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Please use this identifier to cite or link to this item: http://acervodigital.unesp.br/handle/11449/34115
Title: 
Shikimate kinase: A potential target for development of novel antitubercular agents
Author(s): 
Institution: 
  • Pontificia Univ Catolica Rio Grande do Sul
  • Universidade Estadual Paulista (UNESP)
ISSN: 
1389-4501
Abstract: 
Tuberculosis (TB) remains the leading cause of mortality due to a bacterial pathogen, Mycobacterium tuberculosis. However, no new classes of drugs for TB have been developed in the past 30 years. Therefore there is an urgent need to develop faster acting and effective new antitubercular agents, preferably belonging to new structural classes, to better combat TB, including MDR-TB, to shorten the duration of current treatment to improve patient compliance, and to provide effective treatment of latent tuberculosis infection. The enzymes in the shikimate pathway are potential targets for development of a new generation of antitubercular drugs. The shikimate pathway has been shown by disruption of aroK gene to be essential for the Mycobacterium tuberculosis. The shikimate kinase (SK) catalyses the phosphorylation of the 3-hydroxyl group of shikimic acid (shikimate) using ATP as a co-substrate. SK belongs to family of nucleoside monophosphate (NMP) kinases. The enzyme is an alpha/beta protein consisting of a central sheet of five parallel beta-strands flanked by alpha-helices. The shikimate kinases are composed of three domains: Core domain, Lid domain and Shikimate-binding domain. The Lid and Shikimate-binding domains are responsible for large conformational changes during catalysis. More recently, the precise interactions between SK and substrate have been elucidated, showing the binding of shikimate with three charged residues conserved among the SK sequences. The elucidation of interactions between MtSK and their substrates is crucial for the development of a new generation of drugs against tuberculosis through rational drug design.
Issue Date: 
1-Mar-2007
Citation: 
Current Drug Targets. Sharjah: Bentham Science Publ Ltd, v. 8, n. 3, p. 459-468, 2007.
Time Duration: 
459-468
Publisher: 
Bentham Science Publ Ltd
Keywords: 
  • tuberculosis
  • Malária
  • shikimate kinase
  • shikimate pathway
  • drug design
  • drug target
  • Mycobacterium tuberculosis
  • Plasmodium
Source: 
http://dx.doi.org/10.2174/138945007780059013
URI: 
Access Rights: 
Acesso restrito
Type: 
outro
Source:
http://repositorio.unesp.br/handle/11449/34115
Appears in Collections:Artigos, TCCs, Teses e Dissertações da Unesp

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