Evaluating the Potential of Nitrofurantoin and Fosfomycin for E.coli UTIs: A Susceptibility Study

This study was designed to find the susceptibility of Nitrofurantoin and Fosfomycin among urinary isolates of Escherichia.coli.Four hundred(400)urine samples were collected for susceptibility of nitrofurantoin and fosfomycin among urinary isolates of E.coli.All indoor and outdoor patients'urinary samples yielded growth of E.coli.Mid-stream urine specimens were inoculated on blood agar and CLED agar and incubated at 35±2°C.Growth was observed,and Escherichia coli was identified by Gram staining,Catalase,Motility test and API 20E(Bio murex)as per standard procedure.Antimicrobial susceptibility testing of isolates for nitrofurantoin and fosfomycin was carried out by the modified Kirby-Bauer disc diffusion method according to CLSI guidelines ATCC 25922.E.coli was used as a quality control strain.A total of 400 samples were tested susceptibility of nitrofurantoin and fosfomycin among urinary isolates of E.coli during this period.A total of 400 samples yielded the growth of E.coli,out of which 178(44.5%)were male and 222(55.5%)were female samples.Among males,18(10%)were tolerant to nitrofurantoin,and 2(1.1%)were tolerant to fosfomycin.Among females,9(4.09%)were susceptible to nitrofurantoin while 6(2.72%)were susceptible to fosfomycin.Among age groups below 45 years old,6(4.76%)were tolerant to nitrofurantoin,and 2(1.58%)were sensitive to fosfomycin.Between 46-66 years old,4(2.81%)were sensitive to nitrofurantoin,and 3(2.11%)were sensitive to fosfomycin.Between 67-90 years old,17(12.87%)were sensitive to nitrofurantoin,and 4(3.03%)were tolerant to fosfomycin.Fosfomycin and nitrofurantoin showed good susceptibility in urinary isolates of E.coli and can be used empirically in our setup.

A practical synthesis of (-)fosfomycin from its enantiomer

（＋）-cis-（1S, 2R）-Epoxypropylphosphonic acid, the enantiomer of fosfomycin, which is the industrial side-product in the preparation of the antibiotic fosfomycin, was converted into （-）fosfomycin by a seven-step procedure. The esterification of the dihydroxyphosphonic intermediate was the key step. The title compound was obtained in good yield and its optical purity was up to the medicine quality standard of Chinese Pharmacopoeia.

Fosfomycin—A Promising Oral Antibiotic for the Treatment of Urinary Tract Infection (UTI)

Background: Among the common morbid causes that are prevalent among all age groups, urinary tract infections top the list. In our country, most of the UTI patients visiting hospitals (OPD or IPD) are already on empirical antibiotics even before getting the sensitivity report in their hand. The purpose of this research was to examine the susceptibility patterns of commonly used antibiotics, particularly fosfomycin, against common uropathogens. Methodology: This was a prospective observational study conducted between January and March 2021 in four private tertiary hospitals in Dhaka, Bangladesh. All the urine samples referred to these four laboratories, obtained from patients of all ages and both genders, clinically diagnosed to have UTI, were included. Urine culture was performed by a semiquantitative method on blood agar media and MacConkey agar media. Following identification, antimicrobial sensitivity testing was performed using the modified Kirby Bauer disk diffusion method in accordance with CLSI standards. The data was put into Statistical Package for Social Sciences (SPSS) statistical software version 25 for the analysis. Results: A total of 5389 urine samples were received from four private hospitals in Dhaka over three months, and of these, 934 (17.33%) isolates were obtained from culture. About 95% of the isolates were gram-negative bacilli (GNBs). The most common isolate was Escherichia coli 615 (65.85%), followed by Klebsiella spp. 154 (16.49%), Pseudomonas spp. 64 (6.85%) and 51 (5.46%) isolates of Enterobacter. Among the gram-positive cocci, the most common were Enterococci fecalis 18 (1.93%) and Staphylococcus aureus 17 (1.82%). Of all the antibiotics tested, fosfomycin sensitivity was 98.4%, 88.88%, and 100% for Escherichia coli, Enterococci fecalis, and Staphylococcus aureus, respectively. All the isolates tested were susceptible to Meropenem (77% - 100%), Amoxiclav (78% - 100%) and Nitrofurantoin (45% - 94%). Sensitivity amongst all the uropathogens for ceftriaxone, ciprofloxacin, and cotrimoxazole was nearly 50% - 77%. Conclusion: The positivity of urinary isolates is 17.33%, with the most common pathogen being Escherichia coli. Common uropathogens show the highest in vitro susceptibility to fosfomycin. So, fosfomycin should be considered as a highly potent and promising alternative oral antibiotic treatment for UTI.

