首页> 美国卫生研究院文献>Infection and Immunity >Cross-reactivity between haptenic muramyl di- or tripeptide derivatives and Mycobacterium bovis BCG: potential application for enhancing tumor immunity.
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Cross-reactivity between haptenic muramyl di- or tripeptide derivatives and Mycobacterium bovis BCG: potential application for enhancing tumor immunity.

机译:半抗原二酰二肽或三肽衍生物与牛分枝杆菌BCG之间的交叉反应性:增强肿瘤免疫力的潜在应用。

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摘要

Muramyl di- or tripeptide (MDP or MTP) hapten derivatives bearing various structures were synthesized, and the correlation of these structures with cross-reactivity with Mycobacterium bovis BCG and their applicability to enhance induction of syngeneic tumor immunity were investigated. The cross-reactivity of MDP or MTP haptens to BCG was examined by T-cell proliferation responses of lymph node cells from BCG-primed C3H/He mice in the stimulation with MDP- or MTP-coupled syngeneic cells. A haptenic MDP derivative (designated L4-MDP) stimulated proliferative responses appreciably. Derivatives in which alanine in the peptide portion of L4-MDP was replaced by methylalanine or valine failed to induce stimulation. However, the cross-reactivity with BCG was regained in the MTP derivative that was formed by adding lysine to dipeptide containing methylalanine or valine. Whether this cross-reactive pattern was correlated with enhanced induction of tumor immunity was further investigated. According to the established protocol for the augmented induction of tumor immunity, BCG-primed C3H/He mice were immunized with various haptenic MDP-coupled syngeneic X5563 tumor cells. Immunization with tumor cells conjugating BCG-cross-reactive haptens resulted in enhanced tumor immunity, whereas immunization with tumor cells coupling non-cross-reactive haptens failed to produce anti-X5563 tumor immunity. These results indicate that the peptide portion in these haptenic structures is critical in the generation of BCG cross-reactivity leading to enhanced tumor immunity.
机译:合成了带有各种结构的Muramyl二肽或三肽(MDP或MTP)半抗原衍生物,并研究了这些结构与牛分枝杆菌BCG交叉反应的相关性及其在增强诱导同基因肿瘤免疫性方面的适用性。 MDP或MTP半抗原与BCG的交叉反应性是通过在MDP或MTP偶联的同系细胞刺激下,来自BCG引发的C3H / He小鼠的淋巴结细胞的T细胞增殖反应来检查的。半抗原的MDP衍生物(称为L4-MDP)可明显刺激增殖反应。其中L4-MDP的肽部分中的丙氨酸被甲基丙氨酸或缬氨酸取代的衍生物不能诱导刺激。但是,通过向包含甲基丙氨酸或缬氨酸的二肽中添加赖氨酸形成的MTP衍生物,又重新获得了与BCG的交叉反应性。进一步研究了这种交叉反应模式是否与增强的肿瘤免疫力相关。根据已建立的增强诱导肿瘤免疫的方案,用各种半抗原与MDP偶联的同系X5563肿瘤细胞免疫BCG启动的C3H / He小鼠。结合BCG交叉反应性半抗原的肿瘤细胞免疫可增强肿瘤免疫力,而结合非交叉反应性半抗原的肿瘤细胞免疫则无法产生抗X5563肿瘤免疫力。这些结果表明,这些半抗原结构中的肽部分在BCG交叉反应性的产生中是至关重要的,从而导致增强的肿瘤免疫力。

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