6lty
From Proteopedia
DNA bound antitoxin HigA3
Structural highlights
FunctionHIGA3_MYCTU Putative antitoxin component of a type II toxin-antitoxin (TA) system. Its cognate toxin would be HigB3.[1] Publication Abstract from PubMedThe bacterial toxin-antitoxin (TA) system regulates cell growth under various environmental stresses. Mycobacterium tuberculosis, the causative pathogen of tuberculosis (TB), has three HigBA type II TA systems with reverse gene organization, consisting of the toxin protein HigB and labile antitoxin protein HigA. Most type II TA modules are transcriptionally autoregulated by the antitoxin itself. In this report, we first present the crystal structure of the M. tuberculosis HigA3 antitoxin (MtHigA3) and MtHigA3 bound to its operator DNA complex. We also investigated the interaction between MtHigA3 and DNA using NMR spectroscopy. The MtHigA3 antitoxin structure is a homodimer that contains a structurally well conserved DNA-binding domain at the N-terminus and a dimerization domain at the C-terminus. Upon comparing the HigA homologue structures, a distinct difference was found in the C-terminal region that possesses the beta-lid, and diverse orientations of two helix-turn-helix (HTH) motifs from HigA homologue dimers were observed. The structure of MtHigA3 bound to DNA reveals that the promoter DNA is bound to two HTH motifs of the MtHigA3 dimer presenting 46.5 degrees bending, and the distance between the two HTH motifs of each MtHigA3 monomer was increased in MtHigA3 bound to DNA. The beta-lid, which is found only in the tertiary structure of MtHigA3 among the HigA homologues, causes the formation of a tight dimerization network and leads to a unique arrangement for dimer formation that is related to the curvature of the bound DNA. This work could contribute to the understanding of the HigBA system of M. tuberculosis at the atomic level and may contribute to the development of new antibiotics for TB treatment. Induced DNA bending by unique dimerization of HigA antitoxin.,Park JY, Kim HJ, Pathak C, Yoon HJ, Kim DH, Park SJ, Lee BJ IUCrJ. 2020 Jun 26;7(Pt 4):748-760. doi: 10.1107/S2052252520006466. eCollection, 2020 Jul 1. PMID:32695421[2] From MEDLINE®/PubMed®, a database of the U.S. National Library of Medicine. References
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