Effective machine-learning assembly for next-generation amplicon sequencing with very low coverage.

Journal: BMC bioinformatics

Published Date: Dec 11, 2019

Abstract

BACKGROUND: In short-read DNA sequencing experiments, the read coverage is a key parameter to successfully assemble the reads and reconstruct the sequence of the input DNA. When coverage is very low, the original sequence reconstruction from the reads can be difficult because of the occurrence of uncovered gaps. Reference guided assembly can then improve these assemblies. However, when the available reference is phylogenetically distant from the sequencing reads, the mapping rate of the reads can be extremely low. Some recent improvements in read mapping approaches aim at modifying the reference according to the reads dynamically. Such approaches can significantly improve the alignment rate of the reads onto distant references but the processing of insertions and deletions remains challenging.

Authors

Louis Ranjard

The Research School of Biology, The Australian National University, Canberra, Australia. louis.ranjard@anu.edu.au.
Thomas K F Wong

The Research School of Biology, The Australian National University, Canberra, Australia.
Allen G Rodrigo

The Research School of Biology, The Australian National University, Canberra, Australia.

Keywords

Algorithms Animals Base Sequence Genome, Mitochondrial High-Throughput Nucleotide Sequencing Machine Learning Macropodidae Nucleotides

External Resources

View on PubMed Access via DOI PubMed (31829137)

Effective machine-learning assembly for next-generation amplicon sequencing with very low coverage.

Abstract

Authors

Keywords

External Resources

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