RU 486 Inhibits Peripheral Effects of Glucocorticoids in Humans*

Gaillard, Rolf C.; Poffet, Dominique; Riondel, A. M.; Saurat, J.‐H.

doi:10.1210/jcem-61-6-1009

Cited by 93 publications

(48 citation statements)

References 13 publications

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“…With respect to reducing GR-dependent signalling, the challenge has been to reduce glucocorticoid action selectively in the blood vessel wall and/or in metabolically important tissues such as liver and adipose tissue, without: i) impairing negative feedback control of the HPA axis, producing compensatory hypercortisolaemia; ii) reducing glucocorticoid action in immune cells, producing a pro-inflammatory state; or iii) preventing an effective cortisol response during stress. Agents that inhibit cortisol biosynthesis or antagonise ligand binding to GR (119,120) are likely to fall at one of these hurdles. However, inhibition of the cortisolgenerating enzyme 11b-HSD1 may be safe and successful (4, 61).…”

Section: Reducing Glucocorticoid Action and Atheroprotectionmentioning

confidence: 99%

Glucocorticoids and Cardiovascular Disease

Walker¹

2007

European Journal of Endocrinology

477

386

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Chronic excessive activation of glucocorticoid receptors induces obesity, insulin resistance, glucose intolerance, dyslipidaemia and hypertension. Subtle abnormalities of the hypothalamic-pituitaryadrenal axis and/or of tissue sensitivity to glucocorticoids are also associated with these cardiovascular risk factors in patients with the metabolic syndrome. Furthermore, glucocorticoids have direct effects on the heart and blood vessels, mediated by both glucocorticoid and mineralocorticoid receptors and modified by local metabolism of glucocorticoids by the 11b-hydroxysteroid dehydrogenase enzymes. These effects influence vascular function, atherogenesis and vascular remodelling following intravascular injury or ischaemia. This article reviews the systemic and cardiovascular effects of glucocorticoids, and the evidence that glucocorticoids not only promote the incidence and progression of atherogenesis but also modify the recovery from occlusive vascular events and intravascular injury. The conclusion is that manipulation of glucocorticoid action within metabolic and cardiovascular tissues may provide novel therapeutic avenues to combat cardiovascular disease.European Journal of Endocrinology 157 545-559

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Section: Reducing Glucocorticoid Action and Atheroprotectionmentioning

confidence: 99%

Glucocorticoids and Cardiovascular Disease

Walker¹

2007

European Journal of Endocrinology

477

386

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“…These data suggest that glucocorticoids may be involved in the regulation of arterial tension in the mammal although so far this has been supposed to be controlled mostly by the brain mineralocorticoid receptor [55]. In fact, oral administration of Mifepristone abolished vasoconstriction produced by topical application of glucocorticoids in normal men [56]. In addition, it also lowered the intraocular pressure in the rabbit eye [57].…”

Section: Cellular Action Of Mifepristonementioning

confidence: 92%

Glucocorticoid antagonists

Agarwal¹,

Hainque²,

Moustaïd³

et al. 1987

FEBS Letters

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The three principal areas of application of hormone antagonists are: clinical, diagnostic, and delineation of hormone action ([l-5] for reviews). Inhibition of synthesis of glucocorticoids in the adrenal cortex was attempted nearly three decades ago using metyrapone and aminogluthemide derivatives [3,5], and more recently with antimycotic agents [6,7]. Some 45 years ago androgens and superandrogens R 2999 and R 4841 [8-l 11, progesterone [12,13] It is generally admitted that adrenocorticoid hormone action proceeds via a soluble, cytoplasmic receptor in the target cell [l-5]. Thus, an 'ideal', specific, antagonist, devoid of side effects, would have to be sought by structural modification of the native hormone in relation to the receptor structure.

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“…In normal humans, mifepristone blocks glucocorticoid negative feedback at the hypothalamic-pituitary level, inducing a compensatory increase in plasma corticotropin and cortisol levels [54]. After one single-dose oral gift of 400 mg, mifepristone induces a response that lasts at least 34 h. When ketoconazole is unable to lower cortisol production and if the clinical condition requires a rapid, more or less acute total blockade of cortisol receptors (i.e.…”

Section: Mifepristonementioning

confidence: 99%