TY - JOUR T1 - Insight and Inference for DVARS JF - bioRxiv DO - 10.1101/125021 SP - 125021 AU - Soroosh Afyouni AU - Thomas E. Nichols Y1 - 2017/01/01 UR - http://biorxiv.org/content/early/2017/04/06/125021.1.abstract N2 - Estimates of functional connectivity using resting state functional magnetic resonance imaging (rs-fMRI) are acutely sensitive to artifacts and large scale nuisance variation. As a result much effort is dedicated to preprocessing rs-fMRI data and using diagnostic measure to identify bad scans. One such diagnostic measure is DVARS, the spatial standard deviation of the data after temporal differencing. A limitation of DVARS however is the lack of concrete interpretation of the absolute values of DVARS, and finding a threshold to distinguish bad scans from good. In this work we describe a variance decomposition of the entire 4D dataset that shows DVARS to be just one of three sources of variation we refer to as D-var, S-var and E-var. D-var and S-var partition the average variance between adjacent time points, while E-var accounts for edge effects, and each can be used to make spatial and temporal summary diagnostic measures. Extending the partitioning to global (and non-global) signal leads to a rs-fMRI DSE ANOVA table, which decomposes the total and global variance into fast (D-var), slow (S-var) and edge (E-var) components. We find expected values for each variance component under nominal models, showing how D-var (and thus DVARS) scales with overall variance and is diminished by temporal autocorrelation. Finally we propose a sampling distribution for squared DVARS (a multiple of D-var) and robust methods to estimate this null model, allowing computations of DVARS p-values. We propose that these diagnostic time series, images, p-values and ANOVA table will provide a succinct summary of the quality of a rs-fMRI dataset that will support comparisons of datasets over preprocessing steps and between subjects. ER -