4.8 Article

Mutant LYS2 mRNAs retained and degraded in the nucleus of Saccharomyces cerevisiae

Publisher

NATL ACAD SCIENCES
DOI: 10.1073/pnas.0604562103

Keywords

mRNA degradation in yeast; Saccharomyces cerevisiae mRNA degradation; CBC1; RRP6; nuclear retention of mRNA

Funding

  1. NIGMS NIH HHS [R01 GM12702, R01 GM012702] Funding Source: Medline

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We previously demonstrated that mRNAs retained in the nucleus of Saccharomyces cerevisiae are subjected to a degradation system-designated DRN (degradation of mRNA in the nucleus), that is diminished in cbc1-Delta or cbc2-Delta mutants lacking components of the cap-binding complex and in rrp6-Delta mutants lacking Rrp6p, a 3' to 5' nuclear exonuclease. Two mutants, lys2-187 and lys2-121, were uncovered by screening numerous lys2 mutants for suppression by cbc1-Delta and rrp6-Delta. Both mutants were identical and contained the two base changes, one of which formed a TGA nonsense codon. L Y52 mRNAs from the lys2-187 and related mutants were rapidly degraded, and the degradation was suppressed by cbcl-Delta and rrp6-Delta. The U1A-GFP imaging procedure was used to show that the lys2-187 mRNA was partially retained in the nucleus, explaining the susceptibility to DRN. The creation of several derivatives of lys2-187 by site-directed mutagenesis revealed that the in-frame TGA by itself was not responsible for the increased susceptibility to DRN. Thus, mRNAs susceptible to DRN can be formed by a 2-bp change. Furthermore, this retention signal causing susceptibility to DRN is lost by altering one of the base pairs, establishing that mRNAs susceptible and unsusceptible to DRN can be attributed to a single nucleotide in the proper context.

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