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10.1109/TCBB.2015.2465952

http://scihub22266oqcxt.onion/10.1109/TCBB.2015.2465952
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C5154690!5154690!27990101
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suck abstract from ncbi


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pmid27990101      IEEE/ACM+Trans+Comput+Biol+Bioinform 2016 ; 13 (4): 767-77
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  • Reconstruction of Gene Regulatory Networks based on Repairing Sparse Low-rank Matrices #MMPMID27990101
  • Chang YH; Dobbe R; Bhushan P; Gray JW; Tomlin CJ
  • IEEE/ACM Trans Comput Biol Bioinform 2016[Jul]; 13 (4): 767-77 PMID27990101show ga
  • With the growth of high-throughput proteomic data, in particular time series gene expression data from various perturbations, a general question that has arisen is how to organize inherently heterogenous data into meaningful structures. Since biological systems such as breast cancer tumors respond differently to various treatments, little is known about exactly how these gene regulatory networks (GRNs) operate under different stimuli. Challenges due to the lack of knowledge not only occur in modeling the dynamics of a GRN but also cause bias or uncertainties in identifying parameters or inferring the GRN structure. This paper describes a new algorithm which enables us to estimate bias error due to the effect of perturbations and correctly identify the common graph structure among biased inferred graph structures. To do this, we retrieve common dynamics of the GRN subject to various perturbations. We refer to the task as ?repairing? inspired by ?image repairing? in computer vision. The method can automatically correctly repair the common graph structure across perturbed GRNs, even without precise information about the effect of the perturbations. We evaluate the method on synthetic data sets and demonstrate an application to the DREAM data sets and discuss its implications to experiment design.
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