Rhodes Jaime D, Kelly Tyler J, Goodman Steven D, Bakaletz Lauren O
Center for Microbial Pathogenesis, Abigail Wexner Research Institute at Nationwide Children's Hospital, Columbus, OH, 43205, United States.
Department of Pediatrics, The Ohio State University College of Medicine, Columbus, OH, 43210, United States.
FEMS Microbiol Lett. 2025 Jan 10;372. doi: 10.1093/femsle/fnaf029.
Bacterial biofilms mediate chronic and recurrent bacterial infections that are extremely difficult to treat by currently available standards of care. In nature, these encased bacterial communities are typically comprised of more than one genus or species. Specifically, in the airway, nontypeable Haemophilus influenzae (NTHI) predominates and is commonly isolated with one or more of the following co-pathogens with which it forms unique relationships: methicillin-resistant Staphylococcus aureus, Burkholderia cenocepacia, Pseudomonas aeruginosa, Streptococcus pneumoniae, and Moraxella catarrhalis. We recently showed that dual-genera biofilms comprised of NTHI plus a co-pathogen are disrupted when the biofilm matrix is destabilized by a pathogen-directed strategy that uses a humanized monoclonal antibody directed against the protective domains of bacterial DNABII proteins found at vertices of crossed strands of eDNA within the biofilm matrix. We also recently showed that a peptide synthesized from the host innate immune effector High Mobility Group Box 1 (HMGB1), called mB Box-97syn, competitively inhibits binding of the bacterial DNABII proteins to eDNA, which thereby also destabilizes single-species biofilms to release biofilm-resident bacteria into a transient yet highly vulnerable state that is more effectively cleared by the host innate immune system and/or antibiotics. Here, we expanded upon these studies to assess the ability of host-augmenting mB Box-97syn to both disrupt two-genera biofilms formed by NTHI plus a common co-pathogen, and prevent their formation. Disruption of established two-genera biofilms ranged from 57% to 88%, whereas prevention of two-genera biofilm formation ranged from 65% to 80% (P = .002 to P < .0001). The sobering recalcitrance of chronic and recurrent respiratory tract infections, combined with growing global concern of antimicrobial resistance (AMR), demands development of more effective management and prevention options. Ideally, novel treatment strategies would both target the pathogens and augment the host's natural abilities to eradicate them. Herein, we provide additional data to support continued development of the latter concept via demonstration of mB Box-97syn's efficacy against polymicrobial biofilms.
细菌生物膜介导的慢性和复发性细菌感染,按照目前可用的治疗标准极难治疗。在自然界中,这些被包裹的细菌群落通常由不止一个属或种组成。具体而言,在气道中,不可分型流感嗜血杆菌(NTHI)占主导地位,并且通常与以下一种或多种共病原体一起分离出来,它与这些共病原体形成独特的关系:耐甲氧西林金黄色葡萄球菌、洋葱伯克霍尔德菌、铜绿假单胞菌、肺炎链球菌和卡他莫拉菌。我们最近发现,当生物膜基质被一种病原体导向策略破坏稳定时,由NTHI加一种共病原体组成的双属生物膜会被破坏,该策略使用一种人源化单克隆抗体,该抗体针对在生物膜基质内eDNA交叉链顶点发现的细菌DNABII蛋白的保护结构域。我们最近还发现,一种由宿主先天免疫效应物高迁移率族蛋白B1(HMGB1)合成的肽,称为mB Box-97syn,竞争性抑制细菌DNABII蛋白与eDNA的结合,从而也破坏单物种生物膜的稳定,将生物膜内的细菌释放到一个短暂但高度脆弱的状态,宿主先天免疫系统和/或抗生素能更有效地清除这种状态下的细菌。在此,我们扩展了这些研究,以评估增强宿主的mB Box-97syn破坏由NTHI加一种常见共病原体形成的双属生物膜以及防止其形成的能力。已形成的双属生物膜的破坏率在57%至88%之间,而双属生物膜形成的预防率在65%至80%之间(P = 0.002至P < 0.0001)。慢性和复发性呼吸道感染令人清醒的顽固性,加上全球对抗菌素耐药性(AMR)的日益关注,需要开发更有效的管理和预防方案。理想情况下,新的治疗策略既要针对病原体,又要增强宿主根除病原体的天然能力。在此,我们通过证明mB Box-97syn对多微生物生物膜的疗效,提供额外数据以支持后一种概念的持续发展。
