| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 5505048 | Biochemical and Biophysical Research Communications | 2017 | 7 Pages |
Abstract
Tuberculosis (TB) is a severe disease caused by Mycobacterium tuberculosis (M. tb) and the well-characterized M. tb MazE/F proteins play important roles in stress adaptation. Recently, the MazF-mt9 toxin has been found to display endonuclease activities towards tRNAs but the mechanism is unknown. We hereby present the crystal structure of apo-MazF-mt9. The enzyme recognizes tRNALys with a central UUU motif within the anticodon loop, but is insensitive to the sequence context outside of the loop. Based on our crystallographic and biochemical studies, we identified key residues for catalysis and proposed the potential tRNA-binding site.
Keywords
Shanghai Synchrotron Radiation FacilityPrescission proteaseSSRFtoxin-antitoxin systemsDTTNi-NTAPMSFPSPAIDSTuberculosisToxin-antitoxinSubstrate specificitydithiothreitolCrystal structureStructure-functionWorld Health Organizationacquired immune deficiency syndrometrigger factorphenylmethylsulfonyl fluorideMycobacterium tuberculosisnickel-nitrilotriacetic acidWHO
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Authors
Ran Chen, Jie Tu, Zhihui Liu, Fanrong Meng, Pinyun Ma, Zhishan Ding, Chengwen Yang, Lei Chen, Xiangyu Deng, Wei Xie,