[LEU31-PRO34] NEUROPEPTIDE-Y IDENTIFIES A SUBTYPE OF I-125 LABELED PEPTIDE-YY BINDING-SITES IN THE RAT-BRAIN

被引:67
作者
GEHLERT, DR
GACKENHEIMER, SL
SCHOBER, DA
机构
[1] Central Nervous System Research, Lilly Research Laboratories, Eli Lilly and Company, Indianapolis
关键词
D O I
10.1016/0197-0186(92)90067-2
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Subtypes of the neuropeptide Y (NPY) receptor in the rat brain were identified by the use of the selective Y-1 analog, [Leu31-Pro34] NPY. In rat brain homogenate binding studies, [Leu31-Pro34] NPY was found to produce a partial inhibition of 100 pM I-125-labeled peptide YY (PYY) binding with a plateau at 50-1000 nM [Leu31-Pro34] NPY resulting in a 70% inhibition of binding. The C-terminal fragment NPY 13-36, a putative Y-2 agonist, exhibited very little selectivity in rat brain homogenates. Scatchard analysis of I-125-labeled PYY binding to rat brain homogenate yielded biphasic plots with K(d) values of 40 and 610 pM. Inclusion of 100 nM [Leu31-Pro34] NPY was found to eliminate the low affinity component of I-125 labeled PYY binding leaving a single, high affinity binding site with a K(d) of 68 pM. In autoradiographic studies. displacement curves indicated that [Leu31-Pro34] NPY completely inhibited binding in the cerebral cortex with little effect on the binding in the hypothalamus. On the other hand NPY 13-36 inhibited binding in the hypothalamus at low concentrations but required higher concentrations to inhibit binding in the cerebral cortex. Other brain regions such as the hippocampus, appeared to contain both subtypes. Subsequent to these studies, a quantitative autoradiographic map was conducted using 50-100 pM I-125-labeled PYY in the presence and absence of [LeU31-Pro34] NPY which produced a selective displacement of binding in certain distinct brain regions. These areas included the cerebral cortex, certain thalamic nuclei and brainstem while ligand binding was retained in other brain regions including the zona lateralis of the substantia nigra, lateral septum nucleus of the solitary tract and the hippocampus. Numerous brain regions appeared to contain both receptor subtypes. Therefore, the Y-1 and Y-2 receptor subtypes exhibited a somewhat distinct distribution in the brain. In addition. I-125-labeled PYY appears to label the Y-2 receptor with relatively higher affinity when compared to the Y-1 receptor.
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页码:45 / 67
页数:23
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