Capillary Electrophoresis in the Presence of Fosfomycin

Fosfomycin, a sodium salt ofcis-(3-methyloxiranyl) phosphonic acid, was used as electrolyte in binary methanol-water media for capillary electrophoresis. The variety of electroosmotic flow with pH*, methanol concentration and ionic strength was investigated. The migration behavior of nine bases was examined under various conditions, and the separation of thymine, cytosine, 5-flurouracil, 4, 6-diamino-pyrimidine, purine was accomplished.

Fosfomycin Resistance in Avian Pathogenic Escherichia coli Isolates

Fosfomycin, a broad-spectrum antibiotic against both Gram-positive and Gram-negative bacteria, is very important in the clinic but many fosfomycin-resistant bacteria have been isolated from patients. In this study, the resistance mechanism of three fosfomycin-resistant avian pathogenic Escherichia coli （APEC） strains （JE1, IF7 and CD11） isolated from septicemic chickens were analyzed. The results showed that their fosfomycin-resistance mechanisms were different. An alteration in the glpT transport system was the main reason of the fosfomycin-resistance mechanisms of strain IF7. Compared with the control stain BL21, the capacity of fosfomycin-uptake was low in all these three stains （JE 1 〉IFT〉CD 11）. Sequence results of murA showed that there were more than 10 sites of nucleotide mutation, but only one amino acid mutation T116A showed in CD11. Real-time detection test showed that the expression level of the murA gene of the three stains was significantly increased （four times increase in strain CD11 and two times increase in strains JE1 and IFT）. The transformation and recombinant test showed that the recombinant bacteria with the murA of JE1 and CD11 showed high minimal inhibitory concentration （MIC） against fosfomycin. From the results of this research, it showed that most of the fosfomycin- resistance mechanisms once showed in patient bacteria have appeared in the APEC strains and the fosfomycin-resistance mechanism of the three APEC isolates was different.

Fosfomycin Therapy for Non-Complicated Lower Urinary Tract Infections during Pregnancy: Tanta University Experience

