Relation of Cellular Potassium to Other Mineral Ions in Hypertension and Diabetes

Author:

Resnick Lawrence M.1,Barbagallo Mario1,Dominguez Ligia J.1,Veniero Joseph M.1,Nicholson J. P.1,Gupta Raj K.1

Affiliation:

1. From the Hypertension Center, New York Presbyterian Hospital-Cornell Medical Center (L.M.R., M.B., J.P.N.), New York, New York; Institute of Internal Medicine and Geriatrics, University of Palermo (M.B., L.J.D.), Palermo, Italy; and Department of Physiology and Biophisics, Albert Einstein College of Medicine (J.M.V., R.K.G.), Bronx, New York.

Abstract

Abstract — To investigate the role of intracellular potassium (K i )and other ions in hypertension and diabetes, we utilized 39 K-, 23 Na-, 31 P-, and 19 F-nuclear magnetic resonance (NMR) spectroscopy to measure K i , intracellular sodium (Na i ), intracellular free magnesium (Mg i ), and cytosolic free calcium (Ca i ), respectively, in red blood cells of fasting normotensive nondiabetic control subjects (n=10), untreated (n=13) and treated (n=14) essential hypertensive subjects, and diabetic subjects (n=5). In 12 subjects (6 hypertensive and 6 normotensive controls), ions were also measured before and after the acute infusion of 1 L of normal saline. Compared with those in controls (K i =148±2.0 mmol/L), K i levels were significantly lower in hypertensive (132.2±2.9 mmol/L, sig=0.05) and in type 2 diabetic subjects (121.2±6.8 mmol/L, sig=0.05). K i was higher in treated hypertensives than in untreated hypertensives (139±3.1 mmol/L, sig=0.05) but was still lower than in normals. Although no significant relation was observed between basal K i and Na i values, saline infusion elevated Na i ( P <0.01) and reciprocally suppressed K i levels (142±2.4 to 131±2.2 mmol/L, P <0.01). K i was strongly and inversely related to Ca i ( r =−0.846, P <0.001), and was directly related to Mg i ( r =0.664, P <0.001). We conclude that (1) K i depletion is a common feature of essential hypertension and type 2 diabetes, (2) treatment of hypertension at least partially restores K i levels toward normal, and (3) fasting steady-state K i levels are closely linked to Ca i and Mg i homeostasis. Altogether, these results emphasize the similar and coordinate nature of ionic defects in diabetes and hypertension and suggest that their interpretation requires an understanding of their interaction.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Internal Medicine

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