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Analysis of the CCKB receptor antagonism of virginiamycin in guinea-pig ileum longitudinal myenteric plexus.

机译:维吉尼亚霉素对豚鼠回肠纵向肌层神经丛的CCKB受体拮抗作用的分析。

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摘要

1. Virginiamycin, a macrolide reported to bind selectively to CCKB/gastrin receptors has been studied in a functional test, namely cholecystokinin-induced contraction of guinea-pig ileum myenteric plexus (LMMP). 2. Virginiamycin (1-10 microM) antagonized the selective CCKB agonist cholecystokinin tetrapeptide (CCK-4). The antagonism appeared not to be competitive as the highest concentration (10 microM) caused a reduction of its maximal effect. An apparent pA2 of 6.64 +/- 0.06 (s.e.) could be estimated if this depression was ignored. The selective CCKB antagonist, L-365,260 (0.01-0.3 microM) antagonized competitively the CCK-4 induced contraction and a pKB of 8.60 +/- 0.16 (s.e.) was estimated. 3. The combined dose-ratio analysis for virginiamycin, tested at 3 and 10 microM in association with 0.03 and 0.1 microM L-365,260, respectively, resulted in observed log dose-ratios of 1.39 and 1.53. That was consistent with both antagonists acting on the same receptor in LMMP. 4. These data, represent the first evidence of the antagonism of virginiamycin in a functional assay and they support the hypothesis of homogeneity between CCKB receptors in the CNS and in peripheral tissues.
机译:1.在功能测试中,即胆囊收缩素诱导的豚鼠回肠肌层神经丛(LMMP)的收缩性研究中,研究了弗吉尼亚霉素,一种据报道与CCKB /胃泌素受体选择性结合的大环内酯。 2.弗吉尼亚霉素(1-10 microM)拮抗选择性CCKB激动剂胆囊收缩素四肽(CCK-4)。拮抗作用似乎没有竞争力,因为最高浓度(10 microM)导致其最大作用降低。如果忽略这种压抑,可以估计出6.64 +/- 0.06(s.e.)的表观pA2。选择性CCKB拮抗剂L-365,260(0.01-0.3 microM)竞争性拮抗CCK-4诱导的收缩,估计pKB为8.60 +/- 0.16(s.e.)。 3.分别以3和10 microM分别与0.03和0.1 microM L-365,260联合测试的维吉尼亚霉素的剂量比综合分析得出的对数剂量比为1.39和1.53。这与作用于LMMP中同一受体的两种拮抗剂一致。 4.这些数据代表了维吉尼亚霉素在功能测定中具有拮抗作用的第一个证据,它们支持中枢神经系统和周围组织中CCKB受体之间同质性的假设。

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