par Janel-Bintz, Régine;Maenhaut, Geneviève 
;Fuchs, Robert P P
Référence Molecular & general genetics : MGG, 245, 3, page (279-285)
Publication Publié, 1994-05
;Fuchs, Robert P PRéférence Molecular & general genetics : MGG, 245, 3, page (279-285)
Publication Publié, 1994-05
Article révisé par les pairs
| Résumé : | N-2-acetylaminofluorene has been shown efficiently to induce both -1 and -2 frameshift mutations in Escherichia coli as well as in mammalian cells. In E. coli, the genetic characteristics of -1 and -2 frameshift mutations were found to be distinct. The -1 frameshift mutation pathway occurs at monotonous runs of G residues (i.e. GGG→GG). This pathway exhibits the same genetic requirements as UV light-induced base substitution mutagenesis. Indeed, optimal mutagenesis requires the expression of both UmuDC and the activated form of RecA. The -2 frameshift mutation pathway operates at short alternating GpC sequences, such as the NarI sequence (i.e. GGCGCC→GGCC). In contrast to the -1 frameshift mutation pathway, optimal induction does not require the UmuDC and RecA proteins. This pathway involves a LexA-repressed function tentatively called Npf (for NarI processing factor). In this paper, we show that MucAB efficiently stimulates the -2 frameshift mutation pathway. However, unlike the Npf pathway, MucAB-mediated stimulation requires expression of the RecA protein. © 1994 Springer-Verlag. |
