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Published online before print March 5, 2008
A more recent version of this article appeared on March 1, 2008
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pr.107.07110v1
60/1/128    most recent
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© 2008 by the American Society for Pharmacology and Experimental Therapeutics
Pharmacological Reviews, 10.1124/pr.107.07110


Review Articles

Sortase as a Target of Anti-Infective Therapy

Anthony W. Maresso 1 Olaf Schneewind 1

1 Department of Microbiology, University of Chicago, Chicago, Illinois


   Abstract

The rise in antibiotic-resistant bacteria is a major concern, in particular because it includes many different species of pathogenic microbes. These |P`superbugs|P' are further characterized by high levels of virulence and disease-associated mortality. There seems to be few new antibiotics in the drug discovery pipeline; recent work has sought to define and validate new drug targets. The assembly of surface proteins and pili in the cell wall envelope of Gram-positive bacteria is catalyzed by sortase. Sortase cleaves a conserved C-terminal sequence of these polypeptides to generate an acyl-enzyme intermediate. The acyl-enzyme is next resolved by nucleophilic attack by the amino groups within cell wall cross-bridges or pilin proteins, thereby covalently attaching the polypeptides to the cell wall or the next pilin subunit. Sortase substrates function as adhesins, internalins, blood clotting and immune evasion factors, and transporters for nutrients across the microbial cell wall envelope; without them, most pathogens cannot sustain an infection. Here we review what is known about sortase catalysis and surface protein function, how surface protein anchoring can be inhibited, and what prospects such inhibition may have for anti-infective therapy.







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