Besson J, Malassiné A, Ferré F
U.55 INSERM, Hôpital Saint-Antoine, Paris, France.
Regul Pept. 1987 Nov;19(3-4):197-207. doi: 10.1016/0167-0115(87)90276-x.
The presence of vasoactive intestinal peptide (VIP) binding sites and the adenylate cyclase activity in response to VIP were examined in the human term placenta. Slices were used in order to preserve the physicochemical environment and the structural integrity of this heterogeneous organ. 125I-VIP binding to placental slices was saturable. The steady state was reached after 90 min at 37 degrees C and was maintained up to 3 h. Unlabeled VIP was able to compete in a dose-dependent manner with an IC50 value of 5.2 +/- 1.3 x 10(-10) M. Autoradiography and histological analysis showed that VIP binding sites were essentially located on fetal vascularization, especially arteries of stem villi. VIP produced a stimulatory effect on cAMP synthesis at a concentration as low as 10(-10) M. The dose-response curve was monophasic with an ED50 value of 2.9 +/- 1.6 x 10(-9) M. The specificity of the VIP effect was tested with peptides structurally related to VIP such as glucagon, secretin, gastric inhibitory polypeptide and human growth-hormone releasing factor. Only secretin at high concentrations (greater than 10(-6) M) increased cAMP production. Leu-enkephalin or insulin were ineffective. The presence of both VIP binding sites on fetal vascularization and VIP-induced adenylate cyclase activation would seem to suggest a regulatory role of the peptide on fetoplacental blood flow.
研究了人足月胎盘血管活性肠肽(VIP)结合位点的存在情况以及对VIP的腺苷酸环化酶活性。为保留这个异质性器官的物理化学环境和结构完整性,使用了胎盘切片。125I-VIP与胎盘切片的结合具有饱和性。在37℃下90分钟后达到稳态,并维持长达3小时。未标记的VIP能够以剂量依赖的方式竞争,IC50值为5.2±1.3×10(-10)M。放射自显影和组织学分析表明,VIP结合位点主要位于胎儿血管,尤其是绒毛干的动脉上。VIP在低至10(-10)M的浓度下对cAMP合成产生刺激作用。剂量反应曲线是单相的,ED50值为2.9±1.6×10(-9)M。用与VIP结构相关的肽如胰高血糖素、促胰液素、胃抑制多肽和人生长激素释放因子测试了VIP作用的特异性。只有高浓度(大于10(-6)M)的促胰液素会增加cAMP的产生。亮脑啡肽或胰岛素无效。胎儿血管上存在VIP结合位点以及VIP诱导的腺苷酸环化酶激活似乎表明该肽对胎儿-胎盘血流具有调节作用。
