Affiliation:
1. Department of Biology, Boston University, Boston, Massachusetts 02215,1 and
2. School of Public Health, Boston University School of Medicine, Boston, Massachusetts 021182
Abstract
ABSTRACT
DNA-DNA interstrand cross-links are the cytotoxic lesions for many chemotherapeutic agents. A plasmid with a single nitrogen mustard (HN2) interstrand cross-link (inter-HN2-pTZSV28) was constructed and transformed into
Escherichia coli
, and its replication efficiency (RE = [number of transformants from inter-HN2-pTZSV28]/[number of transformants from control]) was determined to be ∼0.6. Previous work showed that RE was high because the cross-link was repaired by a pathway involving nucleotide excision repair (NER) but not recombination. (In fact, recombination was precluded because the cells do not receive lesion-free homologous DNA.) Herein, DNA polymerase II is shown to be in this new pathway, since the replication efficiency (RE) is higher in a
polB
+
(∼0.6) than in a Δ
polB
(∼0.1) strain. Complementation with a
polB
+
-containing plasmid restores RE to wild-type levels, which corroborates this conclusion. In separate experiments,
E. coli
was treated with HN2, and the relative sensitivity to killing was found to be as follows: wild type <
polB
<
recA
<
polB recA
∼
uvrA
. Because cells deficient in either recombination (
recA
) or DNA polymerase II (
polB
) are hypersensitive to nitrogen mustard killing,
E. coli
appears to have two pathways for cross-link repair: an NER/recombination pathway (which is possible when the cross-links are formed in cells where recombination can occur because there are multiple copies of the genome) and an NER/DNA polymerase II pathway. Furthermore, these results show that some cross-links are uniquely repaired by each pathway. This represents one of the first clearly defined pathway in which DNA polymerase II plays a role in
E. coli
. It remains to be determined why this new pathway prefers DNA polymerase II and why there are two pathways to repair cross-links.
Publisher
American Society for Microbiology
Subject
Molecular Biology,Microbiology
Cited by
108 articles.
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