Nitric oxide and salt sensitivity

Luigi X. Cubeddu; Anna B. Alfieri; Irene S. Hoffmann; Elizabeth Jimenez; Carmen M. Roa; Roberto Cubeddu; Coromoto Palermo; Rosa M. Baldonedo

doi:10.1016/S0895-7061(00)00283-1

Nitric oxide and salt sensitivity

Luigi X. Cubeddu
, Anna B. Alfieri
, Irene S. Hoffmann
, Elizabeth Jimenez
, Carmen M. Roa
, Roberto Cubeddu
, Coromoto Palermo
, Rosa M. Baldonedo

Research output: Contribution to journal › Article › peer-review

Abstract

Studies in laboratory animals suggest that altered nitric oxide (NO) production may be associated with salt sensitivity. In this investigation we determined whether the endogenous NO production was altered in salt-sensitive human subjects when salt intake was changed. Salt sensitivity was assessed from the magnitude of the blood pressure (BP) lowering obtained when the salt intake was reduced from high to a low intake. The combined urinary excretion of nitrites and nitrates, the major metabolites of NO, was employed as an index of endogenous NO production. Salt-sensitive subjects (n = 23) were older, heavier, and had greater waist-to-hip ratios and higher baseline BP than salt-resistant individuals (n = 25). In salt-sensitive subjects, mean blood pressure (MBP) decreased 11.8 ± 0.7 mm Hg, and NO metabolite excretion increased from 823 ± 102 to 1530 ± 148 mmol/24 h, when salt intake was reduced from 316 to 28 μmol/day. NO metabolite excretion was 45% lower during high salt (0.66 ± 0.1 μmol/mg creatinine) than during low salt intake (1.12 ± 0.1 μmol/mg creatinine) (P < .001). In contrast, when salt intake was reduced, salt-resistant subjects exhibited no significant mean changes in BP or NO metabolite excretion. During low salt intake, NO metabolite excretion (μmol/day) was significantly higher in salt-sensitive individuals. The magnitude of decrease of systolic blood pressure, diastolic blood pressure, or MBP induced by reducing salt intake was not related to the increase in urinary excretion of NO metabolite levels (r2 = 0.009; P = .66). In summary, to the extent that urinary NO metabolite levels reflect the activity of the endogenous NO system, our results support the view that salt sensitivity may in part be determined by an inability to increase or to sustain NO production in response to high salt. Insufficient NO production during high salt may in turn lead to altered pressure-natriuresis relationships and to an increase in BP. The possibility that the increase in BP induced by high salt intake in salt-sensitive individuals could be the key factor in reducing NO metabolite levels can not be ruled out. (C) 2000 American Journal of Hypertension, Ltd.

Original language	English
Pages (from-to)	973-979
Number of pages	7
Journal	American Journal of Hypertension
Volume	13
Issue number	9
DOIs	https://doi.org/10.1016/S0895-7061(00)00283-1
State	Published - Sep 2000

Funding

This study was supported by grants from the Consejo Nacional de Investigaciones Cientificas y Tecnologicas, CONICIT S1-96001890; and from The Consejo de Desarrollo Cientifico y Humanistico de la Universidad Central de Venezuela, CDCH 06-104214-98.

ASJC Scopus Subject Areas

Internal Medicine

Keywords

Essential hypertension
Nitric oxide
Salt sensitivity
Humans
Middle Aged
Male
Drug Resistance/physiology
Urine/chemistry
Blood Pressure/drug effects
Diet, Sodium-Restricted
Adult
Female
Sodium Chloride/pharmacology
Nitric Oxide/biosynthesis

