%0 Journal Article %1 Trivedi:2014:Front-Genet:24834071 %A Trivedi, U H %A Cézard, T %A Bridgett, S %A Montazam, A %A Nichols, J %A Blaxter, M %A Gharbi, K %D 2014 %J Front Genet %K next-generation-sequencing quality-control %P 111-111 %R 10.3389/fgene.2014.00111 %T Quality control of next-generation sequencing data without a reference %U https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4018527/ %V 5 %X Next-generation sequencing (NGS) technologies have dramatically expanded the breadth of genomics. Genome-scale data, once restricted to a small number of biomedical model organisms, can now be generated for virtually any species at remarkable speed and low cost. Yet non-model organisms often lack a suitable reference to map sequence reads against, making alignment-based quality control (QC) of NGS data more challenging than cases where a well-assembled genome is already available. Here we show that by generating a rapid, non-optimized draft assembly of raw reads, it is possible to obtain reliable and informative QC metrics, thus removing the need for a high quality reference. We use benchmark datasets generated from control samples across a range of genome sizes to illustrate that QC inferences made using draft assemblies are broadly equivalent to those made using a well-established reference, and describe QC tools routinely used in our production facility to assess the quality of NGS data from non-model organisms.

@article{Trivedi:2014:Front-Genet:24834071, abstract = {Next-generation sequencing (NGS) technologies have dramatically expanded the breadth of genomics. Genome-scale data, once restricted to a small number of biomedical model organisms, can now be generated for virtually any species at remarkable speed and low cost. Yet non-model organisms often lack a suitable reference to map sequence reads against, making alignment-based quality control (QC) of NGS data more challenging than cases where a well-assembled genome is already available. Here we show that by generating a rapid, non-optimized draft assembly of raw reads, it is possible to obtain reliable and informative QC metrics, thus removing the need for a high quality reference. We use benchmark datasets generated from control samples across a range of genome sizes to illustrate that QC inferences made using draft assemblies are broadly equivalent to those made using a well-established reference, and describe QC tools routinely used in our production facility to assess the quality of NGS data from non-model organisms.}, added-at = {2017-07-26T23:25:07.000+0200}, author = {Trivedi, U H and C{\'e}zard, T and Bridgett, S and Montazam, A and Nichols, J and Blaxter, M and Gharbi, K}, biburl = {https://www.bibsonomy.org/bibtex/26cbb056dd76158e978288f49528565b0/marcsaric}, description = {Quality control of next-generation sequencing data without a reference}, doi = {10.3389/fgene.2014.00111}, interhash = {ba25d17255bb0c9f4d776c1bd95f6044}, intrahash = {6cbb056dd76158e978288f49528565b0}, journal = {Front Genet}, keywords = {next-generation-sequencing quality-control}, pages = {111-111}, pmid = {24834071}, timestamp = {2017-07-26T23:25:07.000+0200}, title = {Quality control of next-generation sequencing data without a reference}, url = {https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4018527/}, volume = 5, year = 2014 }