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无组装的单分子测序从自然微生物群落中恢复完整的病毒基因组。

Assembly-free single-molecule sequencing recovers complete virus genomes from natural microbial communities.

机构信息

Oxford Nanopore Technologies Incorporated, San Francisco, California 94080, USA.

Daniel K. Inouye Center for Microbial Oceanography: Research and Education, University of Hawaii, Honolulu, Hawaii 96822, USA.

出版信息

Genome Res. 2020 Mar;30(3):437-446. doi: 10.1101/gr.251686.119. Epub 2020 Feb 19.

Abstract

Viruses are the most abundant biological entities on Earth and play key roles in host ecology, evolution, and horizontal gene transfer. Despite recent progress in viral metagenomics, the inherent genetic complexity of virus populations still poses technical difficulties for recovering complete virus genomes from natural assemblages. To address these challenges, we developed an assembly-free, single-molecule nanopore sequencing approach, enabling direct recovery of complete virus genome sequences from environmental samples. Our method yielded thousands of full-length, high-quality draft virus genome sequences that were not recovered using standard short-read assembly approaches. Additionally, our analyses discriminated between populations whose genomes had identical direct terminal repeats versus those with circularly permuted repeats at their termini, thus providing new insight into native virus reproduction and genome packaging. Novel DNA sequences were discovered, whose repeat structures, gene contents, and concatemer lengths suggest they are phage-inducible chromosomal islands, which are packaged as concatemers in phage particles, with lengths that match the size ranges of co-occurring phage genomes. Our new virus sequencing strategy can provide previously unavailable information about the genome structures, population biology, and ecology of naturally occurring viruses and viral parasites.

摘要

病毒是地球上最丰富的生物实体,在宿主生态、进化和水平基因转移中发挥着关键作用。尽管病毒宏基因组学最近取得了进展,但病毒群体固有的遗传复杂性仍然给从自然组合中恢复完整病毒基因组带来了技术困难。为了解决这些挑战,我们开发了一种无组装、单分子纳米孔测序方法,能够直接从环境样本中恢复完整的病毒基因组序列。我们的方法产生了数千个全长、高质量的病毒基因组草图序列,这些序列无法通过标准的短读序列组装方法获得。此外,我们的分析区分了基因组具有相同直接末端重复序列的群体与具有环状置换重复序列的群体,从而为了解天然病毒复制和基因组包装提供了新的见解。还发现了新的 DNA 序列,其重复结构、基因含量和串联长度表明它们是噬菌体诱导的染色体岛,这些染色体岛作为噬菌体颗粒中的串联体被包装,长度与共存噬菌体基因组的大小范围相匹配。我们的新病毒测序策略可以提供关于自然发生的病毒和病毒寄生虫的基因组结构、种群生物学和生态学的以前无法获得的信息。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6dcb/7111524/a8c58b4dd9ef/437f01.jpg

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