Objectives: To evaluate the efficacy, compliance, safety and economic cost for Fosfomycin trometamol and Nitofurantoin in uncomplicated lower urinary tract infections during pregnancy. Background: Nitofurantoin and Fosfomycin trometamol are recommended as the first-line agents for treatment of urinary tract infections (UTIs) in the latest guidelines endorsed by the Infectious Diseases Society of America (IDSA) and the European Society for Clinical Microbiology and Infectious Diseases (ESCMID). Fosfomycin is bactericidal and inhibits bacterial cell wall biogenesis and reduces bacterial adherence to uroepithelial cells. Fosfomycin has broad antibacterial activity against both Gram-positive and Gram-negative pathogens, as Escherichia coli, Escherichia faecalis, and various Gram-negatives like Citrobacter and Proteus. Both Nitofurantoin and Fosfomycin are category B in pregnancy. Patients and Methods: This study was conducted at Tanta University Hospitals in the period from June, 1, 2015 to January, 1, 2017. Patients were recruited from outpatient clinics of Obstetrics and Gynecology and Urology Departments presenting with asymptomatic bacteruria or cystitis. Patients were allocated randomly into 2 groups: group I (n = 50 cases) received Fosfomycin therapy and group II (n = 50 cases) received Nitofurantoin therapy (n = 50 cases). After treatment, evaluation of patient symptoms, organism count, patient compliance and cost of treatment were done. Results: The enrolled patients were suffering from lower urinary tract infections;asymptomatic bacteruria (17 cases) or cystitis (83 cases). Ten patients were excluded. The demographic data of included patients were not significant for both groups. Complete relief (100%) of symptoms 5 days after start of treatment was noticed in Fosfomycin group while improvement of symptoms after 5 day-treatment was noticed in 86.49% in Nitofurantoin group (p-value = 0.030). The side effects were recorded in 7 cases (18.42%) in Fosfomycin group compared to (35.14%) with significant difference in the reported side effects, (p-value = 0.003). Compliance was 38/38 (100%) in Fosfomycin group compared to 34/37 (91.89%) in Nitrofuantoin group (p-value = 0.001). Resistance was very minimal in Fosfomycin group where 1/38 case (2.63%) reported resistance for treatment compared to 8/37 cases (21.62%) in Nitofurantoin group (p-value = 0.001). Conclusion: Fosfomycin trometamine proved to be safe, effective, and has limited resistance. Moreover higher patient compliance and fewer side effects were recommending Fosfomycin to be a first choice drug for uncomplicated lower urinary tract infections during pregnancy at Tanta University.

The progress in study of fosfomycin

In recent years, heavy drug resistance in bacteria has become increasingly serious, and the progress of research and development of new antibiotics are slow. Therefore, seeking an alternative from the safe and effective "old medicine" is a strategy for clinical action against infection. Among them, fosfomycin is extremely relevant. Based on the related literature at home and abroad, this review briefly introduces fosfomycin in the context of progress in synthetic methods, pharmacokinetic and pharmacodynamic characteristics, and antibacterial activities, to provide references for clinical rational use.

Activity of Fosfomycin in Extended-Spectrum Beta-Lactamases Producing Klebsiella pneumonae from Hospital Acquired Urinary Tract Infections

Treatment of hospital acquired urinary tract infections (UTIs) caused by extended-spectrum beta-Lactamases producing Klebsiella pneumonae is a major problem. This organism expresses a high level of resistance to many groups of antibiotics. Fosfomycin is an agent which is recommended for treatment of UTIs caused by ESBLs producers. The aim of this study is to determine the sensitivity pattern of ESBLs producing urinary K. pneumonae to antimicrobial agents including fosfomycin in patients of MUHs and determine the prevalence of fosfomycin resistance mediated by plasmid mediated fosfomycin modifying enzymes fosA, fosB and fosA3. Methods: Klebsiella pneumonae urinary isolates were collected from patients with hospital acquired UTIs in Mansoura University Hospitals (MUHs). The susceptibility pattern was determined by Kirby Baur method. Isolates resistant to extended spectrum cephalosporins were tested for ESBLs production by double disc diffusion method. Fosfomycin resistance was determined by broth dilution method. Isolates resistant to fosfomycin were tested for fosA, fosB and fosA3 by PCR. Results: A total of 128 ESBLs producing K. pneumonae isolates were collected. The highest sensitivity was to imipenem (94.5%). The lowest was to trimethoprime-sulphamethoxazole (21.8%). Co-resistance of ESBLs isolates with fosfomycin was 23.2%. Eighteen fosfomycin resistant isolates (18/30) were positive to fosA. Conclusion: ESBLs producing urinary Klebsiella pneumonae express moderate sensitivity to fosfomycin. Resistance is mainly mediated by plasmid mediated fosfomycin modifying enzymes fosA.

