胆囊收缩素的C末端八肽和[亮氨酸11]胃泌素-(5-17)在刺激离体兔胃腺酸分泌方面是否存在差异?
Are C-terminal octapeptide of cholecystokinin and [Leu11]gastrin-(5-17) different in stimulating acid secretion in isolated rabbit gastric glands?
作者信息
Oiry C, Galleyrand J C, Lima-Leite A C, Fulcrand P, Martinez J
机构信息
URA CNRS 1845,Faculte de Pharmacie, Universite de Montpellier I, France.
出版信息
Eur J Pharmacol. 1995 Dec 29;294(2-3):511-9. doi: 10.1016/0014-2999(95)00574-9.
In the present study we compared various CCK(B) receptor antagonists and tried to detect a difference in biological activity between the C-terminal octapeptides of cholecystokinin (CCK-8) and [Leu11]gastrin-(5-17) in isolated rabbit gastric glands. Binding experiments showed that different CCK(B)/gastrin receptor agonists bound with high affinity and that antagonists inhibited this binding in accordance with a CCK(B)/gastrin pharmacological profile. [Leu11]gastrin-(5-17), CCK-8 and cionin were found to induce [14C]aminopyrine accumulation to 25% above the basal level. Under the same experimental conditions, histamine induced a response twice as great as the response obtained with [Leu11]gastrin-(5-17) or CCK-8. [Leu11]gastrin-(5-17) (10(-7) M), CCK-8 (10(-8) M) and cionin (10(-8) M) appeared to be full agonists. CCK(B)/gastrin receptor antagonists including L-365,260 (3R-(+)-N-(2,3-dihydro-1-methyl-2-oxo-5-phenyl-1H-1,4-benzodiazepin++ +-3-yl)-N-(3-methylphenyl) urea), L-364,718 (3S-(-)-N-(2,3-dihydro-1-methyl-2-oxo-5-phenyl-1H-1,4-benzodiazepin++ +-3-yl)-1H-indole-2-carboximide) (a selective CCK(A) receptor antagonist), PD-135,158 (4([2-[[3-(1H-indol-3-yl)-2-methyl-1-oxo-2-[[[1.7.7-trimethyl-bicyclo[2. 2.1]hept-2-yl)oxy]carbonyl]amino]propyl]amino]-1-phenylethyl] amino-4-oxo-[1S-1alpha.2beta[S*(S*)]4alpha]]-butano nate N-methyl-D-glucamine) (bicyclo system 1S-endo), YM-022 ((R)-1-[2,3-dihydro-1-(2'-methylphenacyl)-2-oxo-5-phenyl-1H-1,4-++ +benzodiazepin-3-yl]-3-(3-methylphenyl)urea) and JMV-180 (Boc-Tyr(SO3H)-Nle-Gly-Trp-Nle-Asp-O-CH2-CH2-C6H5) exhibited the same profile for inhibition of [Leu11]gastrin-(5-17) or CCK-8-induced [14C]aminopyrine accumulation in rabbit gastric glands. These results suggested that [Leu11]gastrin-(5-17) and CCK-8 induced [14C]aminopyrine accumulation by the same mechanism. [Leu11]gastrin-(5-17)- or CCK-8-induced [14C]aminopyrine accumulation was inhibited by about 40% by the histamine H2 receptor blocker cimetidine. These results are consistent with there being cooperativity between [Leu11]gastrin-(5-17) (or CCK-8) and histamine in the acid secretory pathway. Similarly, the CCK(B)/gastrin receptor antagonists were tested against histamine-induced [14C]aminopyrine accumulation and surprisingly, only compound L-365,260 appeared active and even more potent than cimetidine.
在本研究中,我们比较了多种胆囊收缩素(CCK)(B)受体拮抗剂,并试图检测胆囊收缩素(CCK-8)的C末端八肽与[亮氨酸11]胃泌素-(5-17)在离体兔胃腺中的生物活性差异。结合实验表明,不同的CCK(B)/胃泌素受体激动剂具有高亲和力结合,且拮抗剂根据CCK(B)/胃泌素药理特性抑制这种结合。发现[亮氨酸11]胃泌素-(5-17)、CCK-8和西奥宁可诱导[14C]氨基比林积累至基础水平以上25%。在相同实验条件下,组胺诱导的反应是[亮氨酸11]胃泌素-(5-17)或CCK-8诱导反应的两倍。[亮氨酸11]胃泌素-(5-17)(10(-7)M)、CCK-8(10(-8)M)和西奥宁(10(-8)M)似乎是完全激动剂。包括L-365,260(3R-(+)-N-(2,3-二氢-1-甲基-2-氧代-5-苯基-1H-1,4-苯并二氮杂卓-3-基)-N-(3-甲基苯基)脲)、L-364,718(3S-(-)-N-(2,3-二氢-1-甲基-2-氧代-5-苯基-1H-1,4-苯并二氮杂卓-3-基)-1H-吲哚-2-甲酰胺)(一种选择性CCK(A)受体拮抗剂)、PD-135,158(4([2-[[3-(1H-吲哚-3-基)-2-甲基-1-氧代-2-[[[1.7.7-三甲基-双环[2.2.1]庚-2-基)氧基]羰基]氨基]丙基]氨基]-1-苯乙基]氨基-4-氧代-[1S-1α.2β[S*(S*)]4α]]-丁酸 N-甲基-D-葡糖胺)(双环系统1S-内型)、YM-022((R)-1-[2,3-二氢-1-(2'-甲基苯甲酰基)-2-氧代-5-苯基-1H-1,4-苯并二氮杂卓-3-基]-3-(3-甲基苯基)脲)和JMV-180(Boc-酪氨酸(SO3H)-Nle-甘氨酸-色氨酸-Nle-天冬氨酸-O-CH2-CH2-C6H5)对[亮氨酸11]胃泌素-(5-17)或CCK-8诱导的兔胃腺中[14C]氨基比林积累的抑制表现出相同的特性。这些结果表明,[亮氨酸11]胃泌素-(5-17)和CCK-8通过相同机制诱导[14C]氨基比林积累。[亮氨酸11]胃泌素-(5-17)或CCK-8诱导的[14C]氨基比林积累被组胺H2受体阻滞剂西咪替丁抑制约40%。这些结果与[亮氨酸11]胃泌素-(5-17)(或CCK-8)与组胺在酸分泌途径中存在协同作用一致。同样,测试了CCK(B)/胃泌素受体拮抗剂对组胺诱导的[14C]氨基比林积累的作用,令人惊讶的是,只有化合物L-365,260表现出活性,且比西咪替丁更有效。
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