The highly conserved cardiac glycoside binding site of Na,K-ATPase plays a role in blood pressure regulation

Dostanic-Larson, Iva; Huysse, James W. Van; Lorenz, John N.; Lingrel, Jerry B.

doi:10.1073/pnas.0507358102

Cited by 173 publications

(202 citation statements)

References 62 publications

(71 reference statements)

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“…In transgenic mice with mutated ␣1 and ␣ 2 Na ϩ pumps, in which ␣ 1 is rendered ouabain sensitive and ␣ 2 is ouabain resistant, ACTH induces a profound, Digibindsensitive hypertension within 24 h (20). The implication is that acute inhibition of ␣ 1 , which increases tone and contractility in isolated arteries (120), can elevate BP.…”

Section: How Does Low-dose Ouabain Augment Contractility?mentioning

confidence: 99%

“…But the NCX and ␣ 2 Na ϩ pumps are colocalized in PM microdomains at PM-SER junctions (Fig. 2) (56,106) where these two transport systems appear to function cooperatively (4,30 (20), and this increases myogenic tone (50,120) by a direct effect on the contractile machinery.…”

Section: Ouabain Antagonism As a Therapy For Hypertensionmentioning

confidence: 99%

“…Moreover, the plasma from mice with ACTHinduced hypertension had significantly elevated levels of a water-soluble substance that cross-reacted with antidigoxinspecific Fab fragments (Digibind) (20). Digibind, which binds ouabain with high affinity (91), abolished the hypertensinogenic effect of ACTH (20,66). Interestingly, plasma from patients with pregnancy-induced hypertension have elevated levels of a ouabain-like compound and marinobufagenin (70).…”

Section: How Does Low-dose Ouabain Augment Contractility?mentioning

confidence: 99%

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How does salt retention raise blood pressure?

Blaustein¹,

Zhang²,

Ling³

et al. 2006

American Journal of Physiology-Regulatory, Integrative and Comp

128

121

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A critical question in hypertension research is: How is long-term blood pressure controlled? Excessive NaCl ingestion or NaCl retention by the kidneys and the consequent tendency toward plasma volume expansion lead to hypertension. Nevertheless, the precise mechanisms linking salt to high blood pressure are unresolved. The discovery of endogenous ouabain, an adrenocortical hormone, provided an important clue. Ouabain, a selective Na ϩ pump inhibitor, has cardiotonic and vasotonic effects. Plasma endogenous ouabain levels are significantly elevated in Ϸ40% of patients with essential hypertension and in animals with several forms of salt-dependent hypertension. Also, prolonged ouabain administration induces hypertension in rodents. Mice with mutant Na ϩ pumps or Na/Ca exchangers (NCX) and studies with a ouabain antagonist and an NCX blocker are revealing the missing molecular mechanisms. These data demonstrate that ␣ 2 Na ϩ pumps and NCX1 participate in long-term regulation of vascular tone and blood pressure. Pharmacological agents or mutations in the ␣ 2 Na ϩ pump that interfere with the action of ouabain on the pump, and reduced NCX1 expression or agents that block NCX all impede the development of salt-dependent or ouabain-induced hypertension. Conversely, nanomolar ouabain, reduced ␣ 2 Na ϩ pump expression, and smooth muscle-specific overexpression of NCX1 all induce hypertension. Furthermore, ouabain and reduced ␣ 2 Na ϩ pump expression increase myogenic tone in isolated mesenteric small arteries in vitro, thereby tying these effects directly to the elevation of blood pressure. Thus, endogenous ouabain, and vascular ␣ 2 Na ϩ pumps and NCX1, are critical links between salt and hypertension. New pharmacological agents that act on these molecular links have potential in the clinical management of hypertension.ouabain; Na ϩ pump; Na/Ca exchanger; Ca 2ϩ ; myogenic tone HYPERTENSION, DEFINED AS A diastolic blood pressure (BP) Ն 90 mmHg and/or systolic BP Ն 140 mmHg, is endemic in Westernized societies. This is a very important public health issue because hypertension is a major risk factor for premature death and disability from heart attack, heart failure, stroke, and many other afflictions (16,59). In the United States, alone, Ϸ20% of the population (i.e., Ϸ50 million individuals) are hypertensive; moreover, more than half of all individuals over the age of 60 years have hypertension. In a small fraction of cases, the hypertension is due to specific causes, such as renal vascular disease or excessive secretion of aldosterone (primary aldosteronism) or catecholamines (pheochromocytoma). The vast majority (Ϸ90%) of patients, however, have elevated BP of unknown cause; hence the terms, primary or essential hypertension. The immediate cause for the elevated BP in nearly all chronic hypertensive persons is excessive narrowing of the small (resistance) arteries. Nevertheless, a key question in any discussion of hypertension is: What specific mechanisms actually lead to the abnormal arterial constriction and elevation ...

