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(Received for publication, April 10, 1997, and in revised form, June 12, 1997)
From Cold Spring Harbor Laboratory, Cold Spring Harbor,
New York 11724
tat, an essential gene of human
immunodeficiency virus, when placed under the control of the RNA
polymerase III promoter from the adenovirus VA
RNA1 gene, is transcribed into an uncapped and nonpolyadenylated mRNA. This VA-Tat RNA is translated to produce functional Tat protein in transfected mammalian cells (Gunnery, S., and
Mathews, M. B. (1995) Mol. Cell. Biol. 15, 3597-3607). The presence of an upstream open reading frame (ORF) in
VA-Tat RNA is inhibitory to the translation of the Tat ORF, suggesting that the RNA is scanned during translation even though it is uncapped. Because the effect of the upstream ORF is relatively small (about 2-fold), we sought more definitive evidence of scanning by introducing secondary structures of varying stabilities into the 5
Volume 272, Number 34,
Issue of August 22, 1997
pp. 21642-21646
©1997 by The American Society for Biochemistry and Molecular Biology, Inc.
-untranslated region of VA-Tat RNA. The results of transfection experiments showed
that highly stable secondary structure was inhibitory to Tat synthesis,
whereas structures of lower stability were not inhibitory, confirming
that uncapped mRNA is subject to scanning. Furthermore, translation
of the downstream ORF was reduced but not eliminated by mutations that
caused the upstream ORF to overlap the Tat ORF. Extending the overlap
of the two ORFs further decreased the translation of the downstream
ORF. This observation implies that ribosomes reinitiate after
termination, possibly after migrating in a 3 to 5 direction through
the overlap region of the mRNA. Similar results were obtained with
a capped polymerase II transcript, indicating that the translation
of polymerase II and polymerase III transcripts occurs through
similar mechanisms.
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