Moriyuki Sakata scite author profile

Moriyuki Sakata

4Publications

33Citation Statements Received

44Citation Statements Given

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101

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Affiliations

Shimano (Japan), Washington University in St. Louis, Ono Pharmaceutical (Japan)

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Is atriopeptin a physiological or pathophysiological substance? Studies in the autoimmune rat.

Greenwald

Sakata²,

Michener³

et al. 1988

J. Clin. Invest.

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Atriopeptin (AP), a natriuretic-diuretic and vasodilatory peptide, is synthesized and secreted from mammalian atria. The definitive role of this peptide on cardiovascular physiology and pathophysiology has yet to be determined. We developed a population of autoimmune rats sensitized against their own AP to evaluate the consequences of prolonged AP deficiency on physiological and pathophysiological processes. Natriuresis in response to acute intravenous volume expansion was inhibited in the autoimmune rat, however, natriuresis produced by chronic oral salt loading was not suppressed in these animals. Plasma AP increased threefold in the spontaneously hypertensive rat when evaluated as a function of blood pressure. Immunization of these rats had no effect on the rate of development, magnitude of their developing hypertension, or their daily sodium excretion when compared with nonimmunized controls. Mineralocorticoid escape occurred during desoxycorticosterone acetate administration to rats. The ability of rats to escape from the sodium-retaining effects of this steroid was not affected by prior immunization against AP. These results suggest that AP is an important natriuretic substance in response to acute intravascular volume loading. However, atriopeptin does not appear to be involved in the natriuretic response to chronic intravascular volume loading, blood pressure regulation, or mineralocorticoid escape.

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Paradoxical relationship between atriopeptin plasma levels and diuresis-natriuresis induced by acute volume expansion.

Sakata

Greenwald

Needleman

1988

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

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Surgical removal of one or both atrial appendages was employed in rats to reduce the intrinsic stores of atriopeptin (AP). In conscious rats (with intact baroreceptor reflexes), bilateral or unilateral atrial appendectomy suppressed the diuresis and natriuresis produced by acute volume expansion. Surprisingly, volume expansion (with 4% bovine serum albumin in saline at 1.5 ml/kg per min for 15 min) did not result in an increase in plasma AP immunoreactivity (APir) in control or atrial-appendectomized conscious rats. Previous studies demonstrated that acute volume expansion in anesthetized animals caused increased plasma APir. Indeed, we found that volume expansion causes comparable diuresisnatriuresis in conscious and chloral hydrate-anesthetized rats, but only the latter group exhibits an increase in plasma APir. Brattleboro rats, which are deficient in vasopressin, exhibit the same response as Long-Evans controls in that acute volume expansion in conscious animals produces a pronounced diuresis and natriuresis but no APir release, but when these same animals are anesthetized, there is a simultaneous induction of diuresis-natriuresis and APir release by volume expansion. Plasma AP does not increase in conscious rats despite a large volume load, 3040% of the total blood volume given in 15 min, and the natriuresis-diuresis appears to also be independent of vasopressin. On the other hand, the diuresis induced by acute volume expansion in anesthetized rats seems dependent on the elevated APir, since rats made autoimmune to AP (which are nonresponsive to exogenous AP infusions) exhibit a diuresis in conscious but not anesthetized rats. We therefore conclude that the participation of AP in volume homeostasis is more likely in pathophysiological states and that another mechanism or possibly another atrial factor mediates the diuresis-natriuresis induced by volume expansion in conscious rats.Atrial distension produced by elevation of atrial pressure or head-out water immersion (1), volume expansion (2-5), and administration of pressor agents (1, 6) lead to release of atriopeptin (AP) from the atria. Many investigators have reported that AP immunoreactivity (APir) release appears to be stimulated by atrial distension through acute volume expansion both in animals (2,3,7,8) and in humans (4-9). Removal of right atrial appendages in anesthetized rats attenuated the urinary volume (UV) and urinary sodium excretion (UNaV) in response to volume expansion (10).Similarly, conscious rats 2 weeks after bilateral atrial appendectomy exhibited reduced UV and UNaV during volume expansion (11 In the present study we examined the changes in plasma APir in atrial appendectomized rats. We decided to perform these experiments in conscious precannulated animals because we had observed that basal plasma APir levels were considerably higher in chloral hydrate-anesthetized animals compared to unanesthetized controls. The choice of these conditions led us to an unanticipated finding: the diuresis caused by volume expansion of conscio...

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Effects of ONO-3708, an antagonist of the thromboxane A2/prostaglandin endoperoxide receptor, on platelet aggregation and thrombosis

Kondo

Seo

Naka

et al. 1989

European Journal of Pharmacology

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Pharmacological studies on expectorants.

Kasé¹,

Yakushiji²,

Seo³

et al. 1977

Folia Pharmacologica Japonica

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Moriyuki Sakata

Is atriopeptin a physiological or pathophysiological substance? Studies in the autoimmune rat.

Paradoxical relationship between atriopeptin plasma levels and diuresis-natriuresis induced by acute volume expansion.

Effects of ONO-3708, an antagonist of the thromboxane A2/prostaglandin endoperoxide receptor, on platelet aggregation and thrombosis

Pharmacological studies on expectorants.

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