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J. Biol. Chem., Vol. 268, Issue 29, 21613-21617, 10, 1993
C Liu, KE Roth, BA Shepard, JB Shaffer and JA Dias
Residues Phe33 and Arg35, individually, and a composite mutation of
residues Arg42, Ser43, and Lys44 were changed to alanine in the human
glycoprotein hormone common alpha-subunit using site-directed mutagenesis.
These specific residues are highly conserved across species and have by
chemical modification and synthetic peptide approaches been implicated in
the binding of human chorionic gonadotropin (hCG) to leutinizing hormone
(LH) receptor. In the present study we tested the hypothesis that specific
alpha-subunit amino acid residues which stabilize the hormone receptor
interaction for hCG have the same function in human follicle-stimulating
hormone (hFSH). Wild type or mutant alpha-subunit cDNAs were coexpressed
with wild type hFSH or hCG beta cDNA in sialylation defective Chinese
hamster ovary cells. Recombinant hormones were tested in a radioligand
receptor competition assay, using rat testis membranes as a source of FSH
and LH receptors. Mutant hFSH heterodimers F33A-FSH, R35A-FSH,
Arg42-Ser43-Lys44/Ala42- Ala43-Ala44- FSH all displaced 125I-hFSH in a
similar fashion, indicating that these residues are not important for
binding of hFSH to the rat FSH receptor. On the other hand, F33A-CG
evidenced a 5-fold decrease in binding, while R35A-CG had over a 100-fold
decrease in binding to the rat LH receptor when compared to the wild type
recombinant hCG. These data demonstrate that a receptor-binding site on the
common alpha-subunit which is very important for hCG binding to LH receptor
is not important for the binding of hFSH to FSH receptor. Our
interpretation of these findings is that there are fundamental structural
differences in the receptor interface contacts of the common alpha-subunit,
which stabilize receptor binding among members of the glycoprotein hormone
family.
Site-directed alanine mutagenesis of Phe33, Arg35, and Arg42-Ser43- Lys44 in the human gonadotropin alpha-subunit
School of Public Health, Department of Biomedical Sciences, State University New York, Albany 12201.
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