Previous studies by our group have identified ionic aspects of insulin resistance in hypertension, in which cellular responses to insulin were influenced by the basal intracellular ionic environment-the lower the cytosolic free magnesium (Mg-i), the less Mg-i increased following insulin stimulation. To investigate whether this ionic insulin resistance represents a more general abnormality of cellular responsiveness in hypertension, we studied Mgi responses to nonhormonal signals such as hyperglycemia (15 mmol/L) and used P-31-nuclear magnetic resonance (NMR) spectroscopy to measure Mg-i in erythrocytes from normal (NL, n= 14) and hypertensive (HTN, n= 12) subjects before and 30, 60, 120, and 180 minutes after in vitro glucose incubations. Basal Mg-i levels were significantly lower in HTN subjects than in NL subjects (169 +/- 10 versus 205 +/-8 mu mol (.) L (-1), P <0.01). In NL cells, hyperglycemia significantly lowered Mg-i, from 205 +/-8 mu mol (.) L-1 (basal, T = 0) to 181 +/-8, 162 +/-6, 152 +/-7, and 175 +/-9 mu mol (.) L-1 (T = 30, 60, 120, and 180, respectively; P <0.005 versus T=0 at all times). In HTN cells, maximal Mg-i responses to hyperglycemia were blunted, from 169 +/- 10 mu mol (.) L-1 (basal, T=0) to 170 +/- 11, 179 +/- 12, 181 +/- 14, and 17315 mu mol (.) L-1 (T=30, 60, 120, and 180, respectively; P=NS versus T=0 at all times). For all subjects, Mg-i responses to hyperglycemia were closely related to basal Mg-i levels: the higher the Mg-i, the greater the response (n=26, r=0.620, P <0.001). Thus, (1) erythrocytes from hypertensive vis-a-vis normotensive subjects are resistant to the ionic effects of extracellular hyperglycemia on Mg-i levels, and (2) cellular ionic responses to glucose depend oil the basal Mg-i environment. Altogether, these data support a role for altered extracellular glucose levels in regulating cellular magnesium metabolism and also suggest the importance of ionic factors in determining cellular responsiveness to nonhormonal as well as hormonal signals.
Altered cellular magnesium responsiveness to hyperglycemia in hypertensive subjects
Dominguez L.J.;
2001-01-01
Abstract
Previous studies by our group have identified ionic aspects of insulin resistance in hypertension, in which cellular responses to insulin were influenced by the basal intracellular ionic environment-the lower the cytosolic free magnesium (Mg-i), the less Mg-i increased following insulin stimulation. To investigate whether this ionic insulin resistance represents a more general abnormality of cellular responsiveness in hypertension, we studied Mgi responses to nonhormonal signals such as hyperglycemia (15 mmol/L) and used P-31-nuclear magnetic resonance (NMR) spectroscopy to measure Mg-i in erythrocytes from normal (NL, n= 14) and hypertensive (HTN, n= 12) subjects before and 30, 60, 120, and 180 minutes after in vitro glucose incubations. Basal Mg-i levels were significantly lower in HTN subjects than in NL subjects (169 +/- 10 versus 205 +/-8 mu mol (.) L (-1), P <0.01). In NL cells, hyperglycemia significantly lowered Mg-i, from 205 +/-8 mu mol (.) L-1 (basal, T = 0) to 181 +/-8, 162 +/-6, 152 +/-7, and 175 +/-9 mu mol (.) L-1 (T = 30, 60, 120, and 180, respectively; P <0.005 versus T=0 at all times). In HTN cells, maximal Mg-i responses to hyperglycemia were blunted, from 169 +/- 10 mu mol (.) L-1 (basal, T=0) to 170 +/- 11, 179 +/- 12, 181 +/- 14, and 17315 mu mol (.) L-1 (T=30, 60, 120, and 180, respectively; P=NS versus T=0 at all times). For all subjects, Mg-i responses to hyperglycemia were closely related to basal Mg-i levels: the higher the Mg-i, the greater the response (n=26, r=0.620, P <0.001). Thus, (1) erythrocytes from hypertensive vis-a-vis normotensive subjects are resistant to the ionic effects of extracellular hyperglycemia on Mg-i levels, and (2) cellular ionic responses to glucose depend oil the basal Mg-i environment. Altogether, these data support a role for altered extracellular glucose levels in regulating cellular magnesium metabolism and also suggest the importance of ionic factors in determining cellular responsiveness to nonhormonal as well as hormonal signals.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
