Validation and Implementation of Clinical Laboratory Improvements Act-Compliant Whole-Genome Sequencing in the Public Health Microbiology Laboratory

Varvara K Kozyreva; Chau-Linda Truong; Alexander L Greninger; John Crandall; Rituparna Mukhopadhyay; Vishnu Chaturvedi

doi:10.1128/JCM.00361-17

Validation and Implementation of Clinical Laboratory Improvements Act-Compliant Whole-Genome Sequencing in the Public Health Microbiology Laboratory

J Clin Microbiol. 2017 Aug;55(8):2502-2520. doi: 10.1128/JCM.00361-17. Epub 2017 Jun 7.

Authors

Varvara K Kozyreva¹, Chau-Linda Truong¹, Alexander L Greninger¹, John Crandall¹, Rituparna Mukhopadhyay¹, Vishnu Chaturvedi²

Affiliations

¹ Microbial Diseases Laboratory, California Department of Public Health, Richmond, California, USA.
² Microbial Diseases Laboratory, California Department of Public Health, Richmond, California, USA Vishnu.Chaturvedi@cdph.ca.gov.

Abstract

Public health microbiology laboratories (PHLs) are on the cusp of unprecedented improvements in pathogen identification, antibiotic resistance detection, and outbreak investigation by using whole-genome sequencing (WGS). However, considerable challenges remain due to the lack of common standards. Here, we describe the validation of WGS on the Illumina platform for routine use in PHLs according to Clinical Laboratory Improvements Act (CLIA) guidelines for laboratory-developed tests (LDTs). We developed a validation panel comprising 10 Enterobacteriaceae isolates, 5 Gram-positive cocci, 5 Gram-negative nonfermenting species, 9 Mycobacterium tuberculosis isolates, and 5 miscellaneous bacteria. The genome coverage range was 15.71× to 216.4× (average, 79.72×; median, 71.55×); the limit of detection (LOD) for single nucleotide polymorphisms (SNPs) was 60×. The accuracy, reproducibility, and repeatability of base calling were >99.9%. The accuracy of phylogenetic analysis was 100%. The specificity and sensitivity inferred from multilocus sequence typing (MLST) and genome-wide SNP-based phylogenetic assays were 100%. The following objectives were accomplished: (i) the establishment of the performance specifications for WGS applications in PHLs according to CLIA guidelines, (ii) the development of quality assurance and quality control measures, (iii) the development of a reporting format for end users with or without WGS expertise, (iv) the availability of a validation set of microorganisms, and (v) the creation of a modular template for the validation of WGS processes in PHLs. The validation panel, sequencing analytics, and raw sequences could facilitate multilaboratory comparisons of WGS data. Additionally, the WGS performance specifications and modular template are adaptable for the validation of other platforms and reagent kits.

Keywords: CLIA; WGS; bacteria; bioinformatics pipeline; laboratory-developed test; performance specifications; public health; quality management; validation; whole-genome sequencing.

Publication types

Validation Study

MeSH terms

Bacterial Infections / diagnosis*
Bacteriological Techniques / methods*
Humans
Molecular Diagnostic Techniques / methods*
Molecular Epidemiology / methods*
Reproducibility of Results
Sensitivity and Specificity
Whole Genome Sequencing / methods*

Grants and funding

U50 CK000410/CK/NCEZID CDC HHS/United States