Affiliation:
1. Departments of Molecular and Cellular Biology
2. Chemistry and Biochemistry, University of Arizona, Tucson, Arizona 85721
Abstract
ABSTRACT
Complex gene regulatory circuits exhibit emergent properties that are difficult to predict from the behavior of the components. One such property is the stability of regulatory states. Here we analyze the stability of the lysogenic state of phage λ. In this state, the virus maintains a stable association with the host, and the lytic functions of the virus are repressed by the viral CI repressor. This state readily switches to the lytic pathway when the host SOS system is induced. A low level of SOS-dependent switching occurs without an overt stimulus. We found that the intrinsic rate of switching to the lytic pathway, measured in a host lacking the SOS response, was almost undetectably low, probably less than 10
−8
/generation. We surmise that this low rate has not been selected directly during evolution but results from optimizing the rate of switching in a wild-type host over the natural range of SOS-inducing conditions. We also analyzed a mutant, λ
prm240
, in which the promoter controlling CI expression was weakened, rendering lysogens unstable. Strikingly, the intrinsic stability of λ
prm240
lysogens depended markedly on the growth conditions; lysogens grown in minimal medium were nearly stable but switched at high rates when grown in rich medium. These effects on stability likely reflect corresponding effects on the strength of the
prm240
promoter, measured in an uncoupled assay system. Several derivatives of λ
prm240
with altered stabilities were characterized. This mutant and its derivatives afford a model system for further analysis of stability.
Publisher
American Society for Microbiology
Subject
Molecular Biology,Microbiology
Reference63 articles.
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