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A simulation study of sample size for DNA barcoding

机译:DNA条形码的样本量模拟研究

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摘要

AbstractFor some groups of organisms, DNA barcoding can provide a useful tool in taxonomy, evolutionary biology, and biodiversity assessment. However, the efficacy of DNA barcoding depends on the degree of sampling per species, because a large enough sample size is needed to provide a reliable estimate of genetic polymorphism and for delimiting species. We used a simulation approach to examine the effects of sample size on four estimators of genetic polymorphism related to DNA barcoding: mismatch distribution, nucleotide diversity, the number of haplotypes, and maximum pairwise distance. Our results showed that mismatch distributions derived from subsamples of ≥20 individuals usually bore a close resemblance to that of the full dataset. Estimates of nucleotide diversity from subsamples of ≥20 individuals tended to be bell-shaped around that of the full dataset, whereas estimates from smaller subsamples were not. As expected, greater sampling generally led to an increase in the number of haplotypes. We also found that subsamples of ≥20 individuals allowed a good estimate of the maximum pairwise distance of the full dataset, while smaller ones were associated with a high probability of underestimation. Overall, our study confirms the expectation that larger samples are beneficial for the efficacy of DNA barcoding and suggests that a minimum sample size of 20 individuals is needed in practice for each population.
机译:摘要对于某些生物体,DNA条形码可以为分类学,进化生物学和生物多样性评估提供有用的工具。但是,DNA条形码的效率取决于每个物种的采样程度,因为需要足够大的样本量才能提供可靠的遗传多态性估计值并为物种定界。我们使用一种模拟方法来检查样本大小对与DNA条形码相关的遗传多态性的四个估计量的影响:错配分布,核苷酸多样性,单倍型数量和最大成对距离。我们的结果表明,来自≥20个人的子样本的失配分布通常与整个数据集的分布非常相似。来自≥20个个体的子样本的核苷酸多样性估计值倾向于在整个数据集的周围呈钟形,而来自较小子样本的估计值则不是。如预期的那样,更多的采样通常导致单倍型数量的增加。我们还发现,≥20个人的子样本可以很好地估计整个数据集的最大成对距离,而较小的样本与被低估的可能性很高。总体而言,我们的研究证实了对更大样本有益于DNA条形码编码的期望,并建议在实践中每个人群至少需要20个人的样本量。

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