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Mol Cell Biol, August 1998, p. 4509-4518, Vol. 18, No. 8
0270-7306/98/$04.00+0
Copyright © 1998, American Society for Microbiology. All rights reserved.
The Host Gene for Intronic U17 Small Nucleolar RNAs in Mammals
Has No Protein-Coding Potential and Is a Member of the 5'-Terminal
Oligopyrimidine Gene Family
Pawel
Pelczar and
Witold
Filipowicz*
Friedrich Miescher-Institut, CH-4002 Basel,
Switzerland
Received 18 February 1998/Returned for modification 30 March
1998/Accepted 11 May 1998
Intron-encoded U17a and U17b RNAs are members of the H/ACA-box
class of small nucleolar RNAs (snoRNAs) participating in rRNA processing and modification. We have investigated the organization and
expression of the U17 locus in human cells and found that intronic U17a
and U17b sequences are transcribed as part of the three-exon
transcription unit, named U17HG, positioned approximately 9 kb upstream of the RCC1 locus. Comparison of the human and
mouse U17HG genes has revealed that snoRNA-encoding intron
sequences but not exon sequences are conserved between the two species
and that neither human nor mouse spliced U17HG
poly(A)+ RNAs have the potential to code for proteins.
Analyses of polysome profiles and effects of translation inhibitors on
the abundance of U17HG RNA in HeLa cells indicated that
despite its cytoplasmic localization, little if any U17HG
RNA is associated with polysomes. This distinguishes U17HG
RNA from another non-protein-coding snoRNA host gene product,
UHG RNA, described previously (K. T. Tycowski, M. D. Shu, and J. A. Steitz, Nature 379:464-466, 1996).
Determination of the 5' terminus of the U17HG RNA revealed
that transcription of the U17HG gene starts with a C
residue followed by a polypyrimidine tract, making this gene a member
of the 5'-terminal oligopyrimidine (5'TOP) family, which includes genes
encoding ribosomal proteins and some translation factors.
Interestingly, other known snoRNA host genes, including the
UHG gene (Tycowski et al., op. cit.), have features of the
5'TOP genes. Similar characteristics of the transcription start site
regions in snoRNA host and ribosomal protein genes raise the
possibility that expression of components of ribosome biogenesis and
translational machineries is coregulated.
*
Corresponding author. Mailing address: Friedrich
Miescher-Institut, P.O. Box 2543, CH-4002 Basel, Switzerland. Phone:
(61) 6976993 or 6978234. Fax: (61) 6973976. E-mail:
Filipowi{at}FMI.CH.
Mol Cell Biol, August 1998, p. 4509-4518, Vol. 18, No. 8
0270-7306/98/$04.00+0
Copyright © 1998, American Society for Microbiology. All rights reserved.
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