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Hypertension 

Spironolactone and Chlorthalidone: A Novel and Effective Antihypertensive Regimen?

By Gregory W. Rutecki, MD | July 13, 2012
Dr Rutecki is Professor of Medicine at the University of South Alabama in Mobile.

A recent podcast1  and article2 visited resuscitation of an “old” antihypertensive agent—the thiazide diuretic chlorthalidone. They told the upside of the chlorthalidone story.

Despite its advantages, however, chlorthalidone has its downsides. Like other thiazides, it increases weight and insulin resistance, lowers potassium levels, and can lead to volume depletion and hyponatremia. In fact, with its longer half-life, it may be associated with more insulin resistance than its thiazide cousins. Recent data also suggest that chlorthalidone activates the sympathetic nervous system.3 Heightened activity is not a good thing for hypertensive patients. The activation may be a consequence of chlorthalidone-induced elevations of both angiotensin and aldosterone levels.

That axis may be where something new can be combined with chlorthalidone for benefit—namely spironolactone(Drug information on spironolactone).

Spironolactone has been around for a while, but it is unrecognized as a potent antihypertensive. This aldosterone receptor antagonist has become a remarkable addition to therapy in patients with resistant hypertension.4 Evidence is also emerging to suggest that a combination of spironolactone and chlorthalidone is synergistic. The two disparate diuretics may become a novel and efficacious antihypertensive regimen.

Seventeen patients with previously untreated essential hypertension underwent baseline sympathetic nerve activity measurements.3 They then underwent crossover therapy with
• 12 weeks of chlorthalidone as monotherapy
•  Chlorthalidone plus spironolactone, and
•  Chlorthalidone plus irbesartan(Drug information on irbesartan), an angiotensin receptor blocker

In group 1, chlorthalidone decreased 24-hour ambulatory blood pressures from 135 ± 3/84 ± 2 to 124 ± 2/78 ± 2 mm/Hg. But monotherapy with chlorthalidone increased sympathetic nerve activity. Although a combination of irbesartan plus chlorthalidone was as effective in lowering blood pressure, it did not reduce the chlorthalidone-mediated rise in sympathetic activity (group 3). However, sympathetic activity was returned to baseline when spironolactone was added to chlorthalidone. Blood pressure did well with the addition. Also noted was that chlorthalidone monotherapy increased markers for insulin resistance. Adding spironolactone in combination with it obviated this downside. 

Yes, the study is small. Bigger numbers need to follow. But neither chlorthalidone nor spironolactone can be ignored in today’s antihypertensive armamentarium. Spironolactone indications are increasing. It has demonstrated efficacy in resistant hypertension complicating obstructive sleep apnea.4 Both agents, alone or in combination, have appealing indications.

Be on the lookout for more and larger studies.

References

1. Rutecki GW, Wright B. Chlorthalidone for hypertension: time to resuscitate an old, tried-and-true agent? June 13, 2012. http://www.consultantlive.com/display/article/10162/2089916.
2. Rutecki GW. Leaving a “legacy effect” on hypertension: a 22-year-old revisit to SHEP. July 12, 2012. http://www.consultantlive.com/display/article/10162/2089903.
3. Raheja P, Price A, Wang Z, et al. Spironolactone prevents chlorthalidone-induced sympathetic activation and insulin resistance in hypertensive patients. Hypertension. 2012 Jun 25; [Epub ahead of print].
4. Adams M, Bellone JM, Wright BM, Rutecki GW. Evaluation and pharmacologic approach to patients with resistant hypertension. Postgrad Med. 2012;124:74-82.
 

 

 

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by susan kweskin | July 18, 2012 2:03 PM EDT

Gregory Rutecki responds:

Thank you for the comment.

A recent publication evaluated 157 patients treated with spironolactone for heart failure. Complications/side effects were defined as: 1.) hyperkalemia 2.) elevated creatinine (> 2.0 meq/L) 3.) hyponatremia 4.) hypotension 5.) gynecomastia. 6/157 patients stopped spironolactone (3.8%). Only 1 patient stopped spironolactone because of gynecomastia (0.06%). No one on spironolactone required hospitalization or urgent treatment for side effects.

Although gynecomastia may result from spironolactone use, it is extremely rare. If it occurs, the patient can be treated with eplerenone. Not using spironolactone for an increasing list of indications only because gynecomastia might result would be "throwing the baby away with the bath water."

Goland S, Nuagolny V, Korbut Z, et. al. Appropriateness and complications of the use of spironolactone in patients treated in a heart failure clinic. Eur J Intern Med. 2011;22:424-427.

by Henry Izurieta | July 17, 2012 2:03 PM EDT

I agree with Chlorthalidone, however, Spironolactone has a side efect that is not good for men:GYNECOMASTIA

More On This Topic

Hypertension, Diabetes, and Kidney Disease: Predicting Serious Kidney Problems

Lower-Intensity Physical Activity Boosts Kidney Function

Leaving a “Legacy Effect” on Hypertension: A 22-Year-Old Revisit to SHEP

When Medicine Isn’t Enough: Renal Sympathetic Denervation and Resistant Hypertension

The Growing Need for Combination Rx in Hypertension

What’s New in Hypertension? A Contemporary Primer

Chlorthalidone for Hypertension: Time to Resuscitate an Old, Tried-and-True Agent?

Spironolactone and Chlorthalidone: A Novel and Effective Antihypertensive Regimen?

New Spin on Hypertension: Sequelae of Excess Glucocorticoids and Mineralocorticoids






 
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