利用生物膜蛋白Pase 1作为新型分散剂对抗多重耐药革兰氏阴性菌的联合治疗

Michelle J. Lin
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引用次数: 0

摘要

耐多药革兰氏阴性(MDRGN)细菌中抗菌素耐药基因的出现导致死亡率大幅增加,并对全球健康构成重大威胁。目前的治疗方法甚至最后手段药物(DoLRs)都未能成功治疗这些感染,因此需要一种新的和立即的解决方案。本文主要研究了一种最佳的共处理分散剂的合成和研究。先前对鲍曼不动杆菌(ESKAPE的一种高毒力的医院内革兰氏阴性病原体)的基因组进行筛选,鉴定出假设的基因片段Pase 1具有细菌分散的潜在特征。通过对多种多重耐药革兰氏阴性细菌生物膜和ESKAPE病原菌的处理,结果表明AB-Pase 1作为共处理分散剂表现出最佳特性,与大肠杆菌pase 1相比,具有更高的分散百分比和可控的分散速率。因此,随着AB-Pase 1在联合治疗中的扩展,成功对抗多重耐药细菌的潜力巨大,这是医学领域的重大突破。
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Combating Multidrug-Resistant Gram-Negative Bacteria Using Biofilm Protein Pase 1 as Novel Dispersal Agent for Co-Treatment Therapy
The emergence of antimicrobial resistance genes in multidrug-resistant gram-negative (MDRGN) bacteria leads to an immense increase in mortality rates and poses a major threat to global health. Current treatment methods and even drugs of last resort (DoLRs) have failed to successfully treat these infections, warranting the need for a new and immediate solution. This study focuses on the synthesis and investigation of an optimal dispersal agent for co-treatment. Previous screening of the genome of Acinetobacter baumannii, a highly virulent nosocomial gram-negative pathogen of ESKAPE, identified the hypothetical gene segment Pase 1 with potential characteristics of bacterial dispersion. Through treatment of various multidrug-resistant gram-negative bacterial biofilms and ESKAPE pathogens, the results indicated that AB-Pase 1 exhibited optimal characteristics as a co-treatment dispersal agent, with higher dispersion percentages and controlled dispersal rates in comparison to E. coli-Pase 1. Therefore, with the expansion of AB-Pase 1 in co-treatment therapy, there is an immense potential for successfully combating multi-resistant bacteria, a crucial breakthrough in the medical field.
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