Yap1 overproduction restores arsenite resistance to the ABC transporter deficient mutant ycf1 by activating ACR3 expression

Ycf1 and Acr3 are transporters that have been previously shown to protect S accharomyces cerevisiae cells from the toxic effects of arsenite. Ycf1 and Acr3 are positively regulated by distinct, but related bZIP transcriptional activators, Yap1 and Yap8, respectively. In this study, we show that overe xpression of Yap1 complemented the arsenite hypersensitivity of the ycf1 nu ll mutant, but only if the ACR3 gene is functional. We further show that th e expression of either an ACR3-lacZ promoter fusion reporter or the endogen ous ACR3 gene was stimulated by the overproduction of Yap1 upon exposure to arsenite. These data suggest that Yap1 confers arsenite resistance to the ycf1 null mutant by activating expression of the Yap8-dependent target gene , ACR3. Our data also show Yap8-dependent ACR3-lacZ expression was greatly stimulated by arsenite in a dose-dependent manner in the parental strain. H owever, overproduction of Yap1 in the parental strain severely limited dose -dependent activation of the reporter by arsenite. We conclude that Yap1 ma y compete with Yap8 for binding to the ACR3 promoter, but is unable to act as a potent activator.