Nature

The genome of the bacterium Borrelia burgdorferi B31, the aetiologic agent of Lyme disease, contains a linear chromosome of 910,725 base pairs and at least 17 linear and circular plasmids with a combined size of more than 533,000 base pairs. The chromosome contains 853 genes encoding a basic set of proteins for DNA replication, transcription, translation, solute transport and energy metabolism, but, like Mycoplasma genitalium, it contains no genes for cellular biosynthetic reactions. Because B. burgdorferi and M. genitalium are distantly related eubacteria, we suggest that their limited metabolic capacities reflect convergent evolution by gene loss from more metabolically competent progenitors. Of 430 genes on 11 plasmids, most have no known biological function; 39% of plasmid genes are paralogues that form 47 gene families. The biological significance of the multiple plasmid-encoded genes is not clear, although they may be involved in antigenic variation or immune evasion.

Source:http://purl.uniprot.org/citations/9403685

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Predicate	Object
rdf:type	uniprot:Journal_Citation
rdfs:comment	The genome of the bacterium Borrelia burgdorferi B31, the aetiologic agent of Lyme disease, contains a linear chromosome of 910,725 base pairs and at least 17 linear and circular plasmids with a combined size of more than 533,000 base pairs. The chromosome contains 853 genes encoding a basic set of proteins for DNA replication, transcription, translation, solute transport and energy metabolism, but, like Mycoplasma genitalium, it contains no genes for cellular biosynthetic reactions. Because B. burgdorferi and M. genitalium are distantly related eubacteria, we suggest that their limited metabolic capacities reflect convergent evolution by gene loss from more metabolically competent progenitors. Of 430 genes on 11 plasmids, most have no known biological function; 39% of plasmid genes are paralogues that form 47 gene families. The biological significance of the multiple plasmid-encoded genes is not clear, although they may be involved in antigenic variation or immune evasion.
skos:exactMatch	http://purl.uniprot.org/medline/98065943, http://purl.uniprot.org/pubmed/9403685
uniprot:name	Nature
uniprot:author	Adams M.D., Artiach P., Bowman C., Casjens S., Clayton R.A., Cotton M.D., Dodson R.J., Dougherty B.A., Fleischmann R.D., Fraser C.M., Fujii C., Garland S.A., Gocayne J.D., Gwinn M.L., Hanson M., Hatch B., Hickey E.K., Horst K., Huang W.M., Kerlavage A.R., Ketchum K.A., Lathigra R., McDonald L.A., Palmer N., Peterson J.D., Quackenbush J., Richardson D.L., Roberts K.M., Salzberg S.L., Smith H.O., Sutton G.G., Tomb J.-F., Utterback T.R., Venter J.C., Watthey L., Weidman J.F., White O., van Vugt R.
uniprot:date	1997
uniprot:pages	580-586
uniprot:title	Genomic sequence of a Lyme disease spirochaete, Borrelia burgdorferi.
uniprot:volume	390
dc-term:identifier	doi:10.1038/37551