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From Genetic Footprinting to Antimicrobial Drug Targets: Examples in Cofactor Biosynthetic Pathways

Svetlana Y. Gerdes, Michael D. Scholle, Mark D'Souza, Axel Bernal, Mark V. Baev, Michael Farrell, Oleg V. Kurnasov, Matthew D. Daugherty, Faika Mseeh, Boris M. Polanuyer, John W. Campbell, Shubha Anantha, Konstantin Y. Shatalin, Shamim A. K. Chowdhury, Michael Y. Fonstein, Andrei L. Osterman
Svetlana Y. Gerdes
Integrated Genomics Inc., Chicago, Illinois 60612
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Michael D. Scholle
Integrated Genomics Inc., Chicago, Illinois 60612
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Mark D'Souza
Integrated Genomics Inc., Chicago, Illinois 60612
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Axel Bernal
Integrated Genomics Inc., Chicago, Illinois 60612
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Mark V. Baev
Integrated Genomics Inc., Chicago, Illinois 60612
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Michael Farrell
Integrated Genomics Inc., Chicago, Illinois 60612
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Oleg V. Kurnasov
Integrated Genomics Inc., Chicago, Illinois 60612
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Matthew D. Daugherty
Integrated Genomics Inc., Chicago, Illinois 60612
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Faika Mseeh
Integrated Genomics Inc., Chicago, Illinois 60612
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Boris M. Polanuyer
Integrated Genomics Inc., Chicago, Illinois 60612
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John W. Campbell
Integrated Genomics Inc., Chicago, Illinois 60612
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Shubha Anantha
Integrated Genomics Inc., Chicago, Illinois 60612
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Konstantin Y. Shatalin
Integrated Genomics Inc., Chicago, Illinois 60612
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Shamim A. K. Chowdhury
Integrated Genomics Inc., Chicago, Illinois 60612
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Michael Y. Fonstein
Integrated Genomics Inc., Chicago, Illinois 60612
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Andrei L. Osterman
Integrated Genomics Inc., Chicago, Illinois 60612
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  • For correspondence: andrei@integratedgenomics.com
DOI: 10.1128/JB.184.16.4555-4572.2002
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ABSTRACT

Novel drug targets are required in order to design new defenses against antibiotic-resistant pathogens. Comparative genomics provides new opportunities for finding optimal targets among previously unexplored cellular functions, based on an understanding of related biological processes in bacterial pathogens and their hosts. We describe an integrated approach to identification and prioritization of broad-spectrum drug targets. Our strategy is based on genetic footprinting in Escherichia coli followed by metabolic context analysis of essential gene orthologs in various species. Genes required for viability of E. coli in rich medium were identified on a whole-genome scale using the genetic footprinting technique. Potential target pathways were deduced from these data and compared with a panel of representative bacterial pathogens by using metabolic reconstructions from genomic data. Conserved and indispensable functions revealed by this analysis potentially represent broad-spectrum antibacterial targets. Further target prioritization involves comparison of the corresponding pathways and individual functions between pathogens and the human host. The most promising targets are validated by direct knockouts in model pathogens. The efficacy of this approach is illustrated using examples from metabolism of adenylate cofactors NAD(P), coenzyme A, and flavin adenine dinucleotide. Several drug targets within these pathways, including three distantly related adenylyltransferases (orthologs of the E. coli genes nadD, coaD, and ribF), are discussed in detail.

  • Copyright © 2002 American Society for Microbiology
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From Genetic Footprinting to Antimicrobial Drug Targets: Examples in Cofactor Biosynthetic Pathways
Svetlana Y. Gerdes, Michael D. Scholle, Mark D'Souza, Axel Bernal, Mark V. Baev, Michael Farrell, Oleg V. Kurnasov, Matthew D. Daugherty, Faika Mseeh, Boris M. Polanuyer, John W. Campbell, Shubha Anantha, Konstantin Y. Shatalin, Shamim A. K. Chowdhury, Michael Y. Fonstein, Andrei L. Osterman
Journal of Bacteriology Aug 2002, 184 (16) 4555-4572; DOI: 10.1128/JB.184.16.4555-4572.2002

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From Genetic Footprinting to Antimicrobial Drug Targets: Examples in Cofactor Biosynthetic Pathways
Svetlana Y. Gerdes, Michael D. Scholle, Mark D'Souza, Axel Bernal, Mark V. Baev, Michael Farrell, Oleg V. Kurnasov, Matthew D. Daugherty, Faika Mseeh, Boris M. Polanuyer, John W. Campbell, Shubha Anantha, Konstantin Y. Shatalin, Shamim A. K. Chowdhury, Michael Y. Fonstein, Andrei L. Osterman
Journal of Bacteriology Aug 2002, 184 (16) 4555-4572; DOI: 10.1128/JB.184.16.4555-4572.2002
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KEYWORDS

Coenzyme A
Escherichia coli
Flavin-Adenine Dinucleotide
NADP

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