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首页> 外文期刊>Environmental microbiology >Wrinkles in the rare biosphere: pyrosequencing errors can lead to artificial inflation of diversity estimates
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Wrinkles in the rare biosphere: pyrosequencing errors can lead to artificial inflation of diversity estimates

机译:稀有生物圈中的皱纹:焦磷酸测序错误可能导致人为膨胀的多样性估计值

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摘要

P>Massively parallel pyrosequencing of the small subunit (16S) ribosomal RNA gene has revealed that the extent of rare microbial populations in several environments, the 'rare biosphere', is orders of magnitude higher than previously thought. One important caveat with this method is that sequencing error could artificially inflate diversity estimates. Although the per-base error of 16S rDNA amplicon pyrosequencing has been shown to be as good as or lower than Sanger sequencing, no direct assessments of pyrosequencing errors on diversity estimates have been reported. Using only Escherichia coli MG1655 as a reference template, we find that 16S rDNA diversity is grossly overestimated unless relatively stringent read quality filtering and low clustering thresholds are applied. In particular, the common practice of removing reads with unresolved bases and anomalous read lengths is insufficient to ensure accurate estimates of microbial diversity. Furthermore, common and reproducible homopolymer length errors can result in relatively abundant spurious phylotypes further confounding data interpretation. We suggest that stringent quality-based trimming of 16S pyrotags and clustering thresholds no greater than 97% identity should be used to avoid overestimates of the rare biosphere.
机译:P>小亚基(16S)核糖体RNA基因的大规模平行焦磷酸测序表明,在几种环境(“稀有生物圈”)中稀有微生物种群的数量级比以前认为的高几个数量级。使用此方法的一个重要警告是,测序错误可能人为地增加了多样性估计。尽管已显示16S rDNA扩增子焦磷酸测序的每碱基错误与Sanger测序一样好或更低,但尚无直接评估焦磷酸测序错误的多样性估计的报道。仅使用大肠杆菌MG1655作为参考模板,我们发现除非应用了相对严格的读取质量过滤和较低的聚类阈值,否则16S rDNA多样性被高估了。特别是,删除具有未解析碱基和异常读取长度的读取的常规做法不足以确保准确估计微生物多样性。此外,常见且可重现的均聚物长度错误可能导致相对丰富的假系统型,进一步混淆了数据解释。我们建议对16S高温标签进行严格的基于质量的修剪和不超过97%同一性的聚类阈值,以避免对稀有生物圈的高估。

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