Enhancement of CREC sensitivity to fosfomycin by baicalein through increasing outer membrane permeability

Background:To confirm whether baicalein improves the sensitivity of carbapenem-resistant Escherichia coli(CREC)to fosfomycin by increasing the permeability of bacterial outer membrane in vitro experiments.Methods:The clinically isolated CREC strains were amplified and then divided into three groups including baicalein monotherapy groups,fosfomycin monotherapy groups,and baicalein plus fosfomycin groups,and their minimum inhibitory concentrations(MICs)measurement and interpretation were performed according to CLSI interpretive criteria.To determine bacterial permeability after contact with baicalein,CREC were incubated with fluorescein isothiocyanate(FITC)after pretreatment with blank control without baicalein,with 0.25 MIC of baicalein,and with 0.125 MIC of baicalein,followed by observation of the intrabacterial fluorescence intensity of FITC.In addition,CREC were pretreated with 0.125 MIC of baicalein and with blank control without baicalein followed by measurement of alkaline phosphatase(AKP)leak to determine the change of bacterial permeability.Results:The MIC range in baicalein monotherapy groups was from 128 mg/L to 256 mg/L,and the MIC range in fosfomycin monotherapy groups was from 16 mg/L to 1,024 mg/L,but the MIC range in both combination therapy groups was reduced to 4 mg/L to 64 mg/L.The combination use reduced the MIC of each therapy by 75%-96.88%in all strains,and the fractional inhibitory concentration index(FICI)values less than or equal to 0.5.In the permeability assay,no permeabilization of FITC was observed in the blank groups without baicalein,but the intrabacterial FITC aggregation was observed in the groups of pretreatment with 0.25 MIC of baicalein or 0.25 MIC of baicalein.In the AKP leak assay,the AKP leak was more severe at the groups of coincubation with 0.25 MIC of baicalein than those blank groups without baicalein within the first 6 hours.Conclusion:Our study suggests that baicalein may synergistically enhance the antibacterial effect of fosfomycin by increasing the permeability of CREC outer membrane.

含磷霉素的联合抗菌方案治疗耐碳青霉烯革兰阴性杆菌感染疗效:系统评价与荟萃分析

目的评价含磷霉素联合治疗碳青霉烯耐药革兰阴性菌(carbapenem-resistant Gram-negative organism,CRO)感染的疗效。探讨含磷霉素联合治疗CRO感染的最佳方案。方法系统检索中国知网、PubMed、Embase、Web of Science、Cochrane Library数据库,收集建库至2023年7月6日公开发表的关于磷霉素治疗CRO感染的相关文献,按照纳入排除标准进行筛选,使用RevMan5.4.1软件进行荟萃分析。主要结局指标包括临床死亡率。使用R软件对含磷霉素的联合治疗方案进行网状Meta分析。使用Cochrane偏差风险评估工具和Newcastle-Ottawa scale量表评估文献质量。本研究已在PROSPERO注册,CRD42022344659。结果最初检索到11806篇文献,其中有16篇、6篇分别纳入死亡率的Meta分析和网状Meta分析。含磷霉素的联合抗菌治疗方案和其他方案治疗CRO感染的总死亡率分别为25%(76/304)和42.63%(350/821),差异有统计学意义[优势比(odds ratio,OR)=0.44;95%CI=0.32-0.62P<0.0001,I^(2)=48%]。在亚组分析中,含磷霉素的联合抗菌治疗方案和其他方案治疗耐碳青霉烯肠杆菌科细菌(carbapenem-resistant Enterobacteriaceae,CRE)感染的总死亡率分别为22.06%(45/204)和35.96%(228/634),差异有统计学意义(OR=0.62,95%CI=0.41~0.95,P=0.03<0.05,I^(2)=0%)。含磷霉素的联合抗菌治疗方案和其他方案治疗耐碳青霉烯鲍曼不动杆菌(carbapenem-resistant Acinetobacter baumannii,CRAB)感染的总死亡率分别为31.87%(29/91)和66.12%(121/183),差异无统计学意义(OR=0.24,95%CI=0.03~1.76,P=0.16>0.05,I^(2)=91%)。在网络荟萃分析中,多利培南+磷霉素治疗CRO感染的死亡率最低。结论含磷霉素的联合治疗方案可显著降低CRO感染患者的死亡率。此外,多利培南加磷霉素可能是最佳的组合方案。

