| Literature DB >> 27913044 |
Vivek Rathi1, Gavin Wright2, Diana Constantin3, Siok Chang3, Huong Pham3, Kerryn Jones3, Atha Palios3, Sue-Anne Mclachlan4, Matthew Conron5, Penny McKelvie3, Richard Williams3.
Abstract
The advent of massively parallel sequencing has caused a paradigm shift in the ways cancer is treated, as personalised therapy becomes a reality. More and more laboratories are looking to introduce next generation sequencing (NGS) as a tool for mutational analysis, as this technology has many advantages compared to conventional platforms like Sanger sequencing. In Australia all massively parallel sequencing platforms are still considered in-house in vitro diagnostic tools by the National Association of Testing Authorities (NATA) and a comprehensive analytical validation of all assays, and not just mere verification, is a strict requirement before accreditation can be granted for clinical testing on these platforms. Analytical validation of assays on NGS platforms can prove to be extremely challenging for pathology laboratories. Although there are many affordable and easily accessible NGS instruments available, there are no standardised guidelines as yet for clinical validation of NGS assays. We present an accreditation development procedure that was both comprehensive and applicable in a setting of hospital laboratory for NGS services. This approach may also be applied to other NGS applications in service laboratories.Entities:
Keywords: Validation; formalin fixed paraffin embedded; molecular; mutational analysis; next generation sequencing
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Year: 2016 PMID: 27913044 DOI: 10.1016/j.pathol.2016.08.016
Source DB: PubMed Journal: Pathology ISSN: 0031-3025 Impact factor: 5.306