Please use this identifier to cite or link to this item: https://biore.bio.bg.ac.rs/handle/123456789/1460
Title: A RecA protein mutant deficient in its interaction with the UmuDC complex
Authors: Bailone, A.
Sommer, S.
Knežević Vukčević, Jelena 
Dutreix, M.
Devoret, R.
Keywords: complementation of recA mutations;Mut dominant phenotype -;pKM101 plasmid;UmuD′ formation;RecA functions
Issue Date: 1-Jan-1991
Journal: Biochimie
Abstract: 
recA1730 is a dominant point mutation preventing SOS mutagenesis. We demonstrate here that: i) RecA1730 fails to produce mutagenesis even though UmuD′ is formed, ii) recA1730, when complemented by recA+, can cleave LexA protein and it displays a UmuDC- phenotype in spite of adequate concentrations of matured UmuD′ and and UmuC proteins, iii) the Mut- phenotype caused by RecA1730 is partially alleviated by MucAB proteins, functional analogs of UmuDC. To explain the mutant phenotype, we postulate that recA1730 impairs a RecA function required for the positioning of the UmuD'C complex within the replisome at the site of lesions. © 1991.
URI: https://biore.bio.bg.ac.rs/handle/123456789/1460
ISSN: 0300-9084
DOI: 10.1016/0300-9084(91)90115-H
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