Affiliation:
1. Fungal Genomics Unit, Austrian Research Centers and BOKU Vienna, A-1190 Vienna, Austria
2. Istitute de Genetique et Microbiologie, Université Paris-Sud, F-91495 Orsay-CEDEX, France
Abstract
ABSTRACT
In
Aspergillus nidulans
, proline can be used as a carbon and nitrogen source, and its metabolism requires the integration of three signals, including proline induction and nitrogen and carbon metabolite derepression. We have previously shown that the bidirectional promoter in the
prnD-prnB
intergenic region undergoes drastic chromatin rearrangements such that proline induction leads to the loss of positioned nucleosomes, whereas simultaneous carbon and nitrogen metabolite repression results in the partial repositioning of these nucleosomes. In the proline cluster, the inhibition of deacetylases by trichostatin A leads to partial derepression and is associated with a lack of nucleosome positioning. Here, we investigate the effect of histone acetylation in the proline cluster using strains deleted of essential components of putative
A. nidulans
histone acetyltransferase complexes, namely,
gcnE
and
adaB
, the orthologues of the
Saccharomyces cerevisiae GCN5
and
ADA2
genes, respectively. Surprisingly, GcnE and AdaB are not required for transcriptional activation and chromatin remodeling but are required for the repression of
prnB
and
prnD
and for the repositioning of nucleosomes in the divergent promoter region. Chromatin immunoprecipitation directed against histone H3 lysines K9 and K14 revealed that GcnE and AdaB participate in increasing the acetylation level of at least one nucleosome in the
prnD-prnB
intergenic region during activation, but these activities do not determine nucleosome positioning. Our results are consistent with a function of GcnE and AdaB in gene repression of the proline cluster, probably an indirect effect related to the function of CreA, the DNA-binding protein mediating carbon catabolite repression in
A. nidulans
.
Publisher
American Society for Microbiology
Subject
Molecular Biology,General Medicine,Microbiology
Cited by
56 articles.
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