SR121463是一种选择性非肽抗利肌加压素V2受体拮抗剂

C. S. Gal
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引用次数: 60

摘要

SR121463是一种选择性的、口服活性的抗利肌加压素(AVP) v2受体的非肽拮抗剂,在多种动物和人类中具有强大的水生特性。SR121463属于一种被称为aquaretics的新型药物,它能够在不影响电解质平衡的情况下诱导自由水排泄。SR121463对动物和人类v2受体具有高亲和力,并具有显著的选择性v2受体谱。因此,SR121463和[3 H]SR121463被用作表征和标记v2受体的选择性探针。在各种体外功能研究中,SR121463表现为一种有效的拮抗剂。抑制avp刺激的人肾腺苷酸环化酶和dDAVP(1-去氨基,8-D精氨酸-加压素)诱导的大鼠主动脉舒张。SR121463在表达组成型激活的人v2受体突变体的细胞中也可以作为一种逆激动剂。在体外,SR121463通过增加细胞表面表达和恢复v2功能来拯救错误折叠的v2 AVP受体突变体。在正常补水意识的大鼠、狗和猴子中,SR121463通过静脉注射或口服给药,诱导了剂量依赖性脱水,而尿Na +和K +排泄没有重大变化(与传统利尿剂不同)。在有腹水和肾功能受损的肝硬化大鼠中,用SR121463治疗10天,完全纠正了低钠血症,恢复了正常的尿排泄。在糖尿病肾病大鼠模型中,SR121463强烈减少白蛋白排泄。SR121463在体外和体内对参与血管松弛或凝血因子释放的肾外v2(或v2样)受体也有效。在兔高眼压模型中,SR121463单次或多次滴注均可降低眼压。在大鼠、狗或健康的人类志愿者急性和慢性给药后,SR121463被很好地吸收和耐受。在所研究的所有物种中,该药物产生明显的失水作用,而没有任何激动剂作用。因此,SR121463是一种有效的、口服活性的、选择性的v2受体拮抗剂,具有强大的水系特性。它是进一步探讨肾或肾外v2受体功能的有用工具。纯v2受体拮抗剂可能用于治疗几种保水性疾病,如低钠血症、抗利尿激素分泌不当综合征(SIADH)、充血性心力衰竭、肝硬化和其他可能由v2受体介导的疾病(如青光眼)。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
An overview of SR121463, a selective non-peptide vasopressin V2 receptor antagonist
SR121463 is a selective, orally active, non-peptide antagonist of vasopressin (AVP) V 2 receptors with powerful aquaretic properties in various animal species and humans. SR121463 belongs to a new class of drugs, called aquaretics, which are capable of inducing free-water excretion without affecting electrolyte balance. SR121463 displays high affinity for animal and human V 2 receptors and exhibits a remarkably selective V 2 receptor profile. SR121463 and [ 3 H]SR121463 are used, therefore, as selective probes for characterization and labeling of V 2 receptors. In various functional studies in vitro, SR121463 behaves as a potent antagonist. It inhibits AVP-stimulated human renal adenylyl cyclase and dDAVP (1-desamino, 8-D arginine-vasopressin)-induced relaxation of rat aorta. SR121463 also behaves as an inverse agonist in cells expressing a constitutively activated human V 2 receptor mutant. In vitro, SR121463 rescued misfolded V 2 AVP receptor mutants by increasing cell surface expression and restoring V 2 function. In normally hydrated conscious rats, dogs and monkeys, SR121463, by either i.v. or p.o. administration, induced a dose-dependent aquaresis with no major changes in urinary Na + and K + excretion (unlike classical diuretics). In cirrhotic rats with ascites and impaired renal function, a 10-day treatment with SR121463 totally corrected hyponatremia and restored normal urine excretion. In a model of diabetic nephropathy in rats, SR121463 strongly reduced albumin excretion. SR121463 was also effective at extrarenal V 2 (or V 2 -like) receptors involved in vascular relaxation or clotting factor release in vitro and in vivo. In the rabbit model of ocular hypertension, SR121463 by either single or repeated instillation, decreased intraocular pressure. After acute and chronic administration to rats, dogs or healthy human volunteers, SR121463 was well absorbed and well tolerated. In all species studied the drug produced pronounced aquaresis without any agonist effect. Thus, SR121463 is a potent, orally active and selective antagonist at V 2 receptors with powerful aquaretic properties. It is a useful tool for further exploration of function of renal or extrarenal V 2 receptors. Pure V 2 receptor antagonists are likely to be therapeutically useful in several water-retaining diseases such as hyponatremia, Syndrome of Inappropriate Antidiuretic Hormone secretion (SIADH), congestive heart failure, liver cirrhosis, and other disorders possibly mediated by V 2 receptors (e.g., glaucoma).
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