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非人灵长类动物对人黑色素瘤双唾液酸神经节苷脂GD3的血清学反应。

Serological response of non-human primates to human melanoma disialoganglioside GD3.

作者信息

Stuhlmiller G M, Roberson K M, Seigler H F

机构信息

Department of Surgery, Duke University Medical Center, Durham, NC 27710.

出版信息

Cancer Immunol Immunother. 1989;29(3):205-10. doi: 10.1007/BF00199997.

Abstract

The immunogenicity of the disialoganglioside, GD3, a melanoma-tumor-associated antigen, has been evaluated in non-human primates. Sera from four chimpanzees and two monkeys were evaluated for anti-GD3 antibody activity by solid-phase radioimmunoassay using GD3 and control gangliosides as targets. Serum from one monkey, immunized with cells from a melanoma cell line, was strongly reactive with GD3, having a titer of greater than 2500. In contrast, serum from this animal was non-reactive with several other gangliosides including the structurally similar GM3. Anti-GD3 reactivity was also demonstrable, albeit in low titer, in the sera of an additional monkey and a chimpanzee. Each of these animals had likewise been immunized using cells from melanoma cell lines. On the basis of these observations, suggestive of a primate anti-GD3 antibody response, we initiated a series of immunizations of chimpanzee using purified GD3 bound to Salmonella minnesota, R595. IgG reactive with melanoma cells in the cell-binding assay was first detected in sera collected after 4 immunizations and increased in titer against each reactive melanoma cell line during the immunizations. Reactivity of this serum with melanoma cell lines demonstrated a direct correlation with the expression of GD3 by the respective cell line. Anti-GD3 reactivity was evident in solid-phase radioimmunoassay against purified GD3 beginning with serum collected after 11 immunizations. By comparison with its binding to the control ganglioside panel, this serum demonstrated strong specificity for GD3 (titer = 640) while having only marginal reactivity with GM3 (titer = 40). Immune serum from this animal was also able specifically to block subsequent binding of a murine IgM anti-GD3 antibody (DMab7) to target GD3 in solid-phase radioimmunoassay. Together, these observations suggest that GD3, in the form of a purified molecule bound to a bacterial matrix or as part of the intact melanoma cell membrane, can be immunogenic in non-human primates, and is able to elicit an antibody response of appropriate specificity.

摘要

二唾液酸神经节苷脂GD3是一种与黑色素瘤肿瘤相关的抗原,其免疫原性已在非人类灵长类动物中进行了评估。使用GD3和对照神经节苷脂作为靶点,通过固相放射免疫测定法评估了4只黑猩猩和2只猴子的血清中的抗GD3抗体活性。用黑色素瘤细胞系的细胞免疫的一只猴子的血清与GD3强烈反应,效价大于2500。相比之下,该动物的血清与包括结构相似的GM3在内的其他几种神经节苷脂无反应。在另一只猴子和一只黑猩猩的血清中也可证明有抗GD3反应性,尽管效价较低。这些动物中的每一只同样也用黑色素瘤细胞系的细胞进行了免疫。基于这些提示灵长类动物抗GD3抗体反应的观察结果,我们开始了一系列用与明尼苏达沙门氏菌R595结合的纯化GD3对黑猩猩进行免疫的实验。在细胞结合试验中与黑色素瘤细胞反应的IgG首先在4次免疫后收集的血清中被检测到,并且在免疫过程中针对每个反应性黑色素瘤细胞系的效价都有所增加。该血清与黑色素瘤细胞系的反应性与各个细胞系中GD3的表达呈直接相关。从第11次免疫后收集的血清开始,在针对纯化GD3的固相放射免疫测定中抗GD3反应性明显。通过与它与对照神经节苷脂组的结合情况比较,该血清对GD3表现出强特异性(效价=640),而与GM3只有微弱反应性(效价=40)。该动物的免疫血清在固相放射免疫测定中也能够特异性地阻断鼠IgM抗GD3抗体(DMab7)与靶标GD3的后续结合。总之,这些观察结果表明,以与细菌基质结合的纯化分子形式或作为完整黑色素瘤细胞膜一部分的GD3在非人类灵长类动物中具有免疫原性,并且能够引发具有适当特异性的抗体反应。

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