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Journal of Virology, September 1999, p. 7710-7721, Vol. 73, No. 9
0022-538X/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
Evolution and Horizontal Transfer of
dUTPase-Encoding Genes in Viruses and Their Hosts
Angela M.
Baldo
and
Marcella A.
McClure*
Department of Biological Sciences, University
of Nevada-Las Vegas, Las Vegas, Nevada 89154-4004
Received 23 March 1999/Accepted 24 May 1999
dUTPase is a ubiquitous and essential enzyme responsible for
regulating cellular levels of dUTP. The dut gene exists as
single, tandemly duplicated, and tandemly triplicated copies.
Crystallized single-copy dUTPases have been shown to assemble as
homotrimers. dUTPase is encoded as an auxiliary gene in a number of
virus genomes. The origin of viral dut genes has remained
unresolved since their initial discovery. A comprehensive analysis of
dUTPase amino acid sequence relationships was performed to explore the
evolutionary dynamics of dut in viruses and their hosts.
Our data set, comprised of 24 host and 51 viral sequences, includes
representative sequences from available eukaryotes, archaea, eubacteria
cells, and viruses, including herpesviruses. These amino acid sequences
were aligned by using a hidden Markov model approach developed to align
divergent data. Known secondary structures from single-copy crystals
were mapped onto the aligned duplicate and triplicate sequences. We show how duplicated dUTPases might fold into a monomer, and we hypothesize that triplicated dUTPases also assemble as monomers. Phylogenetic analysis revealed at least five viral dUTPase sequence lineages in well-supported monophyletic clusters with eukaryotic, eubacterial, and archaeal hosts. We have identified all five as strong
examples of horizontal transfer as well as additional potential transfer of dut genes among eubacteria, between eubacteria
and viruses, and between retroviruses. The evidence for horizontal transfers is particularly interesting since eukaryotic dut
genes have introns, while DNA virus dut genes do not. This
implies that an intermediary retroid agent facilitated the horizontal
transfer process between host mRNA and DNA viruses.
*
Corresponding author. Mailing address: Department of
Microbiology and Center for Computational Biology, Montana State
University, P.O. Box 17320, 109 Lewis Hall, Bozeman, MT 59717-3520. Phone: (406) 994-2903. Fax: (406) 994-4926. E-mail:
mars{at}nervana@montana.edu.

Present address: Department of Plant Breeding, Cornell University,
Ithaca, N.Y.
Journal of Virology, September 1999, p. 7710-7721, Vol. 73, No. 9
0022-538X/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
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