磷霉素联合亚胺培南对携带blaNDM的耐碳青霉烯类肠杆菌目细菌的体外抗菌活性

目的探究磷霉素与亚胺培南联合使用对携带blaND00M的耐碳青霉烯类肠杆菌目细菌(carbapenem-resistant Enterobacterales,CRE)的体外抗菌活性。方法收集2021—2022年苏州大学附属第二医院医学检验中心临床分离的非重复CRE,并通过聚合酶链式反应(polymerase chain reaction,PCR)筛选出携带bla_(NDM)的耐碳青霉烯类肺炎克雷伯菌(carbapenem-resistant Klebsiella pneumoniae,CR-KP)和耐碳青霉烯类大肠埃希菌(carbapenem-resistant Escherichia coli,CR-E.coli)。通过微量肉汤稀释法测定菌株对常用抗生素的最低抑菌浓度(minimum inhibitory concentration,MIC)和琼脂稀释法测定菌株对磷霉素的MIC;采用棋盘法分别测定磷霉素与6种抗生素联用的部分抑菌浓度指数(fractional inhibitory concentration index,FICI)以判定药物联合效果;通过时间杀菌实验判断磷霉素与亚胺培南体外联合杀菌效果;采用结晶紫染色法检测菌株生物膜形成能力;通过荧光定量PCR检测不同抗生素条件下菌株bla_(NDM)、fosA、mrkA和murA基因的转录水平。结果PCR筛选出24株携带bla_(NDM)基因的CR-KP(12/24)和CR-E.coli(12/24)。棋盘试验显示磷霉素联合亚胺培南的协同作用(FICI≤0.5)相较其他抗生素效果最好(70.8%)。时间杀菌实验显示,磷霉素联合亚胺培南作用24 h内细菌数降低≥3 log_(10)CFU/mL,呈现出较强的杀菌效应。结晶紫染色结果显示磷霉素与亚胺培南联合可以抑制细菌生物膜形成。荧光定量PCR结果显示,磷霉素与亚胺培南联合处理后,生物膜形成与Ⅲ型菌毛合成重要基因mrkA表达相较对照组和亚胺培南组显著下调,而细胞壁形成重要基因murA表达相较其他两组上调。结论磷霉素与亚胺培南联用可以抑制细菌生长,其可能通过减少生物膜形成、影响菌毛和细胞壁形成等方面对携带bla_(NDM)的CR-KP与CR-E.coli发挥协同抗菌或杀菌作用。

Effect of fosfomycin,Cynara scolymus extract,deoxynivalenol and their combinations on intestinal health of weaned piglets

