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人绒毛膜促性腺激素的表位及其与β链突变体免疫原性和交叉反应性的关系。

Epitopes of human chorionic gonadotropin and their relationship to immunogenicity and cross-reactivity of beta-chain mutants.

作者信息

Porakishvili N, Jackson A M, de Souza J B, Dalla Chiesa M, Roitt I M, Delves P J, Lund T

机构信息

University College London Medical School, Immunology Department, United Kingdom.

出版信息

Am J Reprod Immunol. 1998 Sep;40(3):210-4. doi: 10.1111/j.1600-0897.1998.tb00414.x.

Abstract

PROBLEM

Human chrionic gonadotropin (hCG) is a placental glycoprotein hormone, a heterodimeric molecule, consisting of alpha and beta chains. It induces the synthesis of progesterone, which is essential for the maintenance of the fertilized egg. Antibodies directed against hCG can, therefore, prevent pregnancy and serve as a vaccine. hCG belongs to the glycoprotein hormone family and shares the alpha chain with the other members. The beta chain is a hormone-specific subunit that is unique to hCG, but still possesses 85% amino acid homology with the beta chain of luteinizing hormone (LH), which means that prolonged immunization with hCG produces antibodies that cross-react with LH.

METHOD OF STUDY

We have taken an approach involving the mutation of beta hCG to eliminate cross-reactive epitopes without affecting the natural folding of the polypeptide chain and thus the unique beta hCG-specific epitopes.

RESULTS

Several mutants have been constructed that have maintained the binding to hCG-specific monoclonal antibodies (mAbs) but have lost the ability to bind to a panel of LH cross-reactive mAbs. To investigate the immunogenicity of selected mutants, mice were immunized with expression plasmid DNA, containing the gene for wild-type beta hCG and two mutants: mutant 3, with four amino acid substitutions (68 Arg-->Glu; 74 Arg-->Ser; 75 Gly-->His; 79 Val-->His), and mutant 7, with a single amino acid substitution (68 Arg-->Glu).

CONCLUSIONS

Although both mutants were able to elicit antibody responses in at least some animals, the levels were less than those seen with the wild-type beta hCG DNA, and there seems still to be a residual cross-reactivity with LH. Attempts to improve the immunogenicity of the mutants and to further modify the sequence to remove the cross-reactivity are currently underway.

摘要

问题

人绒毛膜促性腺激素(hCG)是一种胎盘糖蛋白激素,为异二聚体分子,由α链和β链组成。它可诱导孕酮的合成,而孕酮对于受精卵的维持至关重要。因此,针对hCG的抗体可预防妊娠并用作疫苗。hCG属于糖蛋白激素家族,与其他成员共享α链。β链是hCG特有的激素特异性亚基,但与促黄体生成素(LH)的β链仍具有85%的氨基酸同源性,这意味着用hCG进行长期免疫会产生与LH发生交叉反应的抗体。

研究方法

我们采用了一种方法,即对β-hCG进行突变,以消除交叉反应性表位,同时不影响多肽链的天然折叠,从而保留β-hCG特有的独特表位。

结果

构建了几种突变体,它们保持了与hCG特异性单克隆抗体(mAb)的结合能力,但失去了与一组LH交叉反应性mAb结合的能力。为了研究所选突变体的免疫原性,用表达质粒DNA对小鼠进行免疫,该质粒DNA包含野生型β-hCG基因和两个突变体:突变体3,有四个氨基酸取代(68位精氨酸→谷氨酸;74位精氨酸→丝氨酸;75位甘氨酸→组氨酸;79位缬氨酸→组氨酸),以及突变体7,有一个氨基酸取代(68位精氨酸→谷氨酸)。

结论

尽管两种突变体都能够在至少一些动物中引发抗体反应,但反应水平低于野生型β-hCG DNA所引发的水平,并且似乎与LH仍存在残留的交叉反应性。目前正在尝试提高突变体的免疫原性,并进一步修改序列以消除交叉反应性。

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