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Departamento de Biología Funcional, Área de Fisiología, Facultad de Medicina. Universidad de Oviedo, Julián Clavería s/n, 33006, Oviedo, Spain and * Laboratorio de Análisis Clínicos, Instituto Nacional de Silicosis, Hospital Central de Asturias, 33006, Oviedo, Spain
2To whom correspondence should be addressed. E-mail: lasheras{at}uniovi.es.
Low selenium levels in humans have been associated with several pathologies; however, an earlier animal investigation found a direct association between Se intake and total plasma homocysteine (tHcy) concentrations. To date, the importance of serum selenium levels in association with tHcy in humans has not been determined. We evaluated the cross-sectional association of blood selenium concentrations with plasma tHcy and other determinants of this cardiovascular disease risk factor. We estimated protein intake and measured the blood status of selenium, tHcy, and several other related factors in serum such as folate, vitamin B-12, and creatinine. Serum selenium was inversely associated with tHcy, explaining 5.8% of tHcy variance with respect to 2.2% accounted for by serum folate. Furthermore, there was a 63% decreased risk of higher tHcy concentrations (>14 µmol/L) for subjects with serum selenium in the highest tertile (P = 0.013). We also found an inverse association of protein intake with tHcy in men (ß = 0.144; P = 0.036), which disappeared after controlling for serum Se concentrations (ß = 0.055; P = 0.003). In conclusion, selenium should be considered as a potential factor to lower tHcy. In addition, the described association between protein intake and homocysteine levels could be mediated by this trace element.
KEY WORDS: homocysteine selenium folate cardiovascular disease trace elements
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