Monogenic forms of mineralocorticoid hypertension: insights into the pathogenesis of ‘essential’ hypertension?

Petrelli, Massimiliano; Stewart, PM

doi:10.1038/sj.jhh.1000512

Cited by 6 publications

(4 citation statements)

References 75 publications

(82 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Whereas an argument exists for attempting complete suppression of abnormally regulated aldosterone production in patients with FH-I (see below), this approach would also be expected to render patients at significant risk of Cushingoid side effects. Indeed, occasional reports (21) of glucocorticoidinduced side effects in treated patients have caused some investigators to express caution in the use of glucocorticoids (22,23) and, in the case of affected children, to favor the use of other agents (such as amiloride) to avoid the growthretarding effects of glucocorticoid treatment in this age group (24). In the current study of eight patients with genetically proven FH-I, glucocorticoid doses of 0.125-0.25 mg dexamethasone daily or 2.5-5 mg prednisolone daily were sufficient to maintain normal blood pressure throughout 0.5-3.8 yr of follow-up without the need for additional antihypertensive medication.…”

Section: Discussionmentioning

confidence: 99%

Treatment of Familial Hyperaldosteronism Type I: Only Partial Suppression of Adrenocorticotropin Required to Correct Hypertension

Stowasser

Bachmann

Huggard

et al. 2000

The Journal of Clinical Endocrinology &Amp; Metabolism

View full text Add to dashboard Cite

In familial hyperaldosteronism type I, inheritance of a hybrid 11␤-hydroxylase/aldosterone synthase gene leads to ACTH-regulated overproduction of aldosterone (causing hypertension) and of "hybrid" steroids, 18-hydroxy-and 18-oxo-cortisol. To determine whether complete suppression of the hybrid gene is necessary to normalize blood pressure, we sought evidence of persisting expression in eight patients who were rendered normotensive for 1.3-4.5 yr by glucocorticoid treatment. At the time of the study, six patients were receiving dexamethasone (0.125-0.25 mg/day) and two patients were taking prednisolone (2.5 or 5 mg/day). Urinary 18-oxo-cortisol levels during treatment demonstrated close correlation with mean "day curve" (blood collected every 2 h for 24 h) cortisol (r ϭ 0.74), consistent with regulation by ACTH. Although urinary 18-oxo-cortisol levels were lower during than before treatment (mean 12.6 Ϯ 2.4 SEM vs. 35.0 Ϯ 5.6 nmol/mmol creatinine; P Ͻ 0.01), they remained above normal (0.8 -5.2 nmol/mmol creatinine) in all eight patients. Although mean upright plasma potassium levels during treatment were higher, aldosterone levels lower, PRA levels higher, and aldosterone to PRA ratios lower than before treatment, PRA levels were uncorrected (Ͻ13 pmol/L⅐min) and aldosterone to PRA ratios were uncorrected (Ͼ65) during treatment in four patients. For each of the eight patients, day curve aldosterone levels during treatment correlated more tightly with cortisol (mean r for the eight patients, 0.87 Ϯ 0.05 SEM) than with PRA (mean r ϭ 0.36 Ϯ 0.10 SEM). Hence, control of hypertension by glucocorticoid treatment was associated, in all patients, with only partial suppression of ACTH-regulated hybrid steroid and aldosterone production. Normalization of urinary hybrid steroid levels and abolition of ACTH-regulated aldosterone production is not a requisite for hypertension control and, if used as a treatment goal, may unnecessarily increase the risk of Cushingoid side effects. (J Clin Endocrinol Metab 85: 3313-3318, 2000)

show abstract

Section: Discussionmentioning

confidence: 99%

Treatment of Familial Hyperaldosteronism Type I: Only Partial Suppression of Adrenocorticotropin Required to Correct Hypertension

Stowasser

Bachmann

Huggard

et al. 2000

The Journal of Clinical Endocrinology &Amp; Metabolism

View full text Add to dashboard Cite

show abstract

“…79 The potential importance of abnormal renal tubular sodium reabsorption as a determinant of sodium balance and of blood pressure has been highlighted by genetic studies of renal sodium transporters in rare familial conditions. 80 For example, Liddle's syndrome is a rare autosomal dominant disorder caused by a molecular defect leading to increased activity of the renal epithelial sodium channel. The increased renal sodium reabsorption and sodium retention leads to high blood pressure and suppression of plasma renin activity.…”

Section: Renal Epithelial Sodium Channelmentioning

confidence: 99%

Why is plasma renin activity lower in populations of African origin?

Sagnella

2000

J Hum Hypertens

View full text Add to dashboard Cite

Plasma renin activity is significantly lower in black people compared with whites independent of age and blood pressure status. The lower PRA appears to be due to a reduction in the rate of secretion of renin but the exact mechanistic events underlying such differences in renin release between blacks and whites are still not fully understood. Nevertheless, given the paramount importance of the renin-angiotensin system in the control of sodium balance, a most likely explanation is that the lower renin is a consequence of differences in renal sodium handling between blacks and whites. The lower PRA does not reflect differences in dietary sodium intake but the evidence available suggests that the low PRA could be part of the corrective mechanisms designed to maintain sodium balance in the presence of an increased tendency for sodium retention in black people. While it is possible that several factors may contribute to the reduced PRA, more recent investigation at

show abstract

“…1 Until recently, however, there were no clues to the molecular basis of GS, another variety of salt-sensitive familial hypertension. Important progress was made in the recent study by Mansfield et al, 6 in which evidence for linkage to chromosomes 1 and 17 was found.…”

Section: Discussionmentioning

confidence: 99%

Linkage of Gordon’s syndrome to the long arm of chromosome 17 in a region recently linked to familial essential hypertension

O’Shaughnessy

Johnson

et al. 1998

J Hum Hypertens

View full text Add to dashboard Cite

Gordon's syndrome (GS) is a salt-sensitive, hyperkalaemic, familial hypertension syndrome which may masquerade in milder forms as essential hypertension. The response of hyperakalaemia to dietary salt restriction and to mineralocorticoids is heterogeneous, suggesting genetic heterogeneity. In a recently published study using small pedigrees, possible linkage of GS to chromosomes 1 and 17 was described. Studying the largest pedigree so far reported with GS, and using fluorescentlabelled microsatellite markers, we sought evidence of linkage to chromosomes 1 and 17. In this family there was no segregation of GS with any of the markers for

show abstract

Monogenic forms of mineralocorticoid hypertension: insights into the pathogenesis of ‘essential’ hypertension?

Cited by 6 publications

References 75 publications

Treatment of Familial Hyperaldosteronism Type I: Only Partial Suppression of Adrenocorticotropin Required to Correct Hypertension

Treatment of Familial Hyperaldosteronism Type I: Only Partial Suppression of Adrenocorticotropin Required to Correct Hypertension

Why is plasma renin activity lower in populations of African origin?

Linkage of Gordon’s syndrome to the long arm of chromosome 17 in a region recently linked to familial essential hypertension

Contact Info

Product

Resources

About