: In a previous study which examined the distribution of apolipoprotein E genotypes and plasma levels in a sample of male coronary heart disease (CHD) patients and controls, we found a significant excess of the genotypes carrying APOE*4 allele in CHD men (18.2%) vs, controls (9.6%) and an association between the APOE*4 allele and the lowest concentrations of apoE. In the present investigation, we re-examined in the same samples two recently identified polymorphisms in the promoter region of APOE, -491A/T and -427T/C, which may alter the level of apoE expression. No differences in the distributions of the -491A/T genotypes and alleles were observed between cases and controls (-491*A=0.760 and 0.757 respectively). Polymorphism -427T/C showed in CHD patients an excess of -427*C allele (patients vs. controls = 0.123 vs. 0.074) and corresponding genotypes that was marginally significant. Stratification of the samples according to the presence/absence of APOE*4 showed that the excess of the -427*C allele concerned only CHD patients not carrying APOE*4 allele (patients vs. controls = 0.133 vs. 0.061; p=0.017). This result suggests that the presence of -427*C allele could represent a risk for developing CHD in subjects with E2/E2, E3/E2, and E3/E3 genotypes. Studies carried out on patients with Alzheimer's disease demonstrated that -491A/T and -427T/C polymorphisms affect the level of plasma apoE. In the present study, carried out on CHD patients and controls, the genetic variation at -427 and -491 sites of the APOE regulatory region had no apparent effect on apoE plasma concentration.

POLYMORPHISMS IN THE APOLIPOPROTEIN E GENE REGULATORY REGION IN RELATION TO CORONARY ARTERY DISEASE AND THEIR EFFECT ON APOLIPOPROTEIN E PLASMA LEVELS / Corbo, Rosa Maria; Scacchi, R.; Vilardo, T.; Ruggeri, M.. - In: CLINICAL CHEMISTRY AND LABORATORY MEDICINE. - ISSN 1434-6621. - STAMPA. - 39:(2001), pp. 2-6. [10.1515/CCLM.2001.002]

POLYMORPHISMS IN THE APOLIPOPROTEIN E GENE REGULATORY REGION IN RELATION TO CORONARY ARTERY DISEASE AND THEIR EFFECT ON APOLIPOPROTEIN E PLASMA LEVELS.

CORBO, Rosa Maria;
2001

Abstract

: In a previous study which examined the distribution of apolipoprotein E genotypes and plasma levels in a sample of male coronary heart disease (CHD) patients and controls, we found a significant excess of the genotypes carrying APOE*4 allele in CHD men (18.2%) vs, controls (9.6%) and an association between the APOE*4 allele and the lowest concentrations of apoE. In the present investigation, we re-examined in the same samples two recently identified polymorphisms in the promoter region of APOE, -491A/T and -427T/C, which may alter the level of apoE expression. No differences in the distributions of the -491A/T genotypes and alleles were observed between cases and controls (-491*A=0.760 and 0.757 respectively). Polymorphism -427T/C showed in CHD patients an excess of -427*C allele (patients vs. controls = 0.123 vs. 0.074) and corresponding genotypes that was marginally significant. Stratification of the samples according to the presence/absence of APOE*4 showed that the excess of the -427*C allele concerned only CHD patients not carrying APOE*4 allele (patients vs. controls = 0.133 vs. 0.061; p=0.017). This result suggests that the presence of -427*C allele could represent a risk for developing CHD in subjects with E2/E2, E3/E2, and E3/E3 genotypes. Studies carried out on patients with Alzheimer's disease demonstrated that -491A/T and -427T/C polymorphisms affect the level of plasma apoE. In the present study, carried out on CHD patients and controls, the genetic variation at -427 and -491 sites of the APOE regulatory region had no apparent effect on apoE plasma concentration.
2001
01 Pubblicazione su rivista::01a Articolo in rivista
POLYMORPHISMS IN THE APOLIPOPROTEIN E GENE REGULATORY REGION IN RELATION TO CORONARY ARTERY DISEASE AND THEIR EFFECT ON APOLIPOPROTEIN E PLASMA LEVELS / Corbo, Rosa Maria; Scacchi, R.; Vilardo, T.; Ruggeri, M.. - In: CLINICAL CHEMISTRY AND LABORATORY MEDICINE. - ISSN 1434-6621. - STAMPA. - 39:(2001), pp. 2-6. [10.1515/CCLM.2001.002]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/98684
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