Disciplines

Internal Medicine

Access to Document

10.1016/S0895-7061(00)00283-1

Cite this

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title = "Nitric oxide and salt sensitivity",

abstract = "Studies in laboratory animals suggest that altered nitric oxide (NO) production may be associated with salt sensitivity. In this investigation we determined whether the endogenous NO production was altered in salt-sensitive human subjects when salt intake was changed. Salt sensitivity was assessed from the magnitude of the blood pressure (BP) lowering obtained when the salt intake was reduced from high to a low intake. The combined urinary excretion of nitrites and nitrates, the major metabolites of NO, was employed as an index of endogenous NO production. Salt-sensitive subjects (n = 23) were older, heavier, and had greater waist-to-hip ratios and higher baseline BP than salt-resistant individuals (n = 25). In salt-sensitive subjects, mean blood pressure (MBP) decreased 11.8 ± 0.7 mm Hg, and NO metabolite excretion increased from 823 ± 102 to 1530 ± 148 mmol/24 h, when salt intake was reduced from 316 to 28 μmol/day. NO metabolite excretion was 45\% lower during high salt (0.66 ± 0.1 μmol/mg creatinine) than during low salt intake (1.12 ± 0.1 μmol/mg creatinine) (P < .001). In contrast, when salt intake was reduced, salt-resistant subjects exhibited no significant mean changes in BP or NO metabolite excretion. During low salt intake, NO metabolite excretion (μmol/day) was significantly higher in salt-sensitive individuals. The magnitude of decrease of systolic blood pressure, diastolic blood pressure, or MBP induced by reducing salt intake was not related to the increase in urinary excretion of NO metabolite levels (r2 = 0.009; P = .66). In summary, to the extent that urinary NO metabolite levels reflect the activity of the endogenous NO system, our results support the view that salt sensitivity may in part be determined by an inability to increase or to sustain NO production in response to high salt. Insufficient NO production during high salt may in turn lead to altered pressure-natriuresis relationships and to an increase in BP. The possibility that the increase in BP induced by high salt intake in salt-sensitive individuals could be the key factor in reducing NO metabolite levels can not be ruled out. (C) 2000 American Journal of Hypertension, Ltd. ",

keywords = "Essential hypertension, Nitric oxide, Salt sensitivity, Humans, Middle Aged, Male, Drug Resistance/physiology, Urine/chemistry, Blood Pressure/drug effects, Diet, Sodium-Restricted, Adult, Female, Sodium Chloride/pharmacology, Nitric Oxide/biosynthesis",

author = "Cubeddu, \{Luigi X.\} and Alfieri, \{Anna B.\} and Hoffmann, \{Irene S.\} and Elizabeth Jimenez and Roa, \{Carmen M.\} and Roberto Cubeddu and Coromoto Palermo and Baldonedo, \{Rosa M.\}",

year = "2000",

month = sep,

doi = "10.1016/S0895-7061(00)00283-1",

language = "English",

volume = "13",

pages = "973--979",

journal = "American Journal of Hypertension",

issn = "0895-7061",

number = "9",

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TY - JOUR

T1 - Nitric oxide and salt sensitivity

AU - Cubeddu, Luigi X.

AU - Alfieri, Anna B.

AU - Hoffmann, Irene S.

AU - Jimenez, Elizabeth

AU - Roa, Carmen M.

AU - Cubeddu, Roberto

AU - Palermo, Coromoto

AU - Baldonedo, Rosa M.

