1. Author's Information
    Z Georgoussi
    Institute of Biology, National Centre of Scientific Research ‘Demokritos’, 153 10 Ag. Paraskevi, P.O. Box 60228, Athens, Greece

    G Milligan
    Molecular Pharmacology Group, Departments of Biochemistry and Pharmacology, University of Glasgow, Glasgow G12 8QQ, Scotland, U.K.

    C Zioudrou
    Institute of Biology, National Centre of Scientific Research ‘Demokritos’, 153 10 Ag. Paraskevi, P.O. Box 60228, Athens, Greece

  2. Abstract
    Solubilization of opioid receptors from rat cortical membranes that retained high-affinity guanine nucleotide-sensitive agonist binding was achieved using 10 mM CHAPS. We report the nature of the interactions of mu and delta opioid receptors with the guanine nucleotide-binding protein G(o) by immunoprecipitation of CHAPS extracts with selective G(o)alpha-subunit protein antisera. Antiserum IM1 raised against amino acids 22-35 of G(o)alpha selectively co-immunoprecipitated G(o)alpha-mu and G(o)alpha-delta opioid receptor complexes detected in the immunoprecipitates by specific [3H][D-Ala2,N-Me-Phe4,Gly5-ol]enkephalin and [3H][D-Ser2,Leu5,Thr6]enkephalin binding respectively. By contrast, antisera directed against the C-terminal decapeptide (OC2) and the N-terminal hexadecapeptide (ON1) of isoforms of G(o)alpha were unable to immunoprecipitate solubilized opioid receptor-G(o) complexes, although both were able to immunoprecipitate solubilized G(o)alpha and have been shown to reduce the affinity of [D-Ala2,D-Leu5]enkephalin for opioid receptors in rat cortical membranes [Georgoussi, Carr and Milligan (1993) Mol. Pharmacol. 44, 62-69]. These findings demonstrate that CHAPS-solubilized mu and delta opioid receptors from rat cortical membranes form stable complexes with one or more variants of G(o).
    Keywords
    receptor-Go-protein, GTP-binding-protein antisera, N-terminal hexadecapeptide

    ADLID: 76703-v4
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  1. Keywords
    receptor-Go-protein GTP-binding-protein antisera N-terminal hexadecapeptide
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