Generating FSH antagonists and agonists through immunization against FSH receptor N-terminal decapeptides

被引:33
作者
Abdennebi, L [1 ]
Couture, L [1 ]
Grebert, D [1 ]
Pajot, E [1 ]
Salesse, R [1 ]
Remy, JJ [1 ]
机构
[1] INRA, Unite Recepteurs & Commun Cellulaires, F-78352 Jouy En Josas, France
关键词
D O I
10.1677/jme.0.0220151
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Follicle-stimulating hormone (FSH) via interaction with G-protein coupled specific receptors plays a central role in the control of gametogenesis in mammals of both sexes. In females, FSH is crucial for follicle growth, follicle maturation and ovulation. FSH receptors, together with luteinizing hormone-chorionic gonadotropin and thyrotropin receptors belong to a subfamily of structurally related receptors within the seven transmembrane receptor family. Among several other regions, the N-terminus of these receptors is believed to be responsible for important specific hormone-receptor contact sites. Recombinant filamentous phages displaying at their surface three overlapping N-terminal decapeptides of the FSH receptor, peptides A18-27, B25-34 and C29-38 were constructed. Ewes and female mice were immunized against the three FSH receptor (FSHR) recombinant phages, Immunoglobulins purified from immunized animals were analyzed for their bio chemical properties on a Chinese hamster ovary cell line expressing the porcine FSH receptor. AntiA and antiB immunoglobulins (IgGs) behave as antagonists for I-125-FSH binding and for FSH-dependent cAMP production, while antiC IgGs did not compete fur hormone binding. By contrast, antibodies against the C29-38 peptide displayed FSH agonist activity and stimulated the FSH receptor, whereas antiA and antiB IgGs did not. Furthermore, when the FSHR phages were used as peptidic vaccines, they induced a reversible inhibition of ovulation rate in ewes, and impaired fertility in female mice.
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页码:151 / 159
页数:9
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