结合位点参与同源亲和结合的证据包括以下观察结果:1)R24的F(ab')2片段能与R24结合;2)一种针对R24的GD3结合位点的抗独特型单克隆抗体抑制R24的同源亲和结合;3)一种IgM抗GD3单克隆抗体也表现出与R24的同源亲和结合;4)同源亲和结合是对GD3的免疫反应性和亲和力的函数。对GD3亲和力降低40倍的R24变体在同源亲和结合方面也有类似程度的降低。由于R24与R24的F(ab')2片段结合且特异性地与抗GD3单克隆抗体结合,同源亲和结合的靶点似乎是抗GD3单克隆抗体V区内某一表位。同源亲和相互作用很可能通过增加抗体-抗原复合物的有效价来提高R24对GD3的亲和力。

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