Pharmacological characterization of YM087, a potent, nonpeptide human vasopressin V1A and V2 receptor antagonist

Tahara, Atsuo; Saito, Masayuki; Sugimoto, Toru; Tomura, Yuichi; Wada, Koh-ichi; Kusayama, Toshiyuki; Tsukada, Junko; Ishii, Noe; Yatsu, Takeyuki; Uchida, Wataru; Tanaka, Akihiro

doi:10.1007/pl00005139

Cited by 80 publications

(101 citation statements)

References 26 publications

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“…which is administered intravenously; in 2009, tolvaptan, an oral agent, was approved. 21,22 It is important to note that much of the clinical experience with these agents comes from use in patients with more common causes of hyponatremia, such as chronic heart failure. 7 Adverse effects of conivaptan include infusion site reactions, nausea and vomiting, and diarrhea.…”

Section: Paraneoplastic Endocrine Syndromesmentioning

confidence: 99%

Paraneoplastic Syndromes: An Approach to Diagnosis and Treatment

Pelosof

Gerber

2010

Mayo Clinic Proceedings

567

514

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Section: Paraneoplastic Endocrine Syndromesmentioning

confidence: 99%

Paraneoplastic Syndromes: An Approach to Diagnosis and Treatment

Pelosof

Gerber

2010

Mayo Clinic Proceedings

567

514

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“…With respect to the low dissociation constant, NOX-F37 might be even more effective in inhibiting AVP signaling via the V 1a receptor than the receptor antagonist conivaptan. For conivaptan, a K i of 6.3 nM has been reported (44). Moreover, the IC 50 value in a cell culture assay is higher for conivaptan (44) than for NOX-F37 (14.3 nM vs. 6.1 nM), which is further strengthened by the fact that the IC 50 of NOX-F37 was determined in an Ϸ4-fold less-sensitive cell assay (EC 50 Ϸ 5 nM) compared with conivaptan (EC 50 Ϸ 1.3 nM; ref.…”

Section: Discussionmentioning

confidence: 99%

An l -RNA-based aquaretic agent that inhibits vasopressin in vivo

Purschke

Eulberg

Buchner

et al. 2006

Proc. Natl. Acad. Sci. U.S.A.

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A class of diuretic͞aquaretic agents based on mirror-image oligonucleotides (so-called Spiegelmers) has been identified. These molecules directly bind and inhibit the neuropeptide vasopressin (AVP). AVP is the major regulatory component of body fluid homeostasis mediated through binding to the renal V2 receptor. Elevated plasma levels of AVP are implicated in several pathological conditions, mainly cardiovascular diseases. In congestive heart failure, AVP is part of a neuroendocrine imbalance that is responsible for progressive worsening of the disease. Employing in vitro selection techniques, RNA aptamers that bind to the unnatural D-configuration of AVP were isolated. The best aptamer displayed an affinity to D-AVP of Ϸ560 pM at 37°C. The corresponding Spiegelmer, a 38-mer mirror-image oligonucleotide (L-RNA) termed NOX-F37, inhibits vasopressin-dependent activation of V1a as well as V2 receptors with IC50 values of 6.1 nM and 1 nM, respectively. NOX-F37 administered to healthy rats effectively neutralized AVP and increased diuresis dose-dependently for 24 h. The mode of action was strictly aquaretic, i.e., the increase in urine volume was not accompanied by an increase in electrolytes. These results clearly prove the in vivo efficacy of NOX-F37 and points out its potential as a drug in the treatment of diseases that are associated with body fluid overload.aptamer ͉ congestive heart failure ͉ diureses ͉ water homeostasis ͉ Spiegelmer T he cyclic nonapeptide vasopressin (AVP) is a neurohormone that is synthesized in the hypothalamus and stored in the hypophysis from where it is released into the circulation (1). AVP is also known as antidiuretic hormone because its main peripheral function is the maintenance of volume and osmolality of body fluids by regulating the free water reabsorption in the kidneys. Under physiological concentrations, AVP acts vasoconstrictive. AVP's actions are mediated through specific G proteincoupled receptors (2). The V 2 receptor, mainly expressed on cells of the basolateral membrane of the collecting duct in the kidneys, mediates the antidiuretic effect via enhanced cAMP levels (3). As a result, aquaporin channels are inserted into the cytoplasma membranes, and the transcription of aquaporin mRNA is induced. The V 1a receptor, mainly expressed on vascular smooth muscle cells and on cells of the myocardium, exerts vasoconstrictive effects through the second messengers inositoltrisphosphate and diacylglycerol. Subsequently, intracellular Ca 2ϩ is mobilized from the endoplasmic reticulum, and Ca 2ϩ channels as well as Na ϩ ͞H ϩ exchangers are activated (4). In addition to vasoactive effects, binding of AVP to the V 1a receptor also stimulates cell growth and proliferation in vascular smooth muscle cells through activation of the mitogen-activated protein kinase pathway (5).AVP release into the circulation is tightly regulated by osmoreceptors in the hypothalamus and baroreceptors in the heart and large arteries. Whereas osmoreceptors respond to small changes (1%) in osmolality, barorec...

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“…Each is a potent antagonist of the targeted receptors as demonstrated in binding assays and in the expected physiologic responses observed in animal studies. [21][22][23][24][25][26][27] Any of the agents possessing V 2 receptor antagonist activity would be expected to be useful in treating the hyponatremia of CHF.…”

Section: Avp Receptor Antagonistsmentioning

confidence: 99%

Treatment Options for Hyponatremia in Heart Failure

Goldsmith¹

2010

Congestive Heart Failure

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Hyponatremia is independently associated with adverse outcomes in patients with congestive heart failure (CHF). The primary cause of hyponatremia in CHF is the inappropriate secretion of the antidiuretic hormone arginine vasopressin (AVP). The binding of AVP to V2 receptors in the renal collecting duct promotes water retention, a process that can lead to dilutional hyponatremia as well as increased ventricular preload. Conventional treatment of hyponatremia in CHF is largely based on water restriction, which is neither effective nor well‐tolerated. V2‐ and dual V1a/V2‐receptor antagonists offer physiologically based treatment for dilutional hyponatremia. Clinical trials in patients with hyponatremia including those with CHF using both selective and nonselective vasopressin antagonists have demonstrated the effectiveness and safety of these agents in correcting this common electrolyte abnormality. Congest Heart Fail. 2010;16(4)(suppl 1):S15–S18. ©2010 Wiley Periodicals, Inc.

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Pharmacological characterization of YM087, a potent, nonpeptide human vasopressin V1A and V2 receptor antagonist

Cited by 80 publications

References 26 publications

Paraneoplastic Syndromes: An Approach to Diagnosis and Treatment

Paraneoplastic Syndromes: An Approach to Diagnosis and Treatment

An l -RNA-based aquaretic agent that inhibits vasopressin in vivo

Treatment Options for Hyponatremia in Heart Failure

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