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The Alliance of Genome Resources: Building a Modern Data Ecosystem for Model Organism Databases.
Model organisms are essential experimental platforms for discovering gene functions, defining protein and genetic networks, uncovering functional consequences of human genome variation, and for modeling human disease. For decades, researchers who use model organisms have relied on Model Organism Databases (MODs) and the Gene Ontology Consortium (GOC) for expertly curated annotations, and for access to integrated genomic and biological information obtained from the scientific literature and public data archives. Through the development and enforcement of data and semantic standards, these genome resources provide rapid access to the collected knowledge of model organisms in human readable and computation-ready formats that would otherwise require countless hours for individual researchers to assemble on their own. Since their inception, the MODs for the predominant biomedical model organisms [Mus sp (laboratory mouse), Saccharomyces cerevisiae, Drosophila melanogaster, Caenorhabditis elegans, Danio rerio, and Rattus norvegicus] along with the GOC have operated as a network of independent, highly collaborative genome resources. In 2016, these six MODs and the GOC joined forces as the Alliance of Genome Resources (the Alliance). By implementing shared programmatic access methods and data-specific web pages with a unified "look and feel," the Alliance is tackling barriers that have limited the ability of researchers to easily compare common data types and annotations across model organisms. To adapt to the rapidly changing landscape for evaluating and funding core data resources, the Alliance is building a modern, extensible, and operationally efficient "knowledge commons" for model organisms using shared, modular infrastructure
Identification of control targets in Boolean molecular network models via computational algebra
Motivation: Many problems in biomedicine and other areas of the life sciences
can be characterized as control problems, with the goal of finding strategies
to change a disease or otherwise undesirable state of a biological system into
another, more desirable, state through an intervention, such as a drug or other
therapeutic treatment. The identification of such strategies is typically based
on a mathematical model of the process to be altered through targeted control
inputs. This paper focuses on processes at the molecular level that determine
the state of an individual cell, involving signaling or gene regulation. The
mathematical model type considered is that of Boolean networks. The potential
control targets can be represented by a set of nodes and edges that can be
manipulated to produce a desired effect on the system. Experimentally, node
manipulation requires technology to completely repress or fully activate a
particular gene product while edge manipulations only require a drug that
inactivates the interaction between two gene products. Results: This paper
presents a method for the identification of potential intervention targets in
Boolean molecular network models using algebraic techniques. The approach
exploits an algebraic representation of Boolean networks to encode the control
candidates in the network wiring diagram as the solutions of a system of
polynomials equations, and then uses computational algebra techniques to find
such controllers. The control methods in this paper are validated through the
identification of combinatorial interventions in the signaling pathways of
previously reported control targets in two well studied systems, a p53-mdm2
network and a blood T cell lymphocyte granular leukemia survival signaling
network.Comment: 12 pages, 4 figures, 2 table
Detection of regulator genes and eQTLs in gene networks
Genetic differences between individuals associated to quantitative phenotypic
traits, including disease states, are usually found in non-coding genomic
regions. These genetic variants are often also associated to differences in
expression levels of nearby genes (they are "expression quantitative trait
loci" or eQTLs for short) and presumably play a gene regulatory role, affecting
the status of molecular networks of interacting genes, proteins and
metabolites. Computational systems biology approaches to reconstruct causal
gene networks from large-scale omics data have therefore become essential to
understand the structure of networks controlled by eQTLs together with other
regulatory genes, and to generate detailed hypotheses about the molecular
mechanisms that lead from genotype to phenotype. Here we review the main
analytical methods and softwares to identify eQTLs and their associated genes,
to reconstruct co-expression networks and modules, to reconstruct causal
Bayesian gene and module networks, and to validate predicted networks in
silico.Comment: minor revision with typos corrected; review article; 24 pages, 2
figure
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