PT - JOURNAL ARTICLE AU - Cynthia A. Kalita AU - Gregory A. Moyerbrailean AU - Christopher Brown AU - Xiaoquan Wen AU - Francesca Luca AU - Roger Pique-Regi TI - QuASAR-MPRA: Accurate allele-specific analysis for massively parallel reporter assays AID - 10.1101/105627 DP - 2017 Jan 01 TA - bioRxiv PG - 105627 4099 - http://biorxiv.org/content/early/2017/07/12/105627.short 4100 - http://biorxiv.org/content/early/2017/07/12/105627.full AB - Motivation The majority of the human genome is composed of non-coding regions containing regulatory elements such as enhancers, which are crucial for controlling gene expression. Many variants associated with complex traits are in these regions, and may disrupt gene regulatory sequences. Consequently, it is important to not only identify true enhancers but also to test if a variant within an enhancer affects gene regulation. Recently, allele-specific analysis in high-throughput reporter assays, such as massively parallel reporter assays (MPRA), have been used to functionally validate non-coding variants. However, we are still missing high-quality and robust data analysis tools for these datasets.Results We have further developed our method for allele-specific analysis QuASAR (quantitative allele-specific analysis of reads) to analyze allele-specific signals in barcoded read counts data from MPRA. Using this approach, we can take into account the uncertainty on the original plasmid proportions, over-dispersion, and sequencing errors. The provided allelic skew estimate and its standard error also simplifies meta-analysis of replicate experiments. Additionally, we show that a beta-binomial distribution better models the variability present in the allelic imbalance of these synthetic reporters and results in a test that is statistically well calibrated under the null. Applying this approach to the MPRA data by Tewhey et al. (2016), we found 602 SNPs with significant (FDR 10%) allele-specific regulatory function in LCLs. We also show that we can combine MPRA with QuASAR estimates to validate existing experimental and computational annotations of regulatory variants. Our study shows that with appropriate data analysis tools, we can improve the power to detect allelic effects in high throughput reporter assays.Availability http://github.com/piquelab/QuASAR/tree/master/mpraContact fluca{at}wayne.edu; rpique{at}wayne.edu