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一种针对咪唑克生的抗血清可识别出人类血清和脑脊液中的一种免疫反应性物质,该物质并非胍丁胺。

An antiserum to idazoxan recognizes an immunoreactive substance in human serum and cerebral spinal fluid which is not agmatine.

作者信息

Wang H, Regunathan S, McGowan D, Bramwell S, Reis D J

机构信息

Department of Neurology and Neuroscience, Cornell University Medical College, New York, NY 10021, USA.

出版信息

Neurochem Int. 1997 Jan;30(1):85-94. doi: 10.1016/s0197-0186(96)00041-1.

Abstract

A polyclonal antibody was generated in rabbits to an idazoxan-albumin antigen. The anti-idazoxan antiserum had high affinity for unconjugated 3H-idazoxan (Kd of 19.8 nM) in a radio-immunoassay (RIA). Of various drugs and native molecules only idazoxan potently (Ki of 24 nM) inhibited 3H-idazoxan binding to the anti-idazoxan antibody. A few drugs weakly inhibited 3H-idazoxan binding (IC50 > 605 microM) with rank order of UK 14304 > guanabenz > cirazoline > amiloride > naphazoline. Neither agmatine, an endogenous clonidine displacing substance (CDS), catecholamines or imidazoles inhibited the binding of 3H-idazoxan to the anti-idazoxan antibody. The anti-idazoxan RIA was 4-6 fold more sensitive than an antibody to para-amino clonidine. The CDS detected by ligand displacement from bovine brain dose-dependently inhibited 3H-idazoxan binding. This immunoreactive (ir-) CDS activity was present in human (0.9-4.1 U/ml) and rat sera (1-2 U/ml) and in the cerebro-spinal fluid of eight patients with serious disease of the central nervous system, but not in controls. We conclude: (1) an anti-idazoxan RIA is a sensitive, selective and clinically applicable RIA for measuring ir-CDS; (2) ir-CDS is not agmatine; (3) CDS represents a family of endogenous ligands for imidazoline receptors including ir-CDS and agmatine.

摘要

用一种咪唑克生 - 白蛋白抗原在兔体内产生了多克隆抗体。在放射免疫分析(RIA)中,抗咪唑克生抗血清对未结合的3H - 咪唑克生具有高亲和力(解离常数Kd为19.8 nM)。在各种药物和天然分子中,只有咪唑克生能有效抑制(抑制常数Ki为24 nM)3H - 咪唑克生与抗咪唑克生抗体的结合。少数药物对3H - 咪唑克生结合有弱抑制作用(半数抑制浓度IC50>605 μM),其抑制强度顺序为UK 14304>胍那苄>可乐定>阿米洛利>萘甲唑啉。内源性可乐定置换物质(CDS)胍丁胺、儿茶酚胺或咪唑类均不抑制3H - 咪唑克生与抗咪唑克生抗体的结合。抗咪唑克生RIA比抗对氨基可乐定抗体灵敏4 - 6倍。通过从牛脑中置换配体检测到的CDS剂量依赖性地抑制3H - 咪唑克生结合。这种免疫反应性(ir - )CDS活性存在于人类血清(0.9 - 4.1 U/ml)和大鼠血清(1 - 2 U/ml)以及8例患有严重中枢神经系统疾病患者的脑脊液中,而对照组中未检测到。我们得出结论:(1)抗咪唑克生RIA是一种灵敏、特异且适用于临床的用于测量ir - CDS的RIA;(2)ir - CDS不是胍丁胺;(3)CDS代表了一类咪唑啉受体的内源性配体家族,包括ir - CDS和胍丁胺。

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