Reassembling haplotypes in a mixture of pooled amplicons when the relative concentrations are known: A proof-of-concept study on the efficient design of next-generation sequencing strategies.
Louis RanjardThomas K F WongAllen G RodrigoPublished in: PloS one (2018)
Next-generation sequencing can be costly and labour intensive. Usually, the sequencing cost per sample is reduced by pooling amplified DNA = amplicons) derived from different individuals on the same sequencing lane. Barcodes unique to each amplicon permit short-read sequences to be assigned appropriately. However, the cost of the library preparation increases with the number of barcodes used. We propose an alternative to barcoding: by using different known proportions of individually-derived amplicons in a pooled sample, each is characterised a priori by an expected depth of coverage. We have developed a Hidden Markov Model that uses these expected proportions to reconstruct the input sequences. We apply this method to pools of mitochondrial DNA amplicons extracted from kangaroo meat, genus Macropus. Our experiments indicate that the sequence coverage can be efficiently used to index the short-reads and that we can reassemble the input haplotypes when secondary factors impacting the coverage are controlled. We therefore demonstrate that, by combining our approach with standard barcoding, the cost of the library preparation is reduced to a third.
Keyphrases
- mitochondrial dna
- copy number
- circulating tumor
- affordable care act
- single cell
- genome wide
- molecularly imprinted
- cell free
- health insurance
- dna methylation
- healthcare
- optical coherence tomography
- phase iii
- circulating tumor cells
- randomized controlled trial
- amino acid
- mass spectrometry
- solid phase extraction
- open label
- study protocol
- tandem mass spectrometry