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Structural genomics of highly conserved microbial genes of unknown function in search of new antibacterial targets
Authors:Abergel  Chantal  Coutard  Bruno  Byrne  Deborah  Chenivesse  Sabine  Claude  Jean-Baptiste  Deregnaucourt   Céline  Fricaux   Thierry  Gianesini-Boutreux  Celine  Jeudy  Sandra  Lebrun  Régine  Maza   Caroline  Notredame   Cédric  Poirot   Olivier  Suhre   Karsten  Varagnol   Majorie  Claverie   Jean-Michel
Affiliation:(1) Structural and Genomic Information Laboratory, UMR 1889 CNRS-AVENTIS, France;(2) Institute for Structural Biology and Microbiology, 31 Chemin Joseph Aiguier, 13402 Marseille cedex 20, France
Abstract:With more than 100 antibacterial drugs at our disposal in the 1980rsquos, the problem of bacterial infection was considered solved. Today, however, most hospital infections are insensitive to several classes of antibacterial drugs, and deadly strains of Staphylococcus aureus resistant to vancomycin – the last resort antibiotic – have recently begin to appear. Other life-threatening microbes, such as Enterococcus faecalis and Mycobacterium tuberculosis are already able to resist every available antibiotic. There is thus an urgent, and continuous need for new, preferably large-spectrum, antibacterial molecules, ideally targeting new biochemical pathways. Here we report on the progress of our structural genomics program aiming at the discovery of new antibacterial gene targets among evolutionary conserved genes of uncharacterized function. A series of bioinformatic and comparative genomics analyses were used to identify a set of 221 candidate genes common to Gram-positive and Gram-negative bacteria. These genes were split between two laboratories. They are now submitted to a systematic 3-D structure determination protocol including cloning, protein expression and purification, crystallization, X-ray diffraction, structure interpretation, and function prediction. We describe here our strategies for the 111 genes processed in our laboratory. Bioinformatics is used at most stages of the production process and out of 111 genes processed – and 17 months into the project – 108 have been successfully cloned, 103 have exhibited detectable expression, 84 have led to the production of soluble protein, 46 have been purified, 12 have led to usable crystals, and 7 structures have been determined.
Keywords:Escherichia coli  Structural Genomics  Comparative Genomics  Bioinformatics  anti-bacterial
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