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Genome Scans for Transmission Ratio Distortion Regions inMice

机译:基因组扫描中的透射比畸变区域老鼠

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摘要

Transmission ratio distortion (TRD) is the departure from the expected genotypic frequencies under Mendelian inheritance. This departure can be due to multiple physiological mechanisms during gametogenesis, fertilization, fetal and embryonic development, and early neonatal life. Although a few TRD loci have been reported in mouse, inheritance patterns have never been evaluated for TRD. In this article, we developed a Bayesian binomial model accounting for additive and dominant deviation TRD mechanisms. Moreover, this model was used to perform genome-wide scans for TRD quantitative trait loci (QTL) on six F2 mouse crosses involving between 296 and 541 mice and between 72 and 1854 genetic markers. Statistical significance of each model was checked at each genetic marker with Bayes factors. Genome scans revealed overdominance TRD QTL located in mouse chromosomes 1, 2, 12, 13, and 14 and additive TRD QTL in mouse chromosomes 2, 3, and 15, although these results did not replicate across mouse crosses. This research contributes new statistical tools for the analysis of specific genetic patterns involved in TRD in F2 populations, our results suggesting a relevant incidence of TRD phenomena in mouse with important implications for both statistical analysesand biological research.
机译:透射比失真(TRD)是孟德尔遗传下与预期基因型频率的偏离。这种偏离可能是由于在配子发生,受精,胎儿和胚胎发育以及新生儿早期生命期间存在多种生理机制。尽管已经在小鼠中报道了一些TRD基因座,但从未对TRD的遗传模式进行评估。在本文中,我们开发了一种贝叶斯二项式模型,该模型考虑了加性和显性偏差TRD机制。此外,此模型用于对六个F2小鼠杂交进行TRD定量性状基因座(QTL)的全基因组扫描,涉及296至541只小鼠和72至1854个遗传标记。使用贝叶斯因子在每个遗传标记处检查每个模型的统计显着性。基因组扫描显示位于小鼠染色体1、2、12、13和14上的TRD QTL占优势,而小鼠染色体2、3和15上的TRD QTL占优势,尽管这些结果在小鼠杂交中没有重复。这项研究为分析F2人群TRD中涉及的特定遗传模式提供了新的统计工具,我们的研究结果表明小鼠中TRD现象的相关发生率对这两种统计分析都具有重要意义和生物学研究。

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