Dickey Seth W, Burgin Dylan J, Antwi Ama N, Villaruz Amer, Galac Madeline R, Cheung Gordon Y C, Rostovtseva Tatiana K, Worrall Liam J, Lazarski Aleksander C, Cino Elio A, Tieleman D Peter, Bezrukov Sergey M, Strynadka Natalie C J, Otto Michael
National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD, USA.
Department of Veterinary Medicine, University of Maryland, College Park, MD, USA.
Nat Commun. 2025 Aug 6;16(1):7231. doi: 10.1038/s41467-025-62604-1.
Bacteriocin peptides are weapons of inter-bacterial warfare and belong to the larger group of antimicrobial peptides (AMPs), which are frequently proposed as alternatives to antibiotics. Many AMPs kill by destroying the target's cytoplasmic membrane using short-lived membrane perturbations. Contrastingly, protein toxins form large pores by stably assembling in the target membrane. Here we describe an AMP class termed TMcins (for transmembrane helix-containing bacteriocin), in which half of the AMP forms a transmembrane helix. This characteristic allows TMcin to assemble into stable and large oligomeric pores. The biosynthetic locus of TMcin, which was broadly active against Gram-positive bacteria, is distributed throughout two major bacterial phyla, yet bears no homology to previously reported bacteriocin biosynthetic gene clusters. Our discovery of an AMP class that achieves pore stability otherwise only found in protein toxins transforms our current understanding of AMP structure and function and underscores the continuing importance of phenotype-initiated investigations in uncovering wholly uncharacterized antimicrobials.
细菌素肽是细菌间战争的武器,属于更大的抗菌肽(AMPs)类别,抗菌肽常被提议作为抗生素的替代品。许多抗菌肽通过短暂的膜扰动破坏靶标的细胞质膜来杀死细胞。相比之下,蛋白质毒素通过在靶膜中稳定组装形成大孔。在这里,我们描述了一类称为TMcins(含跨膜螺旋的细菌素)的抗菌肽,其中一半的抗菌肽形成跨膜螺旋。这一特性使TMcin能够组装成稳定的大寡聚孔。TMcin的生物合成位点对革兰氏阳性菌具有广泛活性,分布在两个主要细菌门中,但与先前报道的细菌素生物合成基因簇没有同源性。我们发现了一类抗菌肽,其能实现孔稳定性,而这种稳定性以前仅在蛋白质毒素中发现,这改变了我们目前对抗菌肽结构和功能的理解,并强调了在发现完全未表征的抗菌剂方面,基于表型的研究仍然具有重要意义。
Zotero 插件
