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Granger causality is among the widely used data-driven approaches for causal analysis of time series data with applications in various areas including economics, molecular biology, and neuroscience. Two of the main challenges of this methodology are: 1) over-fitting as a result of limited data duration, and 2) correlated process noise as a confounding factor, both leading to errors in identifying the causal influences. Sparse estimation via the LASSO has successfully addressed these challenges for parameter estimation. However, the classical statistical tests for Granger causality resort to asymptotic analysis of ordinary least squares, which require long data duration to be useful and are not immune to confounding effects. In this work, we address this disconnect by introducing a LASSO-based statistic and studying its non-asymptotic properties under the assumption that the true models admit sparse autoregressive representations. We establish fundamental limits for reliable identification of Granger causal influences using the proposed LASSO-based statistic. We further characterize the false positive error probability and test power of a simple thresholding rule for identifying Granger causal effects and provide two methods to set the threshold in a data-driven fashion. We present simulation studies and application to real data to compare the performance of our proposed method to ordinary least squares and existing LASSO-based methods in detecting Granger causal influences, which corroborate our theoretical results. 

Extracting directional connectivity in a neuronal ensemble from spiking observations is a key challenge in understanding the circuit mechanisms of brain function. Existing methods proceed in two stages, by first estimating the latent processes that govern spiking, followed by characterizing connectivity using said estimates. As such, the extracted networks in the second stage are highly sensitive to the accuracy of the estimates in the first stage. In this work, we introduce a framework to directly extract Granger causal links from spiking observations, without requiring intermediate time-domain estimation, by explicitly modeling the endogenous and exogenous latent processes that underlie spiking activity. Our proposed method integrates several techniques such as point processes, state-space modeling and Pólya-Gamma augmentation. We demonstrate the utility of our proposed approach using simulated data and application to real data from the rat brain during sleep. 

Neuronal activity correlations are key to understanding how populations of neurons collectively encode information. While two-photon calcium imaging has created a unique opportunity to record the activity of large populations of neurons, existing methods for inferring correlations from these data face several challenges. First, the observations of spiking activity produced by two-photon imaging are temporally blurred and noisy. Secondly, even if the spiking data were perfectly recovered via deconvolution, inferring network-level features from binary spiking data is a challenging task due to the non-linear relation of neuronal spiking to endogenous and exogenous inputs. In this work, we propose a methodology to explicitly model and directly estimate signal and noise correlations from two-photon fluorescence observations, without requiring intermediate spike deconvolution. We provide theoretical guarantees on the performance of the proposed estimator and demonstrate its utility through applications to simulated and experimentally recorded data from the mouse auditory cortex.