Cyclin-dependent protein kinases as therapeutic drug targets for antimalarial drug development

被引:37
|
作者
Waters, NC
Geyer, JA
机构
[1] USA, Army Med Res Unit, Nairobi 09831, Kenya
[2] Walter Reed Army Inst Res, Div Expt Therapeut, Silver Spring, MD 20910 USA
关键词
cell cycle; cyclin-dependent protein kinase (CDK); drug development; kinase inhibitors; malaria; Pfmrk; PfPK5; PfPK6; Plasmodium falciparum;
D O I
10.1517/eott.7.1.7.21162
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Cyclin-dependent protein kinases (CDKs) have been attractive drug targets for the development of anticancer therapies due to their direct and crucial role in the regulation of cellular proliferation. Following this trend, CDKs have been pursued as potential drug targets for several other diseases. Structure-based drug design programmes have focused on the plasmodial CDKs to develop new candidate antimalarial compounds. This review discusses the most recent advances relating to three Plasmodium falciparum CDKs (PfPK5, PfPK6 and Pfmrk) as they are developed as antimalarial drug targets. CDKs are highly conserved, and focus must,be placed upon the amino acid differences between human and plasmodial CDKs in order to develop specific inhibitors. Comparisons of the active sites of human and parasite CDKs reveal sequence and potential structural variations. Using sequence analysis, molecular modelling and in vitro drug screening, it is possible to identify and develop inhibitors that specifically target the plasmodial CDKs. These efforts are aimed at identifying new classes of CDK inhibitors that may be exploited for antimalarial drug development.
引用
收藏
页码:7 / 17
页数:11
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