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Pyrimidine Salvage Enzymes Are Essential for De Novo Biosynthesis of Deoxypyrimidine Nucleotides in Trypanosoma brucei.

PLoS Pathog.. 2016; 
LeijaChristopher,Rijo-FerreiraFilipa,KinchLisa N,GrishinNick V,NischanNicole,KohlerJennifer J,HuZeping,PhillipsMargar
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Gene Synthesis Finally, the remaining TK allele was replaced by a PAC resistance gene synthesized by GenScript...The gene encoding the HsTK open reading frame was synthesized by GenScript and cloned into the pUC57 vector, Get A Quote

摘要

The human pathogenic parasite Trypanosoma brucei possess both de novo and salvage routes for the biosynthesis of pyrimidine nucleotides. Consequently, they do not require salvageable pyrimidines for growth. Thymidine kinase (TK) catalyzes the formation of dTMP and dUMP and is one of several salvage enzymes that appear redundant to the de novo pathway. Surprisingly, we show through analysis of TK conditional null and RNAi cells that TK is essential for growth and for infectivity in a mouse model, and that a catalytically active enzyme is required for its function. Unlike humans, T. brucei and all other kinetoplastids lack dCMP deaminase (DCTD), which provides an alternative route to dUMP formation. Ect... More

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