Affiliation:
1. Max Planck Institute for Terrestrial Microbiology, D-35043 Marburg, and Institute of Genetics and Microbiology, Ludwig-Maxilians-Universität-München, D-80638 Munich, Germany
Abstract
ABSTRACT
In the phytopathogenic fungus
Ustilago maydis
, pheromone-mediated cell fusion is a prerequisite for the generation of the infectious dikaryon. The pheromone signal elevates transcription of the pheromone genes and elicits formation of conjugation hyphae. Cyclic AMP and mitogen-activated protein kinase (MAPK) signaling are involved in this process. The MAPK cascade is presumed to be composed of Ubc4 (MAPK kinase kinase), Fuz7 (MAPK kinase), and Ubc3/Kpp2 (MAPK). We isolated the
kpp4
gene and found it to be allelic to
ubc4
. Epistasis analyses with constitutively active alleles of
kpp4
and
fuz7
substantiate that Kpp4, Fuz7, and Kpp2/Ubc3 are components of the same module. Moreover, we demonstrate that Fuz7 activates Kpp2 and shows interactions in vitro. Signaling via this cascade regulates expression of pheromone-responsive genes, presumably through acting on the transcription factor Prf1. Interestingly, the same cascade is needed for conjugation tube formation, and this process does not involve Prf1. In addition,
fuz7
as well as
kpp4
deletion strains are nonpathogenic, while
kpp2
deletion mutants are only attenuated in pathogenesis. Here we show that strains expressing the unphosphorylatable allele
kpp2
T182A/Y184F
are severely affected in tumor induction and display defects in early infection-related differentiation.
Publisher
American Society for Microbiology
Subject
Molecular Biology,General Medicine,Microbiology
Cited by
124 articles.
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