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SeqSIMLA2:在用户指定的谱系结构中模拟考虑共享环境效应的相关数量性状。

SeqSIMLA2: simulating correlated quantitative traits accounting for shared environmental effects in user-specified pedigree structure.

作者信息

Chung Ren-Hua, Tsai Wei-Yun, Hsieh Chang-Hsun, Hung Kuan-Yi, Hsiung Chao A, Hauser Elizabeth R

机构信息

Division of Biostatistics and Bioinformatics, Institute of Population Health Sciences, National Health Research Institutes, Zhunan, Miaoli, Taiwan.

出版信息

Genet Epidemiol. 2015 Jan;39(1):20-4. doi: 10.1002/gepi.21850. Epub 2014 Sep 22.

Abstract

Simulation tools that simulate sequence data in unrelated cases and controls or in families with quantitative traits or disease status are important for genetic studies. The simulation tools can be used to evaluate the statistical power for detecting the causal variants when planning a genetic epidemiology study, or to evaluate the statistical properties for new methods. We previously developed SeqSIMLA version 1 (SeqSIMLA1), which simulates family or case-control data with a disease or quantitative trait model. SeqSIMLA1, and several other tools that simulate quantitative traits, do not specifically model the shared environmental effects among relatives on a trait. However, shared environmental effects are commonly observed for some traits in families, such as body mass index. SeqSIMLA1 simulates a fixed three-generation family structure. However, it would be ideal to simulate prespecified pedigree structures for studies involving large pedigrees. Thus, we extended SeqSIMLA1 to create SeqSIMLA2, which can simulate correlated traits and considers the shared environmental effects. SeqSIMLA2 can also simulate prespecified large pedigree structures. There are no restrictions on the number of individuals that can be simulated in a pedigree. We used a blood pressure example to demonstrate that SeqSIMLA2 can simulate realistic correlation structures between the systolic and diastolic blood pressure among relatives. We also showed that SeqSIMLA2 can simulate large pedigrees with large chromosomal regions in a reasonable time frame.

摘要

在无关个体的病例与对照中,或在具有数量性状或疾病状态的家系中模拟序列数据的模拟工具,对基因研究而言至关重要。这些模拟工具可用于在规划基因流行病学研究时评估检测因果变异的统计效能,或评估新方法的统计学特性。我们之前开发了SeqSIMLA版本1(SeqSIMLA1),它能通过疾病或数量性状模型模拟家系或病例对照数据。SeqSIMLA1以及其他一些模拟数量性状的工具,并未专门对亲属间性状的共享环境效应进行建模。然而,家系中某些性状,如体重指数,通常会观察到共享环境效应。SeqSIMLA1模拟固定的三代家系结构。然而,对于涉及大型家系的研究,模拟预先指定的系谱结构会更理想。因此,我们对SeqSIMLA1进行扩展,创建了SeqSIMLA2,它能够模拟相关性状并考虑共享环境效应。SeqSIMLA2还能模拟预先指定的大型系谱结构。对系谱中可模拟的个体数量没有限制。我们以血压为例,证明SeqSIMLA2能够模拟亲属间收缩压和舒张压之间真实的相关结构。我们还表明,SeqSIMLA2能够在合理的时间框架内模拟具有大染色体区域的大型家系。

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