疾病特异性前瞻性家庭研究队列增加了家族风险。

John L Hopper
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引用次数: 36

摘要

大多数常见病表现出家族聚集性;患病人群亲属的风险与未患病人群亲属的风险之比(家族风险比)> 1。这意味着亲属之间存在潜在的遗传和/或环境风险因素。这种潜在的“家族风险概况”的风险梯度通常很强,可以从家族史和测量的家族风险因素中预测出来。在乘法模型下,处于家族风险的前25%人群的风险与处于家族风险的后25%人群的风险之比(四分位间风险梯度)比家族风险比大一个数量级。如果一级亲属的家族风险比= 2,就家族风险概况而言:(a)上层四分位数的人的风险将是下层四分位数的20倍以上;(b)大约90%的疾病将发生在中位数以上的人群中。因此,从历史上看,流行病学将病例与具有不同潜在家族风险特征的对照进行比较。如果存在基因-环境和基因-基因的相互作用,环境和基因的影响可能会对家族风险增加的人更强。将对照与家族风险情况更匹配的研究可能会提供更多信息,特别是如果病例和对照都是过度抽样以增加家族风险。前瞻性家庭研究队列(ProF-SC)设计涉及一系列家庭风险概况的人,为流行病学,遗传,行为,心理社会和健康利用研究提供了这样的资源。前瞻性方面为风险估计提供了可信度。家族方面允许基于家族的设计,匹配未测量的因素,调整潜在的家族风险概况,并加强队列维护。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Disease-specific prospective family study cohorts enriched for familial risk.

Disease-specific prospective family study cohorts enriched for familial risk.

Disease-specific prospective family study cohorts enriched for familial risk.

Most common diseases demonstrate familial aggregation; the ratio of the risk for relatives of affected people to the risk for relatives of unaffected people (the familial risk ratio)) > 1. This implies there are underlying genetic and/or environmental risk factors shared by relatives. The risk gradient across this underlying 'familial risk profile', which can be predicted from family history and measured familial risk factors, is typically strong. Under a multiplicative model, the ratio of the risk for people in the upper 25% of familial risk to the risk for those in the lower 25% (the inter-quartile risk gradient) is an order of magnitude greater than the familial risk ratio. If familial risk ratio = 2 for first-degree relatives, in terms of familial risk profile: (a) people in the upper quartile will be at more than 20 times the risk of those in the lower quartile; and (b) about 90% of disease will occur in people above the median. Historically, therefore, epidemiology has compared cases with controls dissimilar for underlying familial risk profile. Were gene-environment and gene-gene interactions to exist, environmental and genetic effects could be stronger for people with increased familial risk profile. Studies in which controls are better matched to cases for familial risk profile might be more informative, especially if both cases and controls are over-sampled for increased familial risk. Prospective family study cohort (ProF-SC) designs involving people across a range of familial risk profile provide such a resource for epidemiological, genetic, behavioural, psycho-social and health utilisation research. The prospective aspect gives credibility to risk estimates. The familial aspect allows family-based designs, matching for unmeasured factors, adjusting for underlying familial risk profile, and enhanced cohort maintenance.

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