Affiliation:
1. Department of Biochemistry, Dartmouth Medical School, Hanover, New Hampshire 03755
2. Department of Molecular Biology and Microbiology, Tufts University School of Medicine and Sackler Graduate School, Boston, Massachusetts 02111
3. Institut de Microbiologie, 1011 Lausanne, Switzerland
Abstract
ABSTRACT
In a screen to identify genes required for mRNA export in
Saccharomyces cerevisiae
, we isolated an allele of poly(A) polymerase (
PAP1
) and novel alleles encoding several other 3′ processing factors. Many newly isolated and some previously described mutants (
rna14
-
48
,
rna14
-
49
,
rna14
-
64
,
rna15
-
58
, and
pcf11
-
1
strains) are defective in polymerase II (Pol II) termination but, interestingly, retain the ability to polyadenylate these improperly processed transcripts at the nonpermissive temperature. Deletion of the
cis
-acting sequences required to couple 3′ processing and termination also produces transcripts that fail to exit the nucleus, suggesting that all of these processes (cleavage, termination, and export) are coupled. We also find that several but not all mRNA export mutants produce improperly 3′ processed transcripts at the nonpermissive temperature. 3′ maturation defects in mRNA export mutants include improper Pol II termination and/or the previously characterized hyperpolyadenylation of transcripts. Importantly, not all mRNA export mutants have defects in 3′ processing. The similarity of the phenotypes of some mRNA export mutants and 3′ processing mutants indicates that some factors from each process may mechanistically interact to couple mRNA processing and export. Consistent with this assumption, we present evidence that Xpo1p interacts in vivo with several 3′ processing factors and that the addition of recombinant Xpo1p to in vitro processing reaction mixtures stimulates 3′ maturation. Of the core 3′ processing factors tested (Rna14p, Rna15p, Pcf11p, Hrp1p, Fip1p, and Cft1p), only Hrp1p shuttles. Overexpression of Rat8p/Dbp5p suppresses both 3′ processing and mRNA export defects found in
xpo1
-
1
cells.
Publisher
American Society for Microbiology
Subject
Cell Biology,Molecular Biology
Cited by
118 articles.
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