Peptidoglycan (PG) serves as an essential target for antimicrobial development. An overlooked reservoir of antimicrobials lies in the form of PG-hydrolyzing enzymes naturally produced for polymicrobial competition, particularly those associated with the type VI secretion system (T6SS). Here, we report that a T6SS effector TseP, from Aeromonas dhakensis, represents a family of effectors with dual amidase-lysozyme activities. In vitro PG-digestion coupled with LC-MS analysis revealed the N-domain's amidase activity, which is neutralized by either catalytic mutations or the presence of the immunity protein TsiP. The N-domain, but not the C-domain, of TseP is sufficient to restore T6SS secretion in T6SS-defective mutants, underscoring its critical structural role. Using pull-down and secretion assays, we showed that these two domains interact directly with a carrier protein VgrG2 and can be secreted separately. Homologs in Aeromonas hydrophila and Pseudomonas syringae exhibited analogous dual functions. Additionally, N- and C-domains display distinctive GC contents, suggesting an evolutionary fusion event. By altering the surface charge through structural-guided design, we engineered the TseP(C4+) effector that successfully lyses otherwise resistant Bacillus subtilis cells, enabling the T6SS to inhibit B. subtilis in a contact-independent manner. This research uncovers TseP as a new family of bifunctional chimeric effectors targeting PG, offering a potential strategy to harness these proteins in the fight against antimicrobial resistance.
Amidase and lysozyme dual functions in TseP reveal a new family of chimeric effectors in the type VI secretion system.
TseP 中的酰胺酶和溶菌酶的双重功能揭示了 VI 型分泌系统中一类新的嵌合效应蛋白
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作者:Wang Zeng-Hang, An Ying, Zhao Ting, Pei Tong-Tong, Wang Dora Yuping, Liang Xiaoye, Qin Wenming, Dong Tao
| 期刊: | Elife | 影响因子: | 6.400 |
| 时间: | 2025 | 起止号: | 2025 Mar 10; 13:RP101125 |
| doi: | 10.7554/eLife.101125 | 研究方向: | 免疫/内分泌 |
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