Affiliation:
1. Department of Biological Sciences, University of Illinois at Chicago, Chicago, Illinois 60607, 1 and
2. Department of Plant Biology, University of Minnesota, St. Paul, Minnesota 551082
Abstract
ABSTRACT
A screen for host mutations which increase the rate of transposition of Ty1 and Ty2 into a chromosomal target was used to identify factors influencing retroelement transposition. The fortuitous presence of a mutation in the
CAC3
gene in the strain in which this screen was undertaken enabled us to discover that double mutaions of
cac3
and
hir3
, but neither of the two single mutations, caused a dramatic increase in the rate of retrotransposition. We further showed that this effect was not due to an increase in the overall level of Ty1 mRNA. Two subtle
cac3
phenotypes, slight methyl methanesulfonate (MMS) sensitivity and reduction of telomeric silencing, were significantly enhanced in the
cac3 hir3
double mutant. In addition, the growth rate of the double mutant was reduced.
HIR3
belongs to a class of
HIR
genes that regulate the transcription of histones, while Cac3p, together with Cac1p and Cac2p, forms chromatin assembly factor I. Other combinations of mutations in
cac
and
hir
genes (
cac3 hir1
,
cac3 hir2
, and
cac2 hir3
) also increase Ty transposition and MMS sensitivity and reduce the growth rate. A model explaining the synergistic interaction between
cac
and
hir
mutations in terms of alterations in chromatin structure is proposed.
Publisher
American Society for Microbiology
Subject
Cell Biology,Molecular Biology
Cited by
52 articles.
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