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一种α-肾上腺素能受体结合抑制剂的鉴定:对糖尿病的潜在影响

Identification of an alpha-adrenoceptor binding inhibitor: possible implications in diabetes mellitus.

作者信息

Wider M D, Dunbar J C, Duhaime P M

出版信息

Acta Diabetol Lat. 1985 Jul-Sep;22(3):263-9. doi: 10.1007/BF02590779.

Abstract

An endogenous adrenergic antagonist extracted from porcine duodenal mucosa was tested for 3H-yohimbine (5 nM) binding inhibitory activity using whole brain membranes. Duodenal mucosa was scraped into liquid N2 and extracted in 2M acetic acid (HAc) + 1 mg/ml ascorbic acid. The supernatant was fractionated on SP-Sephadex C-25 with a stepwise pH gradient. The peak adrenoceptor binding inhibitory (ABI) activity eluted at pH 4.5 and fractionation of this material on Sephadex G-25 SF indicated a relative molecular mass (Mr) of 2000 to 3000. The ABI did not bind to a Pharmacia Pro RPC 5/5 column which resulted in further purification and indicated that the peptide is hydrophilic. ABI activity was specific for 3H-yohimbine and did not affect 3H-dihydroalprenolol binding to beta receptors. Incubation of pancreatic islets isolated from fasted rats with ABI completely reversed the effect of 2.5 X 10(-6)M norepinephrine (NE) on insulin release in the presence of 300 mg/dl glucose. I.v. injection of ABI in rats also prevented the increased serum glucose response to a glucose bolus caused by NE. Preliminary experiments indicate that ABI blocks the stimulation of platelet aggregation by epinephrine as well. The peptide identified in this study causes specific inhibition of binding to alpha-2 adrenergic receptors and exerts a potent glucose dependent effect on adrenergic inhibition of insulin release. Possible implications in diabetes mellitus are discussed.

摘要

从猪十二指肠黏膜中提取的一种内源性肾上腺素能拮抗剂,利用全脑膜测试其对3H-育亨宾(5 nM)结合的抑制活性。将十二指肠黏膜刮入液氮中,并用2M乙酸(HAc)+1 mg/ml抗坏血酸进行提取。上清液在SP-葡聚糖凝胶C-25上以逐步pH梯度进行分级分离。肾上腺素能受体结合抑制(ABI)活性峰在pH 4.5时洗脱,将该物质在葡聚糖凝胶G-25 SF上进行分级分离表明其相对分子质量(Mr)为2000至3000。ABI不与Pharmacia Pro RPC 5/5柱结合,这使得进一步纯化成为可能,并表明该肽具有亲水性。ABI活性对3H-育亨宾具有特异性,并不影响3H-二氢心得舒与β受体的结合。用ABI孵育从禁食大鼠分离的胰岛,在存在300 mg/dl葡萄糖的情况下,完全逆转了2.5×10(-6)M去甲肾上腺素(NE)对胰岛素释放的影响。给大鼠静脉注射ABI也可防止由NE引起的静脉注射葡萄糖推注后血清葡萄糖反应的增加。初步实验表明,ABI也可阻断肾上腺素对血小板聚集的刺激。本研究中鉴定的该肽可特异性抑制与α-2肾上腺素能受体的结合,并对肾上腺素能抑制胰岛素释放发挥强大的葡萄糖依赖性作用。文中讨论了其在糖尿病中的可能意义。

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