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大鼠和家兔肾单位中的心房利钠肽受体:[125I]α-大鼠心房利钠肽在显微解剖的肾小球和肾小管中的结合。

Atrial natriuretic peptide receptors along the rat and rabbit nephrons: [125I] alpha-rat atrial natriuretic peptide binding in microdissected glomeruli and tubules.

作者信息

Butlen D, Mistaoui M, Morel F

出版信息

Pflugers Arch. 1987 Apr;408(4):356-65. doi: 10.1007/BF00581129.

Abstract

Binding of [125I] alpha-rat atrial natriuretic peptide ([125I] alpha-RANP) was measured in glomeruli and pieces of tubule microdissected from rat and rabbit nephrons. High densities of specific ANP binding sites were found only in the glomeruli (10-30 X 10(-18) mol X glom-1), whereas no specific binding could be detected in the proximal tubule, the thin segments of the Henle's loop, the thick ascending limb, the distal tubule and the cortical and outer medullary collecting tubules. Rising the temperature from 4 degrees C to 35 degrees C resulted in biphasic kinetics of binding, suggesting a temperature-dependent inactivation of labelled hormone by glomeruli. At 4 degrees C, specific binding of [125I] alpha-RANP was time and dose-dependent and Scatchard analysis of data indicated an apparent equilibrium dissociation constant of 0.63 nM. Competition experiments revealed the following sequence of stereospecificity for binding to rat glomeruli: RANP 3-28 greater than [125I] alpha-RANP = [125I] alpha-HANP = alpha-RANP = antriopeptin III greater than antriopeptin II, whereas binding was unaffected by pharmacological doses of unrelated peptide hormones, prostaglandins, adrenergic agonists, dopamine, histamine and carbamylcholine. The results indicate that glomerular binding sites might be the physiological ANP receptors.

摘要

在从大鼠和兔肾单位显微解剖得到的肾小球和肾小管片段中,测定了[125I]α-大鼠心房利钠肽([125I]α-RANP)的结合情况。仅在肾小球中发现了高密度的特异性ANP结合位点(10 - 30×10(-18)摩尔×肾小球-1),而在近端小管、亨氏袢细段、髓袢升支粗段、远端小管以及皮质和外髓集合小管中未检测到特异性结合。将温度从4℃升高到35℃导致结合呈现双相动力学,提示肾小球对标记激素有温度依赖性失活作用。在4℃时,[125I]α-RANP的特异性结合具有时间和剂量依赖性,对数据进行Scatchard分析表明表观平衡解离常数为0.63 nM。竞争实验揭示了与大鼠肾小球结合的立体特异性顺序如下:RANP 3 - 28>[125I]α-RANP = [125I]α-HANP = α-RANP = 抗利尿肽III>抗利尿肽II,而与药理学剂量的无关肽激素、前列腺素、肾上腺素能激动剂、多巴胺、组胺和氨甲酰胆碱的结合不受影响。结果表明肾小球结合位点可能是生理性ANP受体。

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