Realizing the potential of full-length transcriptome sequencing | Zendy

Ashley Byrne | Zendy; Charles N. Cole | Zendy; Roger Volden | Zendy; Christopher Vollmers | Zendy

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Realizing the potential of full-length transcriptome sequencing

Author(s) -

Ashley Byrne,

Charles N. Cole,

Roger Volden,

Christopher Vollmers

Publication year - 2019

Publication title -

philosophical transactions of the royal society b biological sciences

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 2.753

H-Index - 272

eISSN - 1471-2970

pISSN - 0962-8436

DOI - 10.1098/rstb.2019.0097

Subject(s) - transcriptome , computational biology , computer science , dna sequencing , data science , biology , gene , genetics , gene expression

Long-read sequencing holds great potential for transcriptome analysis because it offers researchers an affordable method to annotate the transcriptomes of non-model organisms. This, in turn, will greatly benefit future work on less-researched organisms like unicellular eukaryotes that cannot rely on large consortia to generate these transcriptome annotations. However, to realize this potential, several remaining molecular and computational challenges will have to be overcome. In this review, we have outlined the limitations of short-read sequencing technology and how long-read sequencing technology overcomes these limitations. We have also highlighted the unique challenges still present for long-read sequencing technology and provided some suggestions on how to overcome these challenges going forward. This article is part of a discussion meeting issue ‘Single cell ecology’.

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