Effect of Magnesium Administration in Subjects With Family History of Diabetes or Metabolic Syndrome

University of Verona

Status and phase

Completed

Phase 4

Conditions

Family History of Diabetes

Family History of Metabolic Syndrome

Treatments

Drug: magnesium pidolate

Drug: placebo

Study type

Interventional

Funder types

Other

Identifiers

NCT01181830

CF_Mg_fam_MetS

Details and patient eligibility

About

Magnesium is the second most abundant ion in human cells and plays fundamental roles in several enzymatic reactions: it is involved in ATP production, in the phosphorylation of proteins, in glucose metabolism and in the contraction of cytoskeleton.

Several epidemiological studies demonstrated that low dietary magnesium intake is inversely associated with diabetes mellitus, hypertension and metabolic syndrome.

Magnesium could be related to important haemodynamic and metabolic anomalies: at vascular level it acts as an antagonist of calcium, especially in vascular smooth muscle cells, thus its deficit could enhance vascular contraction; with regard to glucose metabolism, magnesium is involved in the physiopathological mechanism of insulin resistance, through a reduction in cellular uptake of glucose. This condition and the subsequent compensatory hyperinsulinemia can ultimately lead to increased synthesis of proinflammatory cytokines and to endothelial dysfunction. Thus, magnesium depletion and subsequent alterations can increase the risk of developing vascular disease such as atherosclerosis and has been associated with cardiovascular events.

Several clinical trials have explored the possible beneficial effect of magnesium supplementation on blood pressure, plasma lipids and insulin resistance but the results are often contradictory. One of the possibilities for these unclear results could be that in some of them the interventions started too late when haemodynamic and metabolic changes are more difficult to revert.

The investigators hypothesis is that magnesium supplementation in a population at increased genetic risk of developing metabolic syndrome but without it could improve blood pressure and the other metabolic syndrome related components.

Thus, the aim of the present study is to evaluate the effect of oral supplementation of magnesium (16.2 mmol/day of magnesium pidolate) on metabolic syndrome's components in a sample of 15 subjects who are at increased risk of developing metabolic syndrome since have a positive familiar history of type II diabetes mellitus and/or metabolic syndrome(AHA/NHLBI criteria).

Enrollment

14 patients

Sex

All

Ages

18 to 50 years old

Volunteers

Accepts Healthy Volunteers

Inclusion criteria

positive family history of type II diabetes mellitus and/or metabolic syndrome(AHA/NHLBI criteria).

Exclusion criteria

any therapy related to metabolic syndrome (that is antihypertensive, anti diabetic, antilipemic drugs);
age < 18 years or >50 years;
previously diagnosed hypertension or immediate need for antihypertensive therapy (BP≥160/100);
diabetes mellitus (ADA criteria);
obesity (BMI>30Kg/m2);
Continuative use of NSAIDs, magnesium or vitamin supplements;
Hypermagnesaemia;
Previous cardio- or cerebrovascular events;
chronic kidney or liver or inflammatory or neoplastic disease;
gastrointestinal dysfunction with hypomotility;
active smoke (>5 cigarettes per day);
Impossibility to give informed consent.