This paper proposes a new method to reverse engineer gene regulatory networks
from experimental data. The modeling framework used is time-discrete
deterministic dynamical systems, with a finite set of states for each of the
variables. The simplest examples of such models are Boolean networks, in which
variables have only two possible states. The use of a larger number of possible
states allows a finer discretization of experimental data and more than one
possible mode of action for the variables, depending on threshold values.
Furthermore, with a suitable choice of state set, one can employ powerful tools
from computational algebra, that underlie the reverse-engineering algorithm,
avoiding costly enumeration strategies. To perform well, the algorithm requires
wildtype together with perturbation time courses. This makes it suitable for
small to meso-scale networks rather than networks on a genome-wide scale. The
complexity of the algorithm is quadratic in the number of variables and cubic
in the number of time points. The algorithm is validated on a recently
published Boolean network model of segment polarity development in Drosophila
melanogaster.Comment: 28 pages, 5 EPS figures, uses elsart.cl