PY - 2000/9

Y1 - 2000/9

N2 - Studies in laboratory animals suggest that altered nitric oxide (NO) production may be associated with salt sensitivity. In this investigation we determined whether the endogenous NO production was altered in salt-sensitive human subjects when salt intake was changed. Salt sensitivity was assessed from the magnitude of the blood pressure (BP) lowering obtained when the salt intake was reduced from high to a low intake. The combined urinary excretion of nitrites and nitrates, the major metabolites of NO, was employed as an index of endogenous NO production. Salt-sensitive subjects (n = 23) were older, heavier, and had greater waist-to-hip ratios and higher baseline BP than salt-resistant individuals (n = 25). In salt-sensitive subjects, mean blood pressure (MBP) decreased 11.8 ± 0.7 mm Hg, and NO metabolite excretion increased from 823 ± 102 to 1530 ± 148 mmol/24 h, when salt intake was reduced from 316 to 28 μmol/day. NO metabolite excretion was 45% lower during high salt (0.66 ± 0.1 μmol/mg creatinine) than during low salt intake (1.12 ± 0.1 μmol/mg creatinine) (P < .001). In contrast, when salt intake was reduced, salt-resistant subjects exhibited no significant mean changes in BP or NO metabolite excretion. During low salt intake, NO metabolite excretion (μmol/day) was significantly higher in salt-sensitive individuals. The magnitude of decrease of systolic blood pressure, diastolic blood pressure, or MBP induced by reducing salt intake was not related to the increase in urinary excretion of NO metabolite levels (r2 = 0.009; P = .66). In summary, to the extent that urinary NO metabolite levels reflect the activity of the endogenous NO system, our results support the view that salt sensitivity may in part be determined by an inability to increase or to sustain NO production in response to high salt. Insufficient NO production during high salt may in turn lead to altered pressure-natriuresis relationships and to an increase in BP. The possibility that the increase in BP induced by high salt intake in salt-sensitive individuals could be the key factor in reducing NO metabolite levels can not be ruled out. (C) 2000 American Journal of Hypertension, Ltd.

AB - Studies in laboratory animals suggest that altered nitric oxide (NO) production may be associated with salt sensitivity. In this investigation we determined whether the endogenous NO production was altered in salt-sensitive human subjects when salt intake was changed. Salt sensitivity was assessed from the magnitude of the blood pressure (BP) lowering obtained when the salt intake was reduced from high to a low intake. The combined urinary excretion of nitrites and nitrates, the major metabolites of NO, was employed as an index of endogenous NO production. Salt-sensitive subjects (n = 23) were older, heavier, and had greater waist-to-hip ratios and higher baseline BP than salt-resistant individuals (n = 25). In salt-sensitive subjects, mean blood pressure (MBP) decreased 11.8 ± 0.7 mm Hg, and NO metabolite excretion increased from 823 ± 102 to 1530 ± 148 mmol/24 h, when salt intake was reduced from 316 to 28 μmol/day. NO metabolite excretion was 45% lower during high salt (0.66 ± 0.1 μmol/mg creatinine) than during low salt intake (1.12 ± 0.1 μmol/mg creatinine) (P < .001). In contrast, when salt intake was reduced, salt-resistant subjects exhibited no significant mean changes in BP or NO metabolite excretion. During low salt intake, NO metabolite excretion (μmol/day) was significantly higher in salt-sensitive individuals. The magnitude of decrease of systolic blood pressure, diastolic blood pressure, or MBP induced by reducing salt intake was not related to the increase in urinary excretion of NO metabolite levels (r2 = 0.009; P = .66). In summary, to the extent that urinary NO metabolite levels reflect the activity of the endogenous NO system, our results support the view that salt sensitivity may in part be determined by an inability to increase or to sustain NO production in response to high salt. Insufficient NO production during high salt may in turn lead to altered pressure-natriuresis relationships and to an increase in BP. The possibility that the increase in BP induced by high salt intake in salt-sensitive individuals could be the key factor in reducing NO metabolite levels can not be ruled out. (C) 2000 American Journal of Hypertension, Ltd.

KW - Essential hypertension

KW - Nitric oxide

KW - Salt sensitivity

KW - Humans

KW - Middle Aged

KW - Male

KW - Drug Resistance/physiology

KW - Urine/chemistry

KW - Blood Pressure/drug effects

KW - Diet, Sodium-Restricted

KW - Adult

KW - Female

KW - Sodium Chloride/pharmacology

KW - Nitric Oxide/biosynthesis

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DO - 10.1016/S0895-7061(00)00283-1

M3 - Article

C2 - 10981546

AN - SCOPUS:0033863841

SN - 0895-7061

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JO - American Journal of Hypertension

JF - American Journal of Hypertension

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ER -

Nitric oxide and salt sensitivity

Abstract

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