Circulating Nitric Oxide (Nitrite/Nitrate) Levels in Postmenopausal Women Substituted With 17β-Estradiol and Norethisterone Acetate

Rosselli, Marinella; Imthurn, Bruno; Keller, Paul J.; Jackson, Edwin K.; Dubey, Raghvendra K.

doi:10.1161/01.hyp.25.4.848

Cited by 237 publications

(116 citation statements)

References 27 publications

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“…18,52 However, by comparison to other osteoporosis-like phenotype models eNOSϪ/Ϫ mice are distinct. For example, osteoprotegerin-gene-deficient mice demonstrate an early onset osteoporosis-like phenotype, 53 similar to eNOSϪ/Ϫ mice but is because of increased osteoclast numbers and resorption rather than attenuated osteoblast activity.…”

Section: Discussionmentioning

confidence: 99%

Endothelial Nitric Oxide Synthase Gene-Deficient Mice Demonstrate Marked Retardation in Postnatal Bone Formation, Reduced Bone Volume, and Defects in Osteoblast Maturation and Activity

Aguirre

Buttery

O'Shaughnessy

et al. 2001

The American Journal of Pathology

218

149

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Nitric oxide (NO) has been implicated in the local regulation of bone metabolism. However, the contribution made by specific NO synthase (NOS) enzymes is unclear. Here we show that endothelial NOS gene knockout mice (eNOS؊/؊) have marked abnormalities in bone formation. Histomorphometric analysis of eNOS؊/؊ femurs showed bone volume and bone formation rate was reduced by up to 45% (P < 0.01) and 52% (P < 0.01), respectively. These abnormalities were prevalent in young (6 to 9 weeks old) adults but by 12 to 18 weeks bone phenotype was restored toward wild-type. Dual energy X-ray absorptiometry analysis confirmed the age-related bone abnormalities revealing significant reductions in femoral (P < 0.05) and spinal bone mineral densities (P < 0.01) at 8 weeks that were normalized at 12 weeks. Reduction in bone formation and volume was not related to increased osteoclast numbers or activity but rather to dysfunctional osteoblasts. Osteoblast numbers and mineralizing activity were reduced in eNOS؊/؊ mice. In vitro, osteoblasts from calvarial explants showed retarded proliferation and differentiation (alkaline phosphatase activity and mineral deposition) that could be restored by exogenous administration of a NO donor. These cells were also unresponsive to 17␤-estradiol and had an attenuated chemotactic response to transforming growth factor-␤. Bone is a vital dynamic connective tissue that has evolved to maintain a balance between its two major functions: provision of mechanical integrity for locomotion and modulation and control of mineral homeostasis. 1 Mineralized bone is continuously resorbed by osteoclasts and new bone is formed by osteoblasts. This process, known as bone remodeling, is highly regulated with maintenance of normal integrity and structure. 2 Systemic hormones including calcitonin, parathyroid hormone, and sex steroids, particularly estrogen, are known to be important regulators of bone cell function. Their effects on bone turnover are in general exerted by activation of local mediators and second messengers present within bone cells. 3 Recent investigations have focused on the role of nitric oxide (NO) as one of these possible local regulators of bone metabolism and bone cell activity. NO is a shortlived radical gas generated from L-arginine by nitric oxide synthase (NOS) isoenzymes. 4 Three distinct isoforms of NOS have been identified: a neuronal form (type I; nNOS) originally isolated from brain, 5 an endothelial form (type III; eNOS) originally isolated from bovine aortic endothelial cells, 6 and an inducible form (type II; iNOS) originally isolated from murine macrophages. 7 Both eNOS and nNOS are expressed constitutively and are characterized by highly regulated rapid but low-output NO production. 4 In contrast the iNOS pathway is generally only activated after stimulation by certain pro-inflammatory cytokines such as interferon-␥, interleukin-1␤, and tumor necrosis factor-␣. The inducible NOS isoform is characterized by production of persistent and high concentrations of NO. 8 There is now am...

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Section: Discussionmentioning

confidence: 99%

Endothelial Nitric Oxide Synthase Gene-Deficient Mice Demonstrate Marked Retardation in Postnatal Bone Formation, Reduced Bone Volume, and Defects in Osteoblast Maturation and Activity

Aguirre

Buttery

O'Shaughnessy

et al. 2001

The American Journal of Pathology

218

149

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“…In humans, acute administration of oestrogen improves vasodilatation induced by acetylcholine in coronary arteries [23,24]. The assumption that this improvement in EDV is mediated by the NO system is further strengthened by the finding that oestrogen supplementation increased the levels of nitrate and nitrite, the breakdown products of NO, in postmenopausal women [25].…”

Section: Discussionmentioning

confidence: 99%

Effects of age, gender and metabolic factors on endothelium‐dependent vasodilation: a population‐based study