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Section: How Does Low-dose Ouabain Augment Contractility?mentioning

confidence: 99%

Section: Ouabain Antagonism As a Therapy For Hypertensionmentioning

confidence: 99%

Section: How Does Low-dose Ouabain Augment Contractility?mentioning

confidence: 99%

See 1 more Smart Citation

How does salt retention raise blood pressure?

Blaustein¹,

Zhang²,

Ling³

et al. 2006

American Journal of Physiology-Regulatory, Integrative and Comp

128

121

View full text Add to dashboard Cite

show abstract

“…However, it is still difficult to draw definitive conclusions regarding the specific function of these molecules in pathophysiology. Although the studies by Dostanic-Larson et al (2) strongly support the suggestion that endogenous cardiac glycoside-like compounds are the naturally occurring ligand, they do not eliminate the possibility that other steroid-like (or, indeed, nonsteroidal) molecules, either previously identified or novel, may play this functional role. Nevertheless, this important work does clearly demonstrate that a naturally occurring regulator must exist and that its interaction with the cardiac glycoside binding site of the Na,K-ATPase plays a role in blood pressure regulation.…”

mentioning

confidence: 81%

“…However, the strong evolutionary conservation of this binding site among almost all species has suggested that important physiological functions may involve recognition of this site by endogenous agents. The work of Dostanic-Larson et al in this issue of PNAS (2) demonstrates that the cardiac glycoside binding site of Na,K-ATPase plays an important physiological role in blood pressure regulation. It is reported that ACTH-induced hypertension is abolished when the interaction of cardiac glycosides with the Na,K-ATPase is disrupted.…”

mentioning

confidence: 99%

The sodium pump and hypertension: A physiological role for the cardiac glycoside binding site of the Na,K-ATPase

Kaplan

2005

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

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An Efficient One‐Pot Enzymatic Synthesis of Cardiac Glycosides with Varied Sugar Chain Lengths

et al. 2019

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An efficient one‐pot enzymatic synthesis of cardiac glycosides with varied sugar chain lengths (average yield >80%) was carried out through sequential glycosylation using a steroid glycosyltransferase UGT74AN3 from Catharanthus roseus and a cyclodextrin glycosyltransferase from Bacillus licheniformis. A series of cardiac glycosides were obtained and showed enhanced affinity and selectivity for inhibition of the α2 isoform of Na+/K+‐ATPase. These findings demonstrate the significant potential of the one‐pot biocatalytic approach in the synthesis of diverse cardiac glycosides as potentially safer cardiotonic agents.

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The highly conserved cardiac glycoside binding site of Na,K-ATPase plays a role in blood pressure regulation

Cited by 173 publications

References 62 publications

How does salt retention raise blood pressure?

How does salt retention raise blood pressure?

The sodium pump and hypertension: A physiological role for the cardiac glycoside binding site of the Na,K-ATPase

An Efficient One‐Pot Enzymatic Synthesis of Cardiac Glycosides with Varied Sugar Chain Lengths

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