51 research outputs found
Synthetic Nucleotides as Probes of DNA Polymerase Specificity
The genetic code is continuously expanding with new nucleobases designed to suit specific research needs. These synthetic nucleotides are used to study DNA polymerase dynamics and specificity and may even inhibit DNA polymerase activity. The availability of an increasing chemical diversity of nucleotides allows questions of utilization by different DNA polymerases to be addressed. Much of the work in this area deals with the A family DNA polymerases, for example, Escherichia coli DNA polymerase I, which are DNA polymerases involved in replication and whose fidelity is relatively high, but more recent work includes other families of polymerases, including the Y family, whose members are known to be error prone. This paper focuses on the ability of DNA polymerases to utilize nonnatural nucleotides in DNA templates or as the incoming nucleoside triphosphates. Beyond the utility of nonnatural nucleotides as probes of DNA polymerase specificity, such entities can also provide insight into the functions of DNA polymerases when encountering DNA that is damaged by natural agents. Thus, synthetic nucleotides provide insight into how polymerases deal with nonnatural nucleotides as well as into the mutagenic potential of nonnatural nucleotides
The Roles of UmuD in Regulating Mutagenesis
All organisms are
subject to DNA damage from both endogenous and
environmental sources. DNA damage that is not
fully repaired can lead to mutations.
Mutagenesis is now understood to be an active
process, in part facilitated by lower-fidelity
DNA polymerases that replicate DNA in an
error-prone manner. Y-family DNA polymerases,
found throughout all domains of life, are
characterized by their lower fidelity on
undamaged DNA and their specialized ability to
copy damaged DNA. Two E. coli Y-family DNA polymerases are responsible for
copying damaged DNA as well as for mutagenesis.
These DNA polymerases interact with different
forms of UmuD, a dynamic protein that regulates
mutagenesis. The UmuD gene
products, regulated by the SOS response, exist
in two principal forms: UmuD2, which prevents mutagenesis, and UmuD2′, which facilitates UV-induced mutagenesis. This paper focuses on the multiple conformations of the UmuD gene products and how their protein interactions regulate mutagenesis
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