Intracellular and Intercellular Gene Regulatory Network Inference From Time-Course Individual RNA-Seq

Gene regulatory network (GRN) inference is an effective approach to understand the molecular mechanisms underlying biological events. Generally, GRN inference mainly targets intracellular regulatory relationships such as transcription factors and their associated targets. In multicellular organisms, there are both intracellular and intercellular regulatory mechanisms. Thus, we hypothesize that GRNs inferred from time-course individual (whole embryo) RNA-Seq during development can reveal intercellular regulatory relationships (signaling pathways) underlying the development. Here, we conducted time-course bulk RNA-Seq of individual mouse embryos during early development, followed by pseudo-time analysis and GRN inference. The results demonstrated that GRN inference from RNA-Seq with pseudo-time can be applied for individual bulk RNA-Seq similar to scRNA-Seq. Validation using an experimental-source-based database showed that our approach could significantly infer GRN for all transcription factors in the database. Furthermore, the inferred ligand-related and receptor-related downstream genes were significantly overlapped. Thus, the inferred GRN based on whole organism could include intercellular regulatory relationships, which cannot be inferred from scRNA-Seq based only on gene expression data. Overall, inferring GRN from time-course bulk RNA-Seq is an effective approach to understand the regulatory relationships underlying biological events in multicellular organisms.

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BTNET : boosted tree based gene regulatory network inference algorithm using time-course measurement data

BMC Systems Biology ◽

10.1186/s12918-018-0547-0 ◽

2018 ◽

Vol 12 (S2) ◽

Cited By ~ 12

Author(s):

Sungjoon Park ◽

Jung Min Kim ◽

Wonho Shin ◽

Sung Won Han ◽

Minji Jeon ◽

...

Keyword(s):

Gene Regulatory Network ◽

Regulatory Network ◽

Time Course ◽

Network Inference ◽

Measurement Data ◽

Inference Algorithm ◽

Gene Regulatory Network Inference ◽

Boosted Tree ◽

Gene Regulatory

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WASABI: a dynamic iterative framework for gene regulatory network inference

10.1101/292128 ◽

2018 ◽

Cited By ~ 1

Author(s):

Arnaud Bonnaffoux ◽

Ulysse Herbach ◽

Angélique Richard ◽

Anissa Guillemin ◽

Sandrine Giraud ◽

...

Keyword(s):

Gene Expression ◽

Single Cell ◽

Gene Regulatory Network ◽

Regulatory Network ◽

Network Inference ◽

Molecular Mechanisms ◽

Gene Regulatory Network Inference ◽

Piecewise Deterministic Markov Processes ◽

Gene Regulatory ◽

Cell Data

AbstractInference of gene regulatory networks from gene expression data has been a long-standing and notoriously difficult task in systems biology. Recently, single-cell transcriptomic data have been massively used for gene regulatory network inference, with both successes and limitations. In the present work we propose an iterative algorithm called WASABI, dedicated to inferring a causal dynamical network from time-stamped single-cell data, which tackles some of the limitations associated with current approaches. We first introduce the concept of waves, which posits that the information provided by an external stimulus will affect genes one-by-one through a cascade, like waves spreading through a network. This concept allows us to infer the network one gene at a time, after genes have been ordered regarding their time of regulation. We then demonstrate the ability of WASABI to correctly infer small networks, which have been simulated in silico using a mechanistic model consisting of coupled piecewise-deterministic Markov processes for the proper description of gene expression at the single-cell level. We finally apply WASABI on in vitro generated data on an avian model of erythroid differentiation. The structure of the resulting gene regulatory network sheds a fascinating new light on the molecular mechanisms controlling this process. In particular, we find no evidence for hub genes and a much more distributed network structure than expected. Interestingly, we find that a majority of genes are under the direct control of the differentiation-inducing stimulus. In conclusion, WASABI is a versatile algorithm which should help biologists to fully exploit the power of time-stamped single-cell data.

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Context likelihood of relatedness with maximal information coefficient for Gene Regulatory Network inference

2015 18th International Conference on Computer and Information Technology (ICCIT) ◽

10.1109/iccitechn.2015.7488088 ◽

2015 ◽

Author(s):

M. A. H. Akhand ◽

R. N. Nandi ◽

S. M. Amran ◽

K. Murase

Keyword(s):

Gene Regulatory Network ◽

Regulatory Network ◽

Network Inference ◽

Gene Regulatory Network Inference ◽

Information Coefficient ◽

Gene Regulatory ◽

Maximal Information Coefficient

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Large scale gene regulatory network inference with a multi-level strategy

Molecular BioSystems ◽

10.1039/c5mb00560d ◽

2016 ◽

Vol 12 (2) ◽

pp. 588-597 ◽

Cited By ~ 14

Author(s):

Jun Wu ◽

Xiaodong Zhao ◽

Zongli Lin ◽

Zhifeng Shao

Keyword(s):

Gene Regulatory Network ◽

Regulatory Network ◽

Large Scale ◽

Network Inference ◽

Biological Processes ◽

Molecular Processes ◽

Gene Regulatory Network Inference ◽

Cell Functions ◽

Multi Level ◽

Gene Regulatory

Transcriptional regulation is a basis of many crucial molecular processes and an accurate inference of the gene regulatory network is a helpful and essential task to understand cell functions and gain insights into biological processes of interest in systems biology.

