Gitanjali Bhushan, Victor Castano, Tania Wong Fok Lung, Courtney Chandler, Thomas H McConville, Robert K Ernst, Alice S Prince, Danielle Ahn
{"title":"耐大肠菌素肺炎克雷伯氏菌的脂质 A 修饰不会改变肺炎小鼠模型的先天免疫反应。","authors":"Gitanjali Bhushan, Victor Castano, Tania Wong Fok Lung, Courtney Chandler, Thomas H McConville, Robert K Ernst, Alice S Prince, Danielle Ahn","doi":"10.1128/iai.00016-24","DOIUrl":null,"url":null,"abstract":"<p><p>Polymyxin resistance in carbapenem-resistant <i>Klebsiella pneumoniae</i> bacteria is associated with high morbidity and mortality in vulnerable populations throughout the world. Ineffective antimicrobial activity by these last resort therapeutics can occur by transfer of <i>mcr-1</i>, a plasmid-mediated resistance gene, causing modification of the lipid A portion of lipopolysaccharide (LPS) and disruption of the interactions between polymyxins and lipid A. Whether this modification alters the innate host immune response or carries a high fitness cost in the bacteria is not well established. To investigate this, we studied infection with <i>K. pneumoniae</i> (KP) ATCC 13883 harboring either the <i>mcr-1</i> plasmid (p<i>mcr-1</i>) or the vector control (pBCSK) ATCC 13883. Bacterial fitness characteristics of <i>mcr-1</i> acquisition were evaluated. Differentiated human monocytes (THP-1s) were stimulated with KP bacterial strains or purified LPS from both parent isolates and isolates harboring <i>mcr-1</i>. Cell culture supernatants were analyzed for cytokine production. A bacterial pneumonia model in WT C57/BL6J mice was used to monitor immune cell recruitment, cytokine induction, and bacterial clearance in the bronchoalveolar lavage fluid (BALF). Isolates harboring <i>mcr-1</i> had increased colistin MIC compared to the parent isolates but did not alter bacterial fitness. Few differences in cytokines were observed with purified LPS from <i>mcr-1</i> expressing bacteria <i>in vitro</i>. However, in a mouse pneumonia model, no bacterial clearance defect was observed between p<i>mcr-1</i>-harboring KP and parent isolates. Consistently, no differences in cytokine production or immune cell recruitment in the BALF were observed, suggesting that other mechanisms outweigh the effect of these lipid A mutations in LPS.</p>","PeriodicalId":13541,"journal":{"name":"Infection and Immunity","volume":" ","pages":"e0001624"},"PeriodicalIF":2.9000,"publicationDate":"2024-06-11","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.ncbi.nlm.nih.gov/pmc/articles/PMC11237409/pdf/","citationCount":"0","resultStr":"{\"title\":\"Lipid A modification of colistin-resistant <i>Klebsiella pneumoniae</i> does not alter innate immune response in a mouse model of pneumonia.\",\"authors\":\"Gitanjali Bhushan, Victor Castano, Tania Wong Fok Lung, Courtney Chandler, Thomas H McConville, Robert K Ernst, Alice S Prince, Danielle Ahn\",\"doi\":\"10.1128/iai.00016-24\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><p>Polymyxin resistance in carbapenem-resistant <i>Klebsiella pneumoniae</i> bacteria is associated with high morbidity and mortality in vulnerable populations throughout the world. Ineffective antimicrobial activity by these last resort therapeutics can occur by transfer of <i>mcr-1</i>, a plasmid-mediated resistance gene, causing modification of the lipid A portion of lipopolysaccharide (LPS) and disruption of the interactions between polymyxins and lipid A. Whether this modification alters the innate host immune response or carries a high fitness cost in the bacteria is not well established. To investigate this, we studied infection with <i>K. pneumoniae</i> (KP) ATCC 13883 harboring either the <i>mcr-1</i> plasmid (p<i>mcr-1</i>) or the vector control (pBCSK) ATCC 13883. Bacterial fitness characteristics of <i>mcr-1</i> acquisition were