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通过体外和体内方法研究的针对有机酸酐化学结构的抗体特异性。

Antibody specificity to the chemical structures of organic acid anhydrides studied by in-vitro and in-vivo methods.

作者信息

Zhang X D, Lötvall J, Skerfving S, Welinder H

机构信息

Department of Occupational and Environmental Medicine, University Hospital, Lund, Sweden.

出版信息

Toxicology. 1997 Mar 28;118(2-3):223-32. doi: 10.1016/s0300-483x(96)03605-0.

Abstract

The objective of the study was to evaluate the structure-activity relationship for the antigenic activity of different organic acid anhydrides (OAAs). The specificity of guinea pig (GP) IgG1 to different anhydrides was studied by ELISA-inhibition, PCA, and airway provocation tests of cross-reactivity with different OAA conjugates. In the airway provocation tests, lung resistance and plasma extravasation of Evan's Blue dye was measured. The ELISA-inhibition tests showed a wide range in antibody specificity. Modelling of ring configuration, methyl group substitution, double bond position, and cis/trans isomerism of anhydride forming carboxyl groups influenced the specificity. There was a general consistency in cross-reactivity of anti-cis-hexahydrophthalic anhydride IgG1 versus GP serum albumin conjugates of trans-hexahydrophthalic anhydride, phthalic anhydride, and succinic anhydride as shown by ELISA-inhibition, PCA, and airway provocation tests. It is concluded that various modifications of the chemical structures of a hapten are recognized by the hapten-specific antibodies, and that these differences may have clinical relevance. In particular, the ring structure and the positions of double bonds and of methyl groups are important. Further, the in-vitro ELISA-inhibition tests show a good agreement with the in-vivo PCA and bronchial provocation tests.

摘要

本研究的目的是评估不同有机酸酐(OAA)的抗原活性的构效关系。通过ELISA抑制试验、被动皮肤过敏反应(PCA)以及与不同OAA结合物交叉反应的气道激发试验,研究豚鼠(GP)IgG1对不同酸酐的特异性。在气道激发试验中,测量肺阻力和伊文思蓝染料的血浆外渗情况。ELISA抑制试验显示抗体特异性范围广泛。酸酐形成羧基的环构型、甲基取代、双键位置和顺/反异构化的模型影响了特异性。ELISA抑制试验、PCA和气道激发试验表明,抗顺式六氢邻苯二甲酸酐IgG1与反式六氢邻苯二甲酸酐、邻苯二甲酸酐和琥珀酸酐的GP血清白蛋白结合物的交叉反应具有总体一致性。得出的结论是,半抗原特异性抗体可识别半抗原化学结构的各种修饰,且这些差异可能具有临床相关性。特别是,环结构以及双键和甲基的位置很重要。此外,体外ELISA抑制试验与体内PCA和支气管激发试验显示出良好的一致性。

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