Abstract
BACKGROUND: Inferring genetic networks from genome-wide expression data is extremely demanding computationally. We have developed fastBMA, a distributed, parallel and scalable implementation of Bayesian model averaging (BMA) for this purpose. fastBMA also includes a novel and computationally efficient method for eliminating redundant indirect edges in the network.
FINDINGS: We evaluated the performance of fastBMA on synthetic data and experimental genome-wide yeast and human datasets. When using a single CPU core, fastBMA is up to 100 times faster than the next fastest method, LASSO, with increased accuracy. It is a memory efficient, parallel and distributed application that scales to human genome wide expression data. A 10,000-gene regulation network can be obtained in a matter of hours using a 32-core cloud cluster.
CONCLUSIONS: fastBMA is a significant improvement over its predecessor ScanBMA. It is orders of magnitude faster and more accurate than other fast network inference methods such as LASSO. The improved scalability allows it to calculate networks from genome scale data in a reasonable timeframe. The transitive reduction method can improve accuracy in denser networks. fastBMA is available as code (M.I.T. license) from GitHub (https://github.com/lhhunghimself/fastBMA), as part of the updated networkBMA Bioconductor package (https://www.bioconductor.org/packages/release/bioc/html/networkBMA.html) and as ready-to-deploy Docker images (https://hub.docker.com/r/biodepot/fastbma/).
LIST OF ABBREVIATIONS
- AUC
- area under the curve
- AUROC
- area under receiver operator curve
- AUPR
- area under precision recall
- BMA
- Bayesian model averaging
- iBMA
- iterative Bayesian model averaging
- BIC
- Bayesian information criterion
- EM
- Estimation Maximization