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用代表人类促卵泡激素β亚基序列33 - 53的抗肽抗血清在体外抑制促卵泡激素的生物活性。

In vitro inhibition of the biological activity of follicle-stimulating hormone by anti-peptide antisera representing the human follicle-stimulating hormone beta subunit sequence 33-53.

作者信息

Westhoff W E, Slootstra J W, Puijk W C, van Leeuwen L, Schaaper W M, Oonk H B, Meloen R H

机构信息

Institute for Animal Science and Health, Department of Molecular Recognition, Lelystad, The Netherlands.

出版信息

Biol Reprod. 1997 Feb;56(2):460-8. doi: 10.1095/biolreprod56.2.460.

DOI:10.1095/biolreprod56.2.460
PMID:9116147
Abstract

There are few male contraceptive methods, and research is required to broaden the scope of available male antifertility methods. Two approaches toward hormonal contraception are currently being investigated. The first relies on elimination of testosterone while the second is based upon immunizations against FSH. However, most anti-whole FSH antisera cross-react with LH, thereby possibly inhibiting testosterone and leading to potential loss of libido. Therefore, a more effective alternative would be to define an FSH peptide that differs significantly from LH in order to prevent cross-reactivity between anti-FSH antisera and LH. Two peptides were selected from the beta subunit of FSH that were considered to be inducers of anti-FSH activity but not anti-LH activity. The first peptide (sequence beta33-53) is a linear antigenic site of human FSH found only in anti-FSH antisera that do not cross-react with LH. The second peptide (sequence beta81-95) is a part of FSH that confers receptor specificity. These peptides, in monomer and tandem form, were used to immunize rabbits. The antisera were tested for inhibition of FSH activity in a bioassay; they were also tested in a Leydig cell assay to detect anti-LH activity. It was found that antisera raised against the beta33-53 tandem could inhibit the FSH bioactivity but not that of LH. Antisera against the beta33-53 monomer or the beta81-95 monomer or tandem did not inhibit FSH. Thus, the tandem peptide beta33-53 is an attractive candidate for use as antigen in a male contraceptive vaccine. The better results obtained with tandem vaccinations might be related to the ability of the tandem peptide to direct the antibody response toward the N-terminal end of the peptide and to raise antisera with the ability to react with shorter chains of amino acids.

摘要

男性避孕方法很少,需要开展研究以扩大可用的男性抗生育方法的范围。目前正在研究两种激素避孕方法。第一种方法依赖于消除睾酮,而第二种方法基于针对促卵泡激素(FSH)的免疫接种。然而,大多数抗全FSH抗血清会与促黄体生成素(LH)发生交叉反应,从而可能抑制睾酮并导致性欲潜在丧失。因此,一种更有效的替代方法是确定一种与LH有显著差异的FSH肽,以防止抗FSH抗血清与LH之间发生交叉反应。从FSH的β亚基中选择了两种肽,它们被认为是抗FSH活性而非抗LH活性的诱导剂。第一种肽(序列β33 - 53)是人类FSH的线性抗原位点,仅存在于不与LH发生交叉反应的抗FSH抗血清中。第二种肽(序列β81 - 95)是赋予FSH受体特异性的一部分。这些肽以单体和串联形式用于免疫兔子。在生物测定中测试抗血清对FSH活性的抑制作用;还在睾丸间质细胞测定中对其进行测试以检测抗LH活性。结果发现,针对β33 - 53串联肽产生的抗血清可以抑制FSH的生物活性,但不能抑制LH的生物活性。针对β33 - 53单体或β81 - 95单体或串联肽产生的抗血清不能抑制FSH。因此,串联肽β33 - 53是用作男性避孕疫苗抗原的有吸引力的候选物。串联接种获得的更好结果可能与串联肽引导抗体反应朝向肽的N末端并产生能够与较短氨基酸链反应的抗血清的能力有关。

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In vitro inhibition of the biological activity of follicle-stimulating hormone by anti-peptide antisera representing the human follicle-stimulating hormone beta subunit sequence 33-53.用代表人类促卵泡激素β亚基序列33 - 53的抗肽抗血清在体外抑制促卵泡激素的生物活性。
Biol Reprod. 1997 Feb;56(2):460-8. doi: 10.1095/biolreprod56.2.460.
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