evaluated. Differentiated human monocytes (THP-1s) were stimulated with KP bacterial strains or purified LPS from both parent isolates and isolates harboring <i>mcr-1</i>. Cell culture supernatants were analyzed for cytokine production. A bacterial pneumonia model in WT C57/BL6J mice was used to monitor immune cell recruitment, cytokine induction, and bacterial clearance in the bronchoalveolar lavage fluid (BALF). Isolates harboring <i>mcr-1</i> had increased colistin MIC compared to the parent isolates but did not alter bacterial fitness. Few differences in cytokines were observed with purified LPS from <i>mcr-1</i> expressing bacteria <i>in vitro</i>. However, in a mouse pneumonia model, no bacterial clearance defect was observed between p<i>mcr-1</i>-harboring KP and parent isolates. 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引用次数: 0
摘要
耐碳青霉烯类肺炎克雷伯氏菌对多粘菌素的耐药性与全世界易感人群的高发病率和高死亡率有关。质粒介导的耐药基因 mcr-1 的转移可导致脂多糖(LPS)的脂质 A 部分发生改变,并破坏多粘菌素与脂质 A 之间的相互作用,从而使这些最后的治疗药物无法发挥有效的抗菌活性。为了研究这个问题,我们研究了携带 mcr-1 质粒(pmcr-1)或载体对照(pBCSK)的肺炎克雷伯菌(KP)ATCC 13883 的感染情况。对获得 mcr-1 的细菌适存特性进行了评估。用 KP 菌株或纯化的 LPS 刺激分化的人单核细胞(THP-1s),这些菌株来自母株分离物和携带 mcr-1 的分离物。对细胞培养上清液进行细胞因子生成分析。用 WT C57/BL6J 小鼠细菌性肺炎模型监测免疫细胞招募、细胞因子诱导和支气管肺泡灌洗液(BALF)中的细菌清除情况。 与亲本分离株相比,携带 mcr-1 的分离株的可乐定 MIC 增加了,但没有改变细菌的适应性。从 mcr-1 表达细菌中提纯的 LPS 在体外观察到的细胞因子几乎没有差异。然而,在小鼠肺炎模型中,pmcr-1-harboring KP 与亲本分离物之间没有观察到细菌清除缺陷。同样,在 BALF 中也没有观察到细胞因子产生或免疫细胞招募方面的差异,这表明 LPS 中的这些脂质 A 突变所产生的影响已被其他机制所取代。
Lipid A modification of colistin-resistant Klebsiella pneumoniae does not alter innate immune response in a mouse model of pneumonia.
Polymyxin resistance in carbapenem-resistant Klebsiella pneumoniae bacteria is associated with high morbidity and mortality in vulnerable populations throughout the world. Ineffective antimicrobial activity by these last resort therapeutics can occur by transfer of mcr-1, a plasmid-mediated resistance gene, causing modification of the lipid A portion of lipopolysaccharide (LPS) and disruption of the interactions between polymyxins and lipid A. Whether this modification alters the innate host immune response or carries a high fitness cost in the bacteria is not well established. To investigate this, we studied infection with K. pneumoniae (KP) ATCC 13883 harboring either the mcr-1 plasmid (pmcr-1) or the vector control (pBCSK) ATCC 13883. Bacterial fitness characteristics of mcr-1 acquisition were evaluated. Differentiated human monocytes (THP-1s) were stimulated with KP bacterial strains or purified LPS from both parent isolates and isolates harboring mcr-1. Cell culture supernatants were analyzed for cytokine production. A bacterial pneumonia model in WT C57/BL6J mice was used to monitor immune cell recruitment, cytokine induction, and bacterial clearance in the bronchoalveolar lavage fluid (BALF). Isolates harboring mcr-1 had increased colistin MIC compared to the parent isolates but did not alter bacterial fitness. Few differences in cytokines were observed with purified LPS from mcr-1 expressing bacteria in vitro. However, in a mouse pneumonia model, no bacterial clearance defect was observed between pmcr-1-harboring KP and parent isolates. Consistently, no differences in cytokine production or immune cell recruitment in the BALF were observed, suggesting that other mechanisms outweigh the effect of these lipid A mutations in LPS.
期刊介绍:
Infection and Immunity (IAI) provides new insights into the interactions between bacterial, fungal and parasitic pathogens and their hosts. Specific areas of interest include mechanisms of molecular pathogenesis, virulence factors, cellular microbiology, experimental models of infection, host resistance or susceptibility, and the generation of innate and adaptive immune responses. IAI also welcomes studies of the microbiome relating to host-pathogen interactions.