Enhanced methods for unbiased deep sequencing of Lassa and Ebola RNA viruses from clinical and biological samples

Matranga Christian B.; Andersen Kristian G.; Winnicki Sarah; Busby Michele; Gladden Adrianne D.; Tewhey Ryan; Stremlau Matthew; Berlin Aaron; Gire Stephen K.; England Eleina; Moses Lina M.; Mikkelsen Tarjei S.; Odia Ikponmwonsa; Ehiane Philomena E.; Folarin Onikepe; Goba Augustine; Kahn S. Humarr; Grant Donald S.; Honko Anna; Hensley Lisa; Happi Christian; Garry Robert F.; Malboeuf Christine M.; Birren Bruce W.; Gnirke Andreas; Levin Joshua Z.; Sabeti Pardis C.

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Enhanced methods for unbiased deep sequencing of Lassa and Ebola RNA viruses from clinical and biological samples

机译：从临床和生物学样本对Lassa和埃博拉RNA病毒进行无偏深测序的增强方法

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We have developed a robust RNA sequencing method for generating complete de novo assemblies with intra-host variant calls of Lassa and Ebola virus genomes in clinical and biological samples. Our method uses targeted RNase H-based digestion to remove contaminating poly(rA) carrier and ribosomal RNA. This depletion step improves both the quality of data and quantity of informative reads in unbiased total RNA sequencing libraries. We have also developed a hybrid-selection protocol to further enrich the viral content of sequencing libraries. These protocols have enabled rapid deep sequencing of both Lassa and Ebola virus and are broadly applicable to other viral genomics studies.

机译：我们已经开发了一种可靠的RNA测序方法，可在临床和生物样品中生成带有Lassa和埃博拉病毒基因组的宿主内变体的完整从头组装。我们的方法使用针对性的基于RNase H的消化来去除污染的poly（rA）载体和核糖体RNA。此消耗步骤可改善无偏总RNA测序文库中数据的质量和信息读取的数量。我们还开发了一种杂交选择方案，以进一步丰富测序文库的病毒含量。这些协议已使拉萨和埃博拉病毒的快速深度测序成为可能，并广泛适用于其他病毒基因组学研究。

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《Genome Biology》 |2014年第11期|共12页
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Matranga Christian B.; Andersen Kristian G.; Winnicki Sarah; Busby Michele; Gladden Adrianne D.; Tewhey Ryan; Stremlau Matthew; Berlin Aaron; Gire Stephen K.; England Eleina; Moses Lina M.; Mikkelsen Tarjei S.; Odia Ikponmwonsa; Ehiane Philomena E.; Folarin Onikepe; Goba Augustine; Kahn S. Humarr; Grant Donald S.; Honko Anna; Hensley Lisa; Happi Christian; Garry Robert F.; Malboeuf Christine M.; Birren Bruce W.; Gnirke Andreas; Levin Joshua Z.; Sabeti Pardis C.;
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1. Enhanced methods for unbiased deep sequencing of Lassa and Ebola RNA viruses from clinical and biological samples [J] . Matranga Christian B., Andersen Kristian G., Winnicki Sarah, Genome Biology . 2014,第11期

机译：从临床和生物学样本对Lassa和埃博拉RNA病毒进行无偏深测序的增强方法
2. Complete viral genome sequence and discovery of novel viruses by deep sequencing of small RNAs: a generic method for diagnosis, discovery and sequencing of viruses. [J] . Kreuze JF, Perez A, Untiveros M Virology . 2009,第1期

机译：通过小RNA的深度测序来完成病毒基因组序列和发现新病毒：这是诊断，发现和测序病毒的通用方法。
3. Physicochemical inactivation of Lassa, Ebola, and Marburg viruses and effect on clinical laboratory analyses. [J] . S W Mitchell, J B McCormick Journal of Clinical Microbiology . 1984,第3期

机译：拉沙病毒，埃博拉病毒和马尔堡病毒的物理化学灭活及其对临床实验室分析的影响。
4. Next generation sequencing and bioinformatic approaches to identify dengue viruses from non-invasive clinical samples [C] . Xuezheng Ma, Shuru Chen, Liping Zhang, International Conference on Computational Intelligence and Applications . 2017

机译：下一代测序和生物信息学方法可从非侵入性临床样品中鉴定登革热病毒
5. DEVELOPMENT OF AN ELISA SYSTEM FOR THE DETECTION AND STRAIN IDENTIFICATION OF LASSA AND EBOLA VIRUSES USING MONOCLONAL ANTIBODIES. [D] . GETCHELL, JANE PENTLAND. 1983

机译：ELISA方法的开发，用于使用单克隆抗体检测和鉴定LASSA和埃博拉病毒。
6. Enhanced methods for unbiased deep sequencing of Lassa and Ebola RNA viruses from clinical and biological samples [O] . Christian B Matranga, Kristian G Andersen, Sarah Winnicki, 2014

机译：从临床和生物学样品对Lassa和埃博拉RNA病毒进行无偏深测序的增强方法
7. Enhanced methods for unbiased deep sequencing of Lassa and Ebola RNA viruses from clinical and biological samples [O] . 2014

机译：从临床和生物学样品对Lassa和埃博拉RNA病毒进行无偏深测序的增强方法

Enhanced methods for unbiased deep sequencing of Lassa and Ebola RNA viruses from clinical and biological samples

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