Affiliation:
1. Wellcome Trust Centre for Cell Biology, University of Edinburgh, Edinburgh EH9 3JR, United Kingdom
Abstract
ABSTRACT
The
pap1
-
5
mutation in poly(A) polymerase causes rapid depletion of mRNAs at restrictive temperatures. Residual mRNAs are polyadenylated, indicating that Pap1-5p retains at least partial activity. In
pap1
-
5
strains lacking Rrp6p, a nucleus-specific component of the exosome complex of 3′-5′ exonucleases, accumulation of poly(A)
+
mRNA was largely restored and growth was improved. The catalytically inactive mutant Rrp6-1p did not increase growth of the
pap1
-
5
strain and conferred much less mRNA stabilization than
rrp6
Δ. This may indicate that the major function of Rrp6p is in RNA surveillance. Inactivation of core exosome components, Rrp41p and Mtr3p, or the nuclear RNA helicase Mtr4p gave different phenotypes, with accumulation of deadenylated and 3′-truncated mRNAs. We speculate that slowed mRNA polyadenylation in the
pap1
-
5
strain is detected by a surveillance activity of Rrp6p, triggering rapid deadenylation and exosome-mediated degradation. In wild-type strains, assembly of the cleavage and polyadenylation complex might be suboptimal at cryptic polyadenylation sites, causing slowed polyadenylation.
Publisher
American Society for Microbiology
Subject
Cell Biology,Molecular Biology
Cited by
85 articles.
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