Sarabi

Millgård

Lind

1999

Journal of Internal Medicine

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Abstract. Sarabi M, Millga Êrd J, Lind L (University Hospital, Uppsala, Sweden). Effects of age, gender and metabolic factors on endothelium-dependent vasodilation: a population-based study. J Intern Med 1999; 246: 265±274.Objectives. A progressive decline in endotheliumdependent vasodilation (EDV) in the human forearm with age has previously been reported. The aim of this study was to evaluate the interplay between age, gender and metabolic factors on EDV in healthy subjects in a population-based study. Setting. Tertiary university hospital. Subjects and design. Thirty-six healthy men and 30 women, aged 20±69 years, underwent measurements of forearm blood flow (FBF) at rest and during local infusions of 2 and 4 mg min 21 of metacholine (evaluating EDV) and 5 and 10 mg min 21 of sodium nitroprusside (evaluating endothelium-independent vasodilation, EIDV) and during reactive hyperaemia by venous occlusion plethysmography. Results. Age was inversely related to EDV (r = ± 0.41, P , 0.05 in men; r = ± 0.61, P , 0.01 in women) and maximal FBF during reactive hyperaemia in both men and women. EIDV was significantly related to age in an inverse way in women only. EDV was more pronounced in females than in males before menopause (48 6 3 SD years, 635 6 186 vs. 502 6 269% in males, P , 0.05), but similar in women and men thereafter (374 6 141 vs. 370 6 185% in men). The slope of the regression line for the relationship between age and EDV was flatter in premenopausal than in postmenopausal women (± 2.3 vs. ± 6.4), whilst this slope was similar in younger and older men (± 5.5 vs. ± 5.3). In multiple regression analysis, fasting blood glucose levels and the waist/hip ratio remained the only significant predictors of EDV in men (P , 0.01 for both), whilst age was the only significant independent predictor of EDV in women (P , 0.01). Conclusion. The interplay between age and metabolic factors as determinants of endothelial function is different in healthy men and women.

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“…[40][41]44 Studies have shown that synthetic progestogens may exert a relative vasoconstrictor effect on the vasculature, the magnitude of the effect being proportional to the relative 'androgenicity' of the individual preparation. [40][41][42]44 In contrast to the vasoconstrictor effects observed with the 'androgenic' progestogens, the 'non-androgenic' progestogens including progesterone and medroxyprogesterone (which was used in the current study) have been shown to have a net vasodilator effect. 38,41,44 The observations in the present study examining the dose-response of cyclical MPA in the presence of a fixed replacement dose of oestrogen are consistent with MPA having either no net effect on vascular tone or a small net vasodilator effect.…”

Section: Discussionmentioning

confidence: 64%

“…37 The magnitude of any progestogen-related effect may also be influenced by the relative androgenicity of the progestogen preparation used. [40][41][42][43][44] In the present study in normotensive postmenopausal women, a randomised, double-blind crossover design was used to compare with placebo the effects on blood pressure and other cardiovascular parameters of cyclical doses spanning the clinical dose range of the C21 progestogen, medroxyprogesterone acetate, in normotensive women receiving a fixed mid-range daily dose of conjugated equine oestrogen. The study tested the null hypothesis that there would be no significant effect on blood pressure from the addition of 'replacement' doses of exogenous semi-synthetic progestogen as cyclical therapy to daily oestrogen supplementation in postmenopausal normotensive women.…”

Section: Introductionmentioning

confidence: 99%

Dose response effect of cyclical medroxyprogesterone on blood pressure in postmenopausal women

et al. 2001

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Objective: This study was designed to compare with placebo the dose-response effect of cyclical doses of the C21 progestogen, medroxyprogesterone acetate (MPA) on blood pressure (BP) when administered to normotensive postmenopausal women receiving a fixed mid-range daily dose of conjugated equine oestrogen (CEE). Materials and methods: Twenty normotensive postmenopausal women (median age 53 years) participated in the study which used a double-blind crossover design. There were four randomised treatment phases, each of 4 weeks duration. The four blinded treatments were MPA 2.5 mg, MPA 5 mg, MPA 10 mg and matching placebo, taken for the last 14 days of each 28 day treatment cycle. CEE 0.625 mg was also administered once daily as open labelled tablets to all subjects throughout the study. Clinic BP was measured weekly with the

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Circulating Nitric Oxide (Nitrite/Nitrate) Levels in Postmenopausal Women Substituted With 17β-Estradiol and Norethisterone Acetate

Cited by 237 publications

References 27 publications

Endothelial Nitric Oxide Synthase Gene-Deficient Mice Demonstrate Marked Retardation in Postnatal Bone Formation, Reduced Bone Volume, and Defects in Osteoblast Maturation and Activity

Endothelial Nitric Oxide Synthase Gene-Deficient Mice Demonstrate Marked Retardation in Postnatal Bone Formation, Reduced Bone Volume, and Defects in Osteoblast Maturation and Activity

Effects of age, gender and metabolic factors on endothelium‐dependent vasodilation: a population‐based study

Dose response effect of cyclical medroxyprogesterone on blood pressure in postmenopausal women

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