The characteristics of a high-affinity antagonist radioligand are compared with those a high-affinity agonist in binding to the cloned corticotropin-releasing factor receptor type 1 (CRF-RI) and type 2 (CRF-R2) and to the native receptors that exist in rat cerebellum and brain stem. The relative potencies of CRF antagonists and agonists to the two types of cloned CRF receptors overexpressed stably in Chinese hamster ovary cells are determined using the antagonist radioligand I-125-[DTyr(1)]astressin (Ast*), and the agonist radioligand, I-125-[Tyr]rat urocortin (Ucn*). The inhibitory binding constants (K-i) of astressin and urocortin are 1 to 2 nM for all receptors and are independent of which radioligand is employed. Astressin binds with high affinity to the native cerebellar/brain stem receptor and relative potencies of selected CRF analogs determined with Ast* on the native receptor are similar to those obtained for the cloned CRF-R1. The specific binding of Ast* to endogenous brain receptors is greater than that of Ucn*, resulting in more sites being detected by the antagonist than by the agonist. In contrast to another CRF agonist, the binding of Ucn* to the cloned receptors is relatively insensitive to guanyl nucleotides at both 20 degrees C and 37 degrees C; however, its binding to the native receptor is displaced by guanyl nucleotides at 37 degrees C and, to a lesser degree, at 20 degrees C. As expected, the binding of the antagonist Ast* is not affected by guanyl nucleotides. Because it is a high-affinity, specific CRF antagonist, astressin is eminently suitable as a ligand for detection and characterization of both endogenous and cloned CRF receptors.
机构:
Eli Lilly & Co, Lilly Corp Ctr, Lilly Res Labs, Div Neurosci, Indianapolis, IN 46285 USAEli Lilly & Co, Lilly Corp Ctr, Lilly Res Labs, Div Neurosci, Indianapolis, IN 46285 USA
Sajdyk, TJ
Gehlert, DR
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Eli Lilly & Co, Lilly Corp Ctr, Lilly Res Labs, Div Neurosci, Indianapolis, IN 46285 USAEli Lilly & Co, Lilly Corp Ctr, Lilly Res Labs, Div Neurosci, Indianapolis, IN 46285 USA
机构:Jikei Univ, Dept Mol Cell Biol, Sch Med, Inst DNA Med,Minato Ku, Tokyo 1058461, Japan
Kamada, Minori
Ikeda, Keiichi
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Jikei Univ, Dept Mol Cell Biol, Sch Med, Inst DNA Med,Minato Ku, Tokyo 1058461, JapanJikei Univ, Dept Mol Cell Biol, Sch Med, Inst DNA Med,Minato Ku, Tokyo 1058461, Japan
Ikeda, Keiichi
Fujioka, Kouki
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Jikei Univ, Dept Mol Cell Biol, Sch Med, Inst DNA Med,Minato Ku, Tokyo 1058461, JapanJikei Univ, Dept Mol Cell Biol, Sch Med, Inst DNA Med,Minato Ku, Tokyo 1058461, Japan
Fujioka, Kouki
Akiyama, Noibutake
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Jikei Univ, Inst DNA Med, Sch Med, Dept Mol Immunol,Minato Ku, Tokyo 1058461, JapanJikei Univ, Dept Mol Cell Biol, Sch Med, Inst DNA Med,Minato Ku, Tokyo 1058461, Japan
Akiyama, Noibutake
Akiyoshi, Kouhei
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Jikei Univ, Dept Mol Cell Biol, Sch Med, Inst DNA Med,Minato Ku, Tokyo 1058461, JapanJikei Univ, Dept Mol Cell Biol, Sch Med, Inst DNA Med,Minato Ku, Tokyo 1058461, Japan
Akiyoshi, Kouhei
Inoue, Yuriko
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Toho Univ, Dept Anat, Sch Med, Fac Med,Oto Ku, Tokyo, JapanJikei Univ, Dept Mol Cell Biol, Sch Med, Inst DNA Med,Minato Ku, Tokyo 1058461, Japan
Inoue, Yuriko
Hanada, Sanshiro
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Natl Ctr Global Hlth & Med, Res Inst, Vice Director Gen Lab, Shinjuku Ku, Tokyo, JapanJikei Univ, Dept Mol Cell Biol, Sch Med, Inst DNA Med,Minato Ku, Tokyo 1058461, Japan
Hanada, Sanshiro
Yamamoto, Kenji
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Natl Ctr Global Hlth & Med, Res Inst, Vice Director Gen Lab, Shinjuku Ku, Tokyo, JapanJikei Univ, Dept Mol Cell Biol, Sch Med, Inst DNA Med,Minato Ku, Tokyo 1058461, Japan
Yamamoto, Kenji
Tojo, Katsuyoshi
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Jikei Univ, Div Diabet & Endocrinol, Sch Med, Dept Internal Med,Minato Ku, Tokyo 1058461, JapanJikei Univ, Dept Mol Cell Biol, Sch Med, Inst DNA Med,Minato Ku, Tokyo 1058461, Japan
Tojo, Katsuyoshi
Manome, Yoshinobu
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Jikei Univ, Dept Mol Cell Biol, Sch Med, Inst DNA Med,Minato Ku, Tokyo 1058461, Japan
Jikei Univ, Core Res Facil, Sch Med, Res Ctr Med Sci,Minato Ku, Tokyo 1058461, JapanJikei Univ, Dept Mol Cell Biol, Sch Med, Inst DNA Med,Minato Ku, Tokyo 1058461, Japan