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Vol. 10, Issue 11, 3567-3581, November 1999
Department of Obstetrics, Gynecology, and Reproductive Sciences,
University of California School of Medicine, San Francisco, California
94143-0556
During oocyte maturation in Xenopus, previously
quiescent maternal mRNAs are translationally activated at specific
times. We hypothesized that the translational recruitment of individual messages is triggered by particular cellular events and investigated the potential for known effectors of the meiotic cell cycle to activate
the translation of the FGF receptor-1 (XFGFR) maternal mRNA. We found
that both c-mos and cdc2 activate the translation of
XFGFR. However, although oocytes matured by injection of recombinant cdc2/cyclin B translate normal levels of XFGFR protein,
c-mos depletion reduces the level of XFGFR protein
induced by cdc2/cyclin B injection. In oocytes blocked for cdc2
activity, injection of mos RNA induced low levels of XFGFR protein,
independent of MAPK activity. Through the use of injected reporter
RNAs, we show that the XFGFR 3' untranslated region inhibitory element
is completely derepressed by cdc2 alone. In addition, we identified a
new inhibitory element through which both mos and cdc2 activate
translation. We found that cdc2 derepresses translation in the absence
of polyadenylation, whereas mos requires poly(A) extension to activate
XFGFR translation. Our results demonstrate that mos and cdc2, in
addition to functioning as key regulators of the meiotic cell cycle,
cooperate in the translational activation of a specific maternal mRNA
during oocyte maturation.
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