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Journal of Bacteriology, May 1999, p. 3293-3297, Vol. 181, No. 10
Department of Biotechnology, Graduate School
of Engineering, Osaka University, 2-1 Yamadaoka, Suita, Osaka
565-0871, Japan
Received 9 November 1998/Accepted 8 March 1999
BarA of Streptomyces virginiae is a specific receptor
protein for virginiae butanolide (VB), one of the
0021-9193/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
Identification and In Vivo Functional Analysis of a Virginiamycin
S Resistance Gene (varS) from Streptomyces
virginiae
-butyrolactone
autoregulators of the Streptomyces species, and acts as a
transcriptional regulator controlling both virginiamycin production and
VB biosynthesis. The downstream gene barB, the
transcription of which is under the tight control of the VB-BarA
system, was found to be transcribed as a polycistronic mRNA with its
downstream region, and DNA sequencing revealed a 1,554-bp open reading
frame (ORF) beginning at 161 bp downstream of the barB
termination codon. The ORF product showed high homology (68 to 73%) to
drug efflux proteins having 14 transmembrane segments and was named
varS (for S. virginiae antibiotic resistance). Heterologous expression of varS with S. lividans as a host resulted in virginiamycin S-specific
resistance, suggesting that varS encoded a virginiamycin
S-specific transport protein. Northern blot analysis indicated that the
bicistronic transcript of barB-varS appeared 1 to 2 h
before the onset of virginiamycin M1 and S production, at
which time VB was produced, while exogenously added virginiamycin S
apparently induced the monocistronic varS transcript.
*
Corresponding author. Mailing address: Department of
Biotechnology, Graduate School of Engineering, Osaka University, 2-1 Yamadaoka, Suita, Osaka 565-0871, Japan. Phone: 81-6-6879-7433. Fax: 81-6-6879-7432. E-mail:
nihira{at}biochem.bio.eng.osaka-u.ac.jp.
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