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Stages of Gene Regulatory Network Inference: the Evolutionary Algorithm Role

Evolutionary Algorithms ◽

10.5772/15182 ◽

2011 ◽

Cited By ~ 4

Author(s):

Alina Sirbu ◽

Heather J. ◽

Martin Crane

Keyword(s):

Evolutionary Algorithm ◽

Gene Regulatory Network ◽

Regulatory Network ◽

Network Inference ◽

Gene Regulatory Network Inference ◽

Gene Regulatory

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A posterior probability approach for gene regulatory network inference in genetic perturbation data

Mathematical Biosciences and Engineering ◽

10.3934/mbe.2016041 ◽

2016 ◽

Vol 13 (6) ◽

pp. 1241-1251 ◽

Cited By ~ 9

Author(s):

William Chad Young ◽

Adrian E. Raftery ◽

Ka Yee Yeung

Keyword(s):

Gene Regulatory Network ◽

Regulatory Network ◽

Posterior Probability ◽

Network Inference ◽

Gene Regulatory Network Inference ◽

Probability Approach ◽

Perturbation Data ◽

Gene Regulatory

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BRANE Cut: Biologically-Related A priori Network Enhancement with Graph cuts for Gene Regulatory Network Inference

10.1101/032383 ◽

2015 ◽

Author(s):

Aurélie Pirayre ◽

Camille Couprie ◽

Frédérique Bidard ◽

Laurent Duval ◽

Jean-Christophe Pesquet

Keyword(s):

Gene Regulatory Network ◽

Regulatory Network ◽

Gene Networks ◽

Network Inference ◽

State Of The Art ◽

A Priori ◽

Graph Cuts ◽

Gene Regulatory Network Inference ◽

Gene Regulatory ◽

Inference Methods

Background: Inferring gene networks from high-throughput data constitutes an important step in the discovery of relevant regulatory relationships in organism cells. Despite the large number of available Gene Regulatory Network inference methods, the problem remains challenging: the underdetermination in the space of possible solutions requires additional constraints that incorporate a priori information on gene interactions. Methods: Weighting all possible pairwise gene relationships by a probability of edge presence, we formulate the regulatory network inference as a discrete variational problem on graphs. We enforce biologically plausible coupling between groups and types of genes by minimizing an edge labeling functional coding for a priori structures. The optimization is carried out with Graph cuts, an approach popular in image processing and computer vision. We compare the inferred regulatory networks to results achieved by the mutual-information-based Context Likelihood of Relatedness (CLR) method and by the state-of-the-art GENIE3, winner of the DREAM4 multifactorial challenge. Results: Our BRANE Cut approach infers more accurately the five DREAM4 in silico networks (with improvements from 6% to 11%). On a real Escherichia coli compendium, an improvement of 11.8% compared to CLR and 3% compared to GENIE3 is obtained in terms of Area Under Precision-Recall curve. Up to 48 additional verified interactions are obtained over GENIE3 for a given precision. On this dataset involving 4345 genes, our method achieves a performance similar to that of GENIE3, while being more than seven times faster. The BRANE Cut code is available at: http://www-syscom.univ-mlv.fr/~pirayre/Codes-GRN-BRANE-cut.html Conclusions: BRANE Cut is a weighted graph thresholding method. Using biologically sound penalties and data-driven parameters, it improves three state-of-the-art GRN inference methods. It is applicable as a generic network inference post-processing, due its computational efficiency.

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Perturbation-based gene regulatory network inference to unravel oncogenic mechanisms

10.1101/735514 ◽

2019 ◽

Author(s):

Daniel Morgan ◽

Matthew Studham ◽

Andreas Tjärnberg ◽

Holger Weishaupt ◽

Fredrik J. Swartling ◽

...

Keyword(s):

Gene Regulatory Network ◽

Regulatory Network ◽

Regulatory Networks ◽

Network Inference ◽

Gene Regulatory Network Inference ◽

Validation Data ◽

Regulatory Interactions ◽

Link Type ◽

Gene Regulatory ◽

Novel Interactions

AbstractThe gene regulatory network (GRN) of human cells encodes mechanisms to ensure proper functioning. However, if this GRN is dysregulated, the cell may enter into a disease state such as cancer. Understanding the GRN as a system can therefore help identify novel mechanisms underlying disease, which can lead to new therapies. Reliable inference of GRNs is however still a major challenge in systems biology.To deduce regulatory interactions relevant to cancer, we applied a recent computational inference framework to data from perturbation experiments in squamous carcinoma cell line A431. GRNs were inferred using several methods, and the false discovery rate was controlled by the NestBoot framework. We developed a novel approach to assess the predictiveness of inferred GRNs against validation data, despite the lack of a gold standard. The best GRN was significantly more predictive than the null model, both in crossvalidated benchmarks and for an independent dataset of the same genes under a different perturbation design. It agrees with many known links, in addition to predicting a large number of novel interactions from which a subset was experimentally validated. The inferred GRN captures regulatory interactions central to cancer-relevant processes and thus provides mechanistic insights that are useful for future cancer research.Data available at GSE125958Inferred GRNs and inference statistics available at https://dcolin.shinyapps.io/CancerGRN/ Software available at https://bitbucket.org/sonnhammergrni/genespider/src/BFECV/Author SummaryCancer is the second most common cause of death globally, and although cancer treatments have improved in recent years, we need to understand how regulatory mechanisms are altered in cancer to combat the disease efficiently. By applying gene perturbations and inference of gene regulatory networks to 40 genes known or suspected to have a role in cancer due to interactions with the oncogene MYC, we deduce their underlying regulatory interactions. Using a recent computational framework for inference together with a novel method for cross validation, we infer a reliable regulatory model of this system in a completely data driven manner, not reliant on literature or priors. The novel interactions add to the understanding of the progressive oncogenic regulatory process and may provide new targets for therapy.

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