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125I标记胰岛素在正常及链脲佐菌素诱导的糖尿病灌注大鼠心脏毛细血管内皮细胞膜和肌纤维细胞膜上的结合情况。

Binding of 125I-insulin on capillary endothelial and myofiber cell membranes in normal and streptozotocin-induced diabetic perfused rat hearts.

作者信息

Haddad R E, Jurjus A R, Ibrahim M Z, Nahle Z A, el-Kasti M M, Bitar K M, Kreydiyyeh S I, Saadeh F A, Bikhazi A B

机构信息

Department of Surgery, American University of Beirut, Lebanon.

出版信息

Comp Biochem Physiol A Physiol. 1997 Aug;117(4):523-30. doi: 10.1016/s0300-9629(96)00399-4.

Abstract

A heart-perfusion technique was employed to measure 125I-insulin binding on capillary endothelial and myocyte cell membranes in Sprague-Dawley rats. Animals were anesthetized, and the anterior chest wall excised to expose the mediastinal contents. The right and left superior and inferior venae cavae were dissected and tied, and another tie was passed around the aorta. A polyethylene catheter was introduced into the aortic lumen from cephalad to caudad to sit with its tip above the aortic valve. Another catheter was introduced into the cavity of the right atrium and both were anchored by sutures. Oxygenated Ringer-Lock buffer containing 20 mM/L K+ and 125I-insulin was perfused at a rate of 1 mL/min via the aortic catheter. Concomitantly, the distal ascending aorta and venae cavae were ligated. The effluent was collected from the right atrial catheter at the same infusion rate. Animals were divided into two groups, the normal group and streptozotocin-induced diabetic group. Heart perfusion was done on both groups either without or after treatment with detergent (CHAPS) to remove the capillary endothelial lining. A physical model for 125I-insulin sequestration as a ligand to its receptors on endothelial and/or myocyte plasma membranes was proposed. The model described a reversible binding of ligand on cellular surface receptor concentration to fit a conservation equation and a first order Bessel function. The binding constants (kn), reversal constants (k-n), dissociation constants kd = k-n/kn, and residency time constants tau = 1/k-n of 125I-insulin in normal untreated, normal CHAPS-treated, diabetic untreated, and diabetic CHAPS-treated hearts were estimated using a theoretically generated curve-fit to the data. Since insulin receptor binding on the capillary endothelial cell surfaces may serve to transport insulin from the intravascular to the subendothelial space, and since streptozotocin-induced diabetes was shown to diminish receptor autophosphorylation and kinase activity and hence internalization of insulin, then one can conclude the following from the data. In the normal heart, removal of the capillary endothelial lining with CHAPS did not alter kn, k-n, kd, and tau of insulin binding as compared to the normal untreated, whereas in the diabetic untreated heart these constants were altered, compared to the diabetic treated. Furthermore, the kn and k-n values in the diabetic CHAPS-treated hearts were the same as for the normals untreated and CHAPS-treated, respectively. In conclusion, the dissociation constants and residency time constants of all groups indicated the possible existence of two types of insulin receptors: the capillary endothelial cell surface insulin receptors with lower residency time (low affinity receptor or combination of insulin and IGF-1 receptors) and the myocyte plasma membrane insulin receptors with higher residency times (high affinity).

摘要

采用心脏灌注技术测量Sprague-Dawley大鼠毛细血管内皮细胞膜和心肌细胞膜上125I胰岛素的结合情况。将动物麻醉,切除前胸壁以暴露纵隔内容物。解剖并结扎左右上下腔静脉,在主动脉周围再扎一道。从头部向尾部将一根聚乙烯导管插入主动脉腔,使其尖端位于主动脉瓣上方。另一根导管插入右心房腔,两根导管均用缝线固定。含20 mM/L K+和125I胰岛素的氧合林格氏液缓冲液以1 mL/min的速度通过主动脉导管灌注。同时,结扎升主动脉远端和腔静脉。以相同的输注速率从右心房导管收集流出液。动物分为两组,正常组和链脲佐菌素诱导的糖尿病组。两组均在不使用去污剂(CHAPS)或使用去污剂处理以去除毛细血管内皮内衬后进行心脏灌注。提出了一个125I胰岛素作为配体与内皮和/或心肌细胞质膜上受体结合的物理模型。该模型描述了配体在细胞表面受体浓度上的可逆结合,以符合守恒方程和一阶贝塞尔函数。使用理论生成的曲线拟合数据估计正常未处理、正常CHAPS处理、糖尿病未处理和糖尿病CHAPS处理心脏中125I胰岛素的结合常数(kn)、逆转常数(k-n)、解离常数kd = k-n/kn和驻留时间常数tau = 1/k-n。由于胰岛素在毛细血管内皮细胞表面的受体结合可能有助于将胰岛素从血管内转运到内皮下空间,并且由于链脲佐菌素诱导的糖尿病显示会降低受体自磷酸化和激酶活性,从而降低胰岛素的内化,那么从这些数据可以得出以下结论。在正常心脏中,与正常未处理组相比,用CHAPS去除毛细血管内皮内衬不会改变胰岛素结合的kn、k-n、kd和tau,而在糖尿病未处理心脏中,与糖尿病处理组相比,这些常数会发生改变。此外,糖尿病CHAPS处理心脏中的kn和k-n值分别与正常未处理和CHAPS处理组相同。总之,所有组的解离常数和驻留时间常数表明可能存在两种类型的胰岛素受体:驻留时间较短的毛细血管内皮细胞表面胰岛素受体(低亲和力受体或胰岛素与IGF-1受体的组合)和驻留时间较长的心肌细胞质膜胰岛素受体(高亲和力)。

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