The Significant Increase in Cardiovascular Disease Risk in APOEɛ4 Carriers is Evident Only in Men Who Smoke: Potential Relationship Between Reduced Antioxidant Status and ApoE4

Abstract

Summary: Data from 1668 men (316 cardiovascular disease events) from the Framingham Offspring Study was reanalysed, specifically examining APOE:smoking interactions. Overall hazard ratio (HR) for smoking was 1.95 (1.52, 2.50) compared to non‐smokers. Using ɛ3/3 as a referent group, in non‐smokers HRs for ɛ2 carriers (ɛ2+; 1.04 (0.61, 1.76) and ɛ4 carriers (ɛ4+; 1.04 (0.70, 1.54) showed no major risk increase. In smokers, HRs were 1.96 (1.26, 2.78) in ɛ3ɛ3 men, 3.46 (2.14, 5.60; p = 0.09 for interaction) in ɛ2+ and 3.81 (2.49, 5.84; p = 0.01 for interaction), with a significant interaction between daily cigarette consumption and APOE genotype on risk (p = 0.03). The potential mechanism for this APOEɛ4:smoking interaction was examined in a second study of 728 Caucasian patients with diabetes, where markers of reactive oxygen species were available. APOE genotype was not associated with plasma OX‐LDL or total antioxidant status (TAOS) in non‐smokers. However, in smokers ɛ4+ had 26.7% higher plasma OX‐LDL than other genotypes (APOE:smoking interaction p = 0.04), while ɛ2+ had 28.4% higher plasma TAOS than ɛ3ɛ3 and ɛ4+ combined (APOE:smoking interaction p = 0.026). Although direct extrapolation needs to be considered with caution, these results identify that the cardiovascular disease risk‐raising effect of ɛ4+ is confined to smokers, and a feasible mechanism is presented by the reduced antioxidant capacity/increased OX‐LDL of apoE4.