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An essential bifunctional enzyme in Mycobacterium tuberculosis for itaconate dissimilation and leucine catabolism

Proc Natl Acad Sci U S A. 2019-07; 
Hua Wang, Alexander A Fedorov, Elena V Fedorov, Debbie M Hunt, Angela Rodgers, Holly L Douglas, Acely Garza-Garcia, Jeffrey B Bonanno, Steven C Almo, Luiz Pedro Sório de Carvalho
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Gene Synthesis Gene sequences for PA0883, PA2011, and MMC lyase were codon-optimized for Escherichia coli (E. coli) expression, synthesised, and then cloned (NdeI-BamHI) into pET-16b by GenScript (Piscataway, NJ). Get A Quote

摘要

Mycobacterium tuberculosis (Mtb) is the etiological agent of tuberculosis. One-fourth of the global population is estimated to be infected with Mtb, accounting for ∼1.3 million deaths in 2017. As part of the immune response to Mtb infection, macrophages produce metabolites with the purpose of inhibiting or killing the bacterial cell. Itaconate is an abundant host metabolite thought to be both an antimicrobial agent and a modulator of the host inflammatory response. However, the exact mode of action of itaconate remains unclear. Here, we show that Mtb has an itaconate dissimilation pathway and that the last enzyme in this pathway, Rv2498c, also participates in l-leucine catabolism. Our results from phylogeneti... More

关键词

Mycobacterium tuberculosis; carbon–carbon bond lyase; enzyme function; itaconate catabolism; leucine catabolism.