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Gene regulatory network

A gene regulatory network (also called a GRN or genetic regulatory network) is a collection of DNA segments in a cell which interact with each other and with other substances in the cell, thereby governing the rates at which genes in the network are transcribed into mRNA.

Contents

Overview

Genes can be viewed as nodes in a network, with input being proteins such as transcription factors, and outputs being the level of gene expression. The node itself can also be viewed as a function which can be obtained by combining basic functions upon the inputs (in the Boolean network described below these are boolean functions or gates computed using the basic AND OR and NOT gates in electronics). These functions have been interpreted as performing a kind information processing within cell which determine cellular behaviour. The basic drivers within cells are levels of some proteins, which determine both spatial (tissue related) and temporal (developmental stage) co-ordinates of the cell, as a kind of "cellular memory". The gene networks are only beginning to be understood, and it is a next step for biology to attempt to deduce the functions for each gene "node", to assist in modeling behaviour of a cell (see systems biology).

Mathematical models of GRNs have been developed to allow predictions of the models to be tested. Various modeling techniques have been used, including boolean networks , Petri nets, Bayesian networks, and sets of differential equations. Conversely, techniques have been proposed for generating models of GRNs that best explain a set of time series observations.

Example: Boolean network

The following example illustrates how a Boolean network can model a GRN together with its gene products (the outputs) and the substances from the environment that affect it (the inputs). Stuart Kauffman was amongst the first biologists to use the metaphor of Boolean networks to model genetic regulatory networks.

  1. Each gene, each input, and each output is represented by a node in a directed graph in which there is an arrow from one node to another if and only if there is a causal link between the two nodes.
  2. Each node in the graph can be in one of two states: on or off.
  3. For a gene, "on" corresponds to the gene being expressed; for inputs and outputs, "on" corresponds to the substance being present.
  4. Time is viewed as proceeding in discrete steps. At each step, the new state of a node is a boolean function of the prior states of the nodes with arrows pointing towards it.

The validity of the model can be tested by comparing simulation results with time series observations.

See also

Bibliography

  • James M. Bower, Hamid Bolouri (editors), (2001) Computational Modeling of Genetic and Biochemical Networks Computational Molecular Biology Series, MIT Press, ISBN 0262024810
  • S. A. Kauffman, "Metabolic stability and epigenesis in randomly constructed genetic nets", J. Theoret. Biol (1969) 22, 434-467

External links

Last updated: 08-05-2005 08:25:26
Last updated: 09-12-2005 02:39:13