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Novel polyadenylylation-dependent neutralization mechanism of the HEPN/MNT toxin/antitoxin system

Jianyun Yao, Xiangkai Zhen, Kaihao Tang, Tianlang Liu, Xiaolong Xu, Zhe Chen, Yunxue Guo, Xiaoxiao Liu, Thomas K. Wood, Songying Ouyang, Xiaoxue Wang

2020Nucleic Acids Research45 citationsDOIOpen Access PDF

Abstract

The two-gene module HEPN/MNT is predicted to be the most abundant toxin/antitoxin (TA) system in prokaryotes. However, its physiological function and neutralization mechanism remains obscure. Here, we discovered that the MntA antitoxin (MNT-domain protein) acts as an adenylyltransferase and chemically modifies the HepT toxin (HEPN-domain protein) to block its toxicity as an RNase. Biochemical and structural studies revealed that MntA mediates the transfer of three AMPs to a tyrosine residue next to the RNase domain of HepT in Shewanella oneidensis. Furthermore, in vitro enzymatic assays showed that the three AMPs are transferred to HepT by MntA consecutively with ATP serving as the substrate, and this polyadenylylation is crucial for reducing HepT toxicity. Additionally, the GSX10DXD motif, which is conserved among MntA proteins, is the key active motif for polyadenylylating and neutralizing HepT. Thus, HepT/MntA represents a new type of TA system, and the polyadenylylation-dependent TA neutralization mechanism is prevalent in bacteria and archaea.

Topics & Concepts

BiologyAntitoxinNeutralizationToxinMechanism (biology)VirologyComputational biologyMicrobiologyVirusPhilosophyEpistemologyBacterial Genetics and BiotechnologyAntibiotic Resistance in BacteriaEnzyme Structure and Function