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犬肾中假定的ETB受体亚型的鉴定及功能

Identification and function of putative ETB receptor subtypes in the dog kidney.

作者信息

Brooks D P, DePalma P D, Pullen M, Gellai M, Nambi P

机构信息

Department of Renal Pharmacology, SmithKline Beecham Pharmaceuticals, King of Prussia, Pennsylvania 19406-0939, USA.

出版信息

J Cardiovasc Pharmacol. 1995;26 Suppl 3:S322-5.

PMID:8587403
Abstract

Binding studies performed in dog kidney, lung, and spleen using [125I]endothelin (ET) 3 and a series of ETB-selective ligands indicated the presence of two subtypes of ETB receptors, an IRL-1620-sensitive (putative ETB1) and an IRL-1620-insensitive (putative ETB2) receptor. The IRL-1620-sensitive (but not IRL-1620-insensitive) ETB receptors displayed similar pharmacology to the cloned human ETB receptor and a high affinity for the ETB receptor antagonist RES-701. ETB1 receptors predominated in the dog kidney and lung and ETB2 receptors predominated in the dog spleen. Stimulation of ETB receptors in dogs in vivo inhibited sodium reabsorption, as ET-1 infusion in the presence of the ETA antagonist BQ123, but not the mixed ETA/ETB receptor antagonist, (+/-)SB 209670, resulted in increased sodium excretion. Furthermore, infusion of the ETB-selective agonist Sarafotoxin S6c (S6c) resulted in an increase in sodium excretion, a response that was attenuated by infusion of RES-701. These data indicate that the putative ETB1 receptor may mediate ET-induced inhibition of tubule sodium reabsorption in the dog. In addition, we observed no putative ETB2 receptor-mediated renal vasoconstriction, consistent with the apparent low abundance of this subtype in the dog kidney.

摘要

使用[125I]内皮素(ET)3和一系列ETB选择性配体在犬肾、肺和脾中进行的结合研究表明存在两种ETB受体亚型,一种对IRL-1620敏感(推定的ETB1)和一种对IRL-1620不敏感(推定的ETB2)受体。对IRL-1620敏感(但对IRL-1620不敏感)的ETB受体表现出与克隆的人ETB受体相似的药理学特性,并且对ETB受体拮抗剂RES-701具有高亲和力。ETB1受体在犬肾和肺中占主导地位,而ETB2受体在犬脾中占主导地位。在体内刺激犬的ETB受体可抑制钠重吸收,因为在ETA拮抗剂BQ123存在下输注ET-1,但混合的ETA/ETB受体拮抗剂(+/-)SB 209670不会导致钠排泄增加。此外,输注ETB选择性激动剂铃蟾毒素S6c(S6c)导致钠排泄增加,该反应被输注RES-701减弱。这些数据表明推定的ETB1受体可能介导ET诱导的犬肾小管钠重吸收抑制。此外,我们未观察到推定的ETB2受体介导的肾血管收缩,这与该亚型在犬肾中明显低丰度一致。

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