Cell-based reference samples designed with specific differences in microRNA biomarkers

P. Scott Pine; Steven P. Lund; Sanford A. Stass; Debra Kukuruga; Feng Jiang; Lynn Sorbara; Sudhir Srivastava; Marc Salit

doi:10.1186/s12896-018-0423-4

BMC Biotechnology (Mar 2018)

Cell-based reference samples designed with specific differences in microRNA biomarkers

P. Scott Pine,
Steven P. Lund,
Sanford A. Stass,
Debra Kukuruga,
Feng Jiang,
Lynn Sorbara,
Sudhir Srivastava,
Marc Salit

Affiliations

P. Scott Pine: Joint Initiative for Metrology in Biology, National Institute of Standards and Technology
Steven P. Lund: Statistical Engineering Division, National Institute of Standards and Technology
Sanford A. Stass: Department of Pathology, University of Maryland School of Medicine
Debra Kukuruga: Department of Pathology, University of Maryland School of Medicine
Feng Jiang: Department of Pathology, University of Maryland School of Medicine
Lynn Sorbara: Division of Cancer Prevention, National Cancer Institute
Sudhir Srivastava: Division of Cancer Prevention, National Cancer Institute
Marc Salit: Joint Initiative for Metrology in Biology, National Institute of Standards and Technology

DOI: https://doi.org/10.1186/s12896-018-0423-4
Journal volume & issue: Vol. 18, no. 1
pp. 1 – 14

Abstract

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Abstract Background We demonstrate the feasibility of creating a pair of reference samples to be used as surrogates for clinical samples measured in either a research or clinical laboratory setting. The reference sample paradigm presented and evaluated here is designed to assess the capability of a measurement process to detect true differences between two biological samples. Cell-based reference samples can be created with a biomarker signature pattern designed in silico. Clinical laboratories working in regulated applications are required to participate in proficiency testing programs; research laboratories doing discovery typically do not. These reference samples can be used in proficiency tests or as process controls that allow a laboratory to evaluate and optimize its measurement systems, monitor performance over time (process drift), assess changes in protocols, reagents, and/or personnel, maintain standard operating procedures, and most importantly, provide evidence for quality results. Results The biomarkers of interest in this study are microRNAs (miRNAs), small non-coding RNAs involved in the regulation of gene expression. Multiple lung cancer associated cell lines were determined by reverse transcription (RT)-PCR to have sufficiently different miRNA profiles to serve as components in mixture designs as reference samples. In silico models based on the component profiles were used to predict miRNA abundance ratios between two different cell line mixtures, providing target values for profiles obtained from in vitro mixtures. Two reference sample types were tested: total RNA mixed after extraction from cell lines, and intact cells mixed prior to RNA extraction. MicroRNA profiling of a pair of samples composed of extracted RNA derived from these cell lines successfully replicated the target values. Mixtures of intact cells from these lines also approximated the target values, demonstrating potential utility as mimics for clinical specimens. Both designs demonstrated their utility as reference samples for inter- or intra-laboratory testing. Conclusions Cell-based reference samples can be created for performance assessment of a measurement process from biomolecule extraction through quantitation. Although this study focused on miRNA profiling with RT-PCR using cell lines associated with lung cancer, the paradigm demonstrated here should be extendable to genome-scale platforms and other biomolecular endpoints.

Published in BMC Biotechnology

ISSN: 1472-6750 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Technology: Chemical technology: Biotechnology
Website: https://bmcbiotechnol.biomedcentral.com

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