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血浆载脂蛋白B的家族相似性:南希研究

Familial resemblance of plasma apolipoprotein B: the Nancy study.

作者信息

Tiret L, Steinmetz J, Herbeth B, Visvikis S, Rakotovao R, Ducimetiere P, Cambien F

机构信息

Institut National de la Santé et de la Recherche Médicale (INSERM) U258, Hôpital Broussais, Paris, France.

出版信息

Genet Epidemiol. 1990;7(3):187-97. doi: 10.1002/gepi.1370070303.

DOI:10.1002/gepi.1370070303
PMID:2369998
Abstract

The familial resemblance of plasma apolipoprotein B (apo B) was investigated in a sample of 102 families including 419 members who volunteered for a free health checkup in the Preventive Center of Vandoeuvre-lès-Nancy, France. The mean levels (+/- SD) of apo B were 141.0 (+/- 32.6), 121.8 (+/- 27.7), and 98.6 (+/- 22.6) mg/dl in fathers, mothers, and offspring, respectively. The familial correlations were 0.04, 0.13, 0.21 (P less than .01), and 0.47 (P less than .001) between spouses, father-offspring, mother-offspring, and siblings, respectively, after adjustment on age, body mass index, and sex. A genetic analysis was performed using the approach proposed by Bonney, which indicated that a recessive and a dominant major-locus model appeared nearly equally supported by the data. Under the recessive model, the frequency q of the most common allele was estimated as 0.825, with a mean difference of 60.4 mg/dl between high and low homozygotes. Under the dominant model, q was estimated as 0.875, with a mean increase of 34.2 mg/dl in heterozygotes and high homozygotes. However, the hypothesis of Mendelian transmission and the environmental hypothesis could not be formally tested because of great numeric difficulties encountered in the estimation of the three transmission probabilities. Given these analytical restrictions, we cannot conclude in favor of a major locus influencing apo B level in our population, even though the evidence is suggestive. The genetic heterogeneity underlying the familial aggregation of apo B level, suggested by several recent publications, might explain the difficulty in discerning a single major locus in a population sample of small nuclear families, not ascertained through patients enriching the sample in high values of apo B. These findings call into question the relevance of the approach through "healthy" populations in the search for major loci influencing biological traits.

摘要

在法国南锡附近旺德厄夫尔预防中心,对102个家庭(共419名成员)进行了免费健康检查,以此研究血浆载脂蛋白B(apo B)的家族相似性。父亲、母亲和后代的apo B平均水平(±标准差)分别为141.0(±32.6)、121.8(±27.7)和98.6(±22.6)mg/dl。在对年龄、体重指数和性别进行调整后,配偶之间、父子之间、母子之间以及兄弟姐妹之间的家族相关性分别为0.04、0.13、0.21(P<0.01)和0.47(P<0.001)。采用邦尼提出的方法进行了遗传分析,结果表明隐性和显性主基因座模型得到的数据支持程度几乎相同。在隐性模型下,最常见等位基因的频率q估计为0.825,高、低纯合子之间的平均差异为60.4 mg/dl。在显性模型下,q估计为0.875,杂合子和高纯合子的平均增加量为34.2 mg/dl。然而,由于在估计三种传递概率时遇到了很大的数值困难,孟德尔遗传传递假说和环境假说无法得到正式检验。鉴于这些分析限制,尽管有证据提示,但我们不能得出在我们的人群中存在影响apo B水平主基因座的结论。最近的几篇出版物表明,apo B水平家族聚集背后的遗传异质性,可能解释了在小型核心家庭的人群样本中难以识别单个主基因座的原因,该样本并非通过apo B高值患者富集而来。这些发现质疑了通过“健康”人群寻找影响生物学性状主基因座方法的相关性。

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引用本文的文献

1
The polymorphism ApoB/4311 in patients with myocardial infarction and controls: the ECTIM Study.
Hum Genet. 1992 May;89(2):169-75. doi: 10.1007/BF00217118.
2
Pedigree and sib-pair linkage analysis suggest the apolipoprotein B gene is not the major gene influencing plasma apolipoprotein B levels.系谱和同胞对连锁分析表明,载脂蛋白B基因不是影响血浆载脂蛋白B水平的主要基因。
Am J Hum Genet. 1992 May;50(5):1038-45.