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肿瘤独特型疫苗。VII. 保护性和非保护性Ab2的结构、独特型及生物学特性的分析与关联

Tumor idiotype vaccines. VII. Analysis and correlation of structural, idiotypic, and biologic properties of protective and nonprotective Ab2.

作者信息

Raychaudhuri S, Kang C Y, Kaveri S V, Kieber-Emmons T, Köhler H

机构信息

IDEC Pharmaceuticals, La Jolla, CA 92037.

出版信息

J Immunol. 1990 Jul 15;145(2):760-7.

PMID:2164069
Abstract

We have previously generated and used anti-Id mAb (Ab2) to induce protective immunity against the L1210 DBA/2 tumor and for immunotherapy of established tumors. Among various anti-Id that were typed serologically as internal image Ab2 of the mouse mammary tumor virus tumor-associated Ag gp52, only one induced protective immunity and was effective in immunotherapy. In this study we compared the structural, idiotypic, and network properties of the protective and nonprotective antiidiotypic antibodies. The DNA sequence of the variable regions of six anti-Id was determined. The VH sequence of four Ab2, including the protective Ab2, are highly homologous, whereas the VL sequences differ and were assigned to different Vk families. In addition, the DH sequence region of the same four Ab2 are identical, whereas one is highly homologous and another one without homology. Search for amino acid sequence homologies between the Ab2 and gp52 showed the strongest similarities in the CDR2 of the L chain from the protective Ab2. In addition, the CDR2 region also had homology with a T cell epitope on gp52. The biologic basis of effective idiotypic mimicry was studied at the level of Ab3 induced by the Ab2. Id inhibition analysis using Ab3 induced by either protective or nonprotective Ab2, revealed differences. Thus, there is evidence for differences among the Ab1-Ab2-Ab3 cascade induced by protective and nonprotective anti-Id.

摘要

我们之前已制备并使用抗独特型单克隆抗体(Ab2)来诱导针对L1210 DBA/2肿瘤的保护性免疫,并用于已形成肿瘤的免疫治疗。在通过血清学鉴定为小鼠乳腺肿瘤病毒肿瘤相关抗原gp52的内影像Ab2的各种抗独特型抗体中,只有一种诱导了保护性免疫且在免疫治疗中有效。在本研究中,我们比较了保护性和非保护性抗独特型抗体的结构、独特型和网络特性。测定了六种抗独特型抗体可变区的DNA序列。包括保护性Ab2在内的四种Ab2的VH序列高度同源,而VL序列不同,并被归入不同的Vk家族。此外,相同的四种Ab2的DH序列区域相同,而一种高度同源,另一种无同源性。搜索Ab2与gp52之间的氨基酸序列同源性发现,保护性Ab2轻链的CDR2中相似性最强。此外,CDR2区域也与gp52上的一个T细胞表位具有同源性。在由Ab2诱导的Ab3水平上研究了有效独特型模拟的生物学基础。使用由保护性或非保护性Ab2诱导的Ab3进行的独特型抑制分析揭示了差异。因此,有证据表明保护性和非保护性抗独特型抗体诱导的Ab1-Ab2-Ab3级联之间存在差异。

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