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小鼠对带有脂质基团的蛋白质载体上大或小分子半抗原偶联物的迟发型超敏反应的特异性

Specificity of murine delayed-type hypersensitivity to conjugates of large or small haptens on protein carriers bearing lipid groups.

作者信息

Snippe H, Johannesen L, Inman J K, Merchant B

出版信息

Immunology. 1978 May;34(5):947-54.

Abstract

Delayed-type hypersensitivity (DH) in the mouse was provoked with different hapten-carrier complexes mixed with the cationic, surface-active lipid, dimethyl dioctadecyl ammonium bromide (DDA). DH was measured as footpad swelling. Conjugates of bovine serum albumin (BSA) with the small haptens dinitrophenyl (DNP), 'arsonate' (ARS) and 'sulphonate' (SULPH) served to generate strong DH reactions towards the homologous antigen. Insertion of a tripeptide spacer between the hapten and carrier resulted in lower DH reactivity. Optimal dosages and optimal time intervals between sensitization and DH elicitation were determined for the enlarged hapten-carrier complexes. Cyclophosphamide (CY) treatment, before priming with complexes mixed with DDA, caused a 5-6 day delay in the expression of DH but failed to evoke enhanced DH for any of the antigens tested. A broad array of cross reactions between small and enlarged hapten-carrier complexes showed a relative lack of specificity in these DH responses. The results are compared with others reported in the literature and are explained mainly by the effects of electrostatically bound lipid groups of DDA in the sensitizing conjugates.

摘要

将不同的半抗原 - 载体复合物与阳离子表面活性脂质二甲基二十八烷基溴化铵(DDA)混合,诱发小鼠的迟发型超敏反应(DH)。以足垫肿胀来测量DH。牛血清白蛋白(BSA)与小半抗原二硝基苯基(DNP)、“砷酸盐”(ARS)和“磺酸盐”(SULPH)的缀合物用于产生针对同源抗原的强烈DH反应。在半抗原和载体之间插入三肽间隔物会导致较低的DH反应性。确定了扩大的半抗原 - 载体复合物的最佳剂量以及致敏和DH激发之间的最佳时间间隔。在用与DDA混合的复合物进行初次免疫之前,用环磷酰胺(CY)处理会使DH的表达延迟5 - 6天,但未能对任何测试抗原诱发增强的DH。小的和扩大的半抗原 - 载体复合物之间广泛的交叉反应表明这些DH反应相对缺乏特异性。将结果与文献中报道的其他结果进行了比较,主要通过致敏缀合物中DDA的静电结合脂质基团的作用来解释。

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