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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Characterization of the antibody response against NeuGcGM3 ganglioside elicited in non-small cell lung cancer patients immunized with an anti-idiotype antibody.
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Characterization of the antibody response against NeuGcGM3 ganglioside elicited in non-small cell lung cancer patients immunized with an anti-idiotype antibody.

机译:在用抗独特型抗体免疫的非小细胞肺癌患者中引起的针对NeuGcGM3神经节苷脂的抗体应答的表征。

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摘要

1E10 mAb is an anti-Id murine mAb (Ab2 mAb) specific for an Ab1 mAb that reacts with NeuGc-containing gangliosides, sulfatides, and Ags expressed in some human tumors. In preclinical studies, this Ab2 Ab was able to mimic NeuGc-containing gangliosides only in animals lacking expression of these Ags in normal tissues. In this study, we report on the immune responses elicited in 20 non-small cell lung cancer patients treated with 1 mg of aluminum hydroxide-precipitated 1E10 mAb. In the hyperimmune sera from 16 of 20 patients, a strong specific Ab response of both IgM and IgG isotypes against NeuGcGM3 ganglioside was observed. Patient immune sera were able to induce complement-independent cell death of NeuGcGM3-expressing X63 murine myeloma target cells. Significant immunoreactivity to NeuGcGM3 was still detected after the complete abrogation of the reactivity against 1E10 mAb by the adsorption of patient sera with this Ab. We hypothesize that Id(-)Ag(+) Abs could reflect the activation of an autologous idiotypic cascade into the patients. Both Id(+)Ag(+) and Id(-)Ag(+) fractions were separated by affinity chromatography and characterized. Although IgG isotype Abs were found in both fractions, IgM isotype Abs were found only in the Id(-)Ag(+) fraction. Both Id(+)Ag(+) and Id(-)Ag(+) Abs were able to specifically recognize and induce cell death in NeuGcGM3-expressing X63 myeloma target cells. Patients that developed IgG and/or IgM Abs against NeuGcGM3 showed longer median survival times.
机译:1E10 mAb是对Ab1 mAb具特异性的抗Id鼠单克隆抗体(Ab2 mAb),它与某些人类肿瘤中表达的含有NeuGc的神经节苷脂,硫苷脂和Ags反应。在临床前研究中,这种Ab2 Ab仅能在正常组织中缺乏这些Ags表达的动物中模拟含NeuGc的神经节苷脂。在这项研究中,我们报道了用1 mg氢氧化铝沉淀的1E10 mAb治疗的20例非小细胞肺癌患者引起的免疫反应。在20例患者中的16例的超免疫血清中,观察到IgM和IgG同种型对NeuGcGM3神经节苷脂的强烈特异性Ab反应。患者的免疫血清能够诱导不依赖补体的表达NeuGcGM3的X63鼠骨髓瘤靶细胞的细胞死亡。通过用该抗体吸附患者血清,完全消除了对1E10 mAb的反应性后,仍然检测到对NeuGcGM3的重要免疫反应性。我们假设Id(-)Ag(+)Abs可以反映出患者自体独特型级联的激活。 Id(+)Ag(+)和Id(-)Ag(+)馏分均通过亲和色谱法分离并表征。尽管在两个馏分中均发现了IgG同种型Abs,但仅在Id(-)Ag(+)馏分中发现了IgM同种型Abs。 Id(+)Ag(+)和Id(-)Ag(+)Abs都能够特异性识别并诱导NeuGcGM3表达X63骨髓瘤靶细胞的细胞死亡。针对NeuGcGM3产生IgG和/或IgM Abs的患者显示更长的中位生存时间。

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