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APOLIPOPROTEIN E4 PHENOTYPE IS NOT AN IMPORTANT RISK FACTOR FOR CORONARY HEART-DISEASE OR STROKE IN ELDERLY SUBJECTS

被引:104
作者
KUUSISTO, J
MYKKANEN, L
KERVINEN, K
KESANIEMI, YA
LAAKSO, M
机构
[1] KUOPIO UNIV HOSP,DEPT MED,SF-70210 KUOPIO,FINLAND
[2] OULU UNIV HOSP,DEPT INTERNAL MED,OULU,FINLAND
[3] UNIV OULU,BIOCTR,OULU,FINLAND
来源
ARTERIOSCLEROSIS THROMBOSIS AND VASCULAR BIOLOGY | 1995年 / 15卷 / 09期
关键词
APOLIPOPROTEIN E; CORONARY DISEASE; STROKE; CARDIOVASCULAR DISEASE;
D O I
10.1161/01.ATV.15.9.1280
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
The allele e4 (ape e4) of apolipoprotein E (ape E) has been associated with an increased risk for coronary heart disease (CHD) in cross-sectional studies in middle-aged subjects. We investigated the risk of CHD and stroke with respect to the number of apo e4 alleles in a prospective study of a Finnish nondiabetic cohort including 1067 subjects 65 to 74 years old at baseline. During the 3.5-year follow-up, CHD mortality was 2.8%, total CHD incidence 6.9%, and the cumulative occurrence of CHD (prevalence at baseline and the 3.5-year incidence combined) 17.0%. The incidence of stroke was 3.4%, and the cumulative occurrence of stroke was 6.0%. The CHD mortality was 3.4% in subjects with no apo e4 allele (n = 734), 1.7% in those with one apo e4 allele (n = 296), and O% in subjects with two apo e4 alleles (n = 37) (P = NS between the three groups). The incidence of CHD according to the number of apo e4 alleles was 6.9% (no apo e4 alleles), 7.4% (one apo e4 allele), and 2.7% (two apo e4 alleles), and the cumulative occurrence of CHD was 16.5%, 18.6%, and 13.5%, respectively (P = NS). The incidence of stroke was 3.8% in subjects with no apo e4 allele, 2.7% in those with one apo e4 allele, and 0% in those with two apo e4 alleles (P = NS). The cumulative occurrence of stroke was 6.0%, 6.4%, and 2.7%, respectively (P = NS). In conclusion, in contrast to middle-aged subjects, the risk of cardiovascular disease in elderly subjects with apo e4 is not increased. Consequently, the allele e4 of apo E cannot be regarded as an important risk factor for CHD or stroke in the elderly.
引用
收藏
页码:1280 / 1286
页数:7
相关论文
共 62 条
[31]  
MYKKANEN K, 1990, DIABETES CARE, V11, P1099
[32]  
MYKKANEN L, 1991, ATHEROSCLEROSIS, V88, P153, DOI 10.1016/0021-9150(91)90077-G
[33]   LIPOPROTEINS AND THEIR GENETIC-VARIATION IN SUBJECTS WITH AND WITHOUT ANGIOGRAPHICALLY VERIFIED CORONARY-ARTERY DISEASE [J].
NIEMINEN, MS ;
MATTILA, KJ ;
AALTOSETALA, K ;
KUUSI, T ;
KONTULA, K ;
KAUPPINENMAKELIN, R ;
EHNHOLM, C ;
JAUHIAINEN, M ;
VALLE, M ;
TASKINEN, MR .
ARTERIOSCLEROSIS AND THROMBOSIS, 1992, 12 (01) :58-69
[34]  
OBRIEN KD, 1994, AM J PATHOL, V144, P538
[35]   LIPOPROTEIN AND APOLIPOPROTEIN PROFILE IN MEN WITH ISCHEMIC STROKE - ROLE OF LIPOPROTEIN(A), TRIGLYCERIDE-RICH LIPOPROTEINS, AND APOLIPOPROTEIN E POLYMORPHISM [J].
PEDROBOTET, J ;
SENTI, M ;
NOGUES, X ;
RUBIESPRAT, J ;
ROQUER, J ;
DOLHABERRIAGUE, L ;
OLIVE, J .
STROKE, 1992, 23 (11) :1556-1562
[36]   COMPARISON OF DIFFERENT ANALYTICAL AND PRECIPITATION METHODS FOR DIRECT ESTIMATION OF SERUM HIGH-DENSITY LIPOPROTEIN CHOLESTEROL [J].
PENTTILA, IM ;
VOUTILAINEN, E ;
LAITINEN, P ;
JUUTILAINEN, P .
SCANDINAVIAN JOURNAL OF CLINICAL & LABORATORY INVESTIGATION, 1981, 41 (04) :353-360
[37]   APOLIPOPROTEIN-E POLYMORPHISM AND ALZHEIMERS-DISEASE [J].
POIRIER, J ;
DAVIGNON, J ;
BOUTHILLIER, D ;
KOGAN, S ;
BERTRAND, P ;
GAUTHIER, S .
LANCET, 1993, 342 (8873) :697-699
[38]  
Prineas R, 1982, MINNESOTA CODE MANUA
[39]  
Rose GA, 1982, CARDIOVASCULAR SURVE
[40]   APOLIPOPROTEIN-E-EPSILON-4 ALLELE DISTRIBUTIONS IN LATE-ONSET ALZHEIMERS-DISEASE AND IN OTHER AMYLOID-FORMING DISEASES [J].
SAUNDERS, AM ;
SCHMADER, K ;
BREITNER, JCS ;
BENSON, MD ;
BROWN, WT ;
GOLDFARB, L ;
GOLDGABER, D ;
MANWARING, MG ;
SZYMANSKI, MH ;
MCCOWN, N ;
DOLE, KC ;
SCHMECHEL, DE ;
STRITTMATTER, WJ ;
PERICAKVANCE, MA ;
ROSES, AD .
LANCET, 1993, 342 (8873) :710-711
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