Weaning is a challenging stage of pig farming.Animals undergo environmental,social and dietary changes leading to weaning stress syndrome.In order to compensate for the detrimental effects of weaning stress,antibiotics and natural extracts are used as feed additives,sometimes without fully understanding the interactions between them or even with low concentrations of mycotoxins that are frequently present in feed.The aim of this study was to evaluate the effect of fosfomycin(FOS),Cynara scolymus extract(CSE),deoxynivalenol(DON) and their combined administration on intestinal health of weaned piglets.The experiment was designed as a 2×2×2 factorial arrangement with 3 factors(FOS,CSE and DON treatments),2 levels each(presence and absence) and 3 repeats.Weaned piglets(n=24)were randomly divided in groups to receive the different treatments,namely DON administered in diet(50 μg/kg BW),FOS administered into the drinking water(30 mg/kg BW),CSE administered in diet(15 mg/kg BW) and all their combinations.After 15 d,the animals were euthanized and gastrointestinal tract samples were immediately taken to evaluate gastrointestinal pH,Enterobacteriaceae to lactic acid bacteria(E:L) ratio,volatile fatty acid(VFA) concentrations,disaccharidase(lactase,sucrase and maltase)activity,histology(intestinal absorptive area [IAA] and goblet cells count) and mucus ability to adhere pathogenic Escherichia coli.From our results,FOS and CSE treatments,individually or combined,produced a lower E:L ratio,an enhanced production of butyrate,increased disaccharidase activity(particularly maltase),and a greater IAA and goblet cells count along with an increase in pathogenic bacteria adherence to intestinal mucus.Deoxynivalenol did not show interactions with the other factors and its administration produced decreases on VFA,disaccharidase activity and goblet cells count.In conclusion,weaning piglets receiving diets containing FOS,CSE or both exhibited evident beneficial intestinal effects compared to animals receiving diets free from these compounds.On the contrary,the presence of DON at sub-toxic concentrations produced detrimental effects on intestinal health.The knowledge of the physiological and pathological gut changes produced by these compounds contributes to understand their potential productive consequences.

完带汤加减结合磷霉素钙颗粒治疗小儿外阴阴道炎(脾虚湿困证)临床观察

目的探讨完带汤加减结合磷霉素钙颗粒治疗小儿外阴阴道炎(脾虚湿困证)的临床疗效。方法选择2021年6月—2022年4月在保定市中医院接受治疗的72例小儿外阴阴道炎患者,采用随机数表法分为试验组和对照组,各36例。对照组给磷霉素钙颗粒口服治疗,试验组给予完带汤加减结合磷霉素钙颗粒口服治疗。比较两组临床疗效、白细胞介素2(interleukin-2,IL-2)、肿瘤坏死因子-α(tumor necrosis factor-α,TNF-α)、白细胞介素13(interleukin-13,IL-13)、中医症状积分、临床症状缓解情况及并发症发生情况。结果治疗后,两组总有效率比较,差异有统计学意义(P<0.05);治疗后,两组IL-2、TNF-α、IL-13水平均降低,试验组降低更为明显(P<0.05);治疗后,两组阴道灼热感、外阴瘙痒、头晕及口干尿赤评分水平均降低,试验组降低更为明显(P<0.05);治疗后,试验组外阴瘙痒、外阴疼痛及白带异常改善时间均显著低于对照组(P<0.05);治疗期间不良反应主要有恶心呕吐、头晕、头痛,两组发生率比较,差异无统计学意义(P>0.05)。结论在小儿外阴阴道炎中完带汤加减结合磷霉素钙颗粒治疗有较好的效果,可有效改善患者炎症水平。

UV/H_(2)O_(2)和UV/PDS体系对磷霉素降解效果的对比

紫外高级氧化技术降解有机污染物,由于操作简单、成本低、不易产生二次污染等优点被广泛应用。文章以磷霉素钠作为污染物,研究了UV/H_(2)O_(2)和UV/过硫酸盐(PDS)两种高级氧化技术对有机磷的降解特性,并对比了两种体系下有机磷的降解动力学和反应机理。试验结果表明,在UV/H_(2)O_(2)和UV/PDS体系中,UV激活氧化剂产生的活性基团可有效降解有机磷,有机磷降解率分别为97.3%和95.0%,初始pH、氧化剂投加量、反应温度均会对有机磷降解产生影响,相比于UV/H_(2)O_(2)体系,UV/PDS体系在降解有机磷时,具有pH适用范围较宽、反应温度低、氧化剂投加量小、反应速率快的优势。在最优条件下,两种体系都具有环境适应性。通过自由基捕获试验与电子顺磁共振技术(EPR)可知,UV/H_(2)O_(2)体系中存在·OH,UV/PDS体系中存在SO_(4)^(·-)和·OH。通过气-质联用(CG/MS)技术,测得两种体系降解磷霉素钠后均含有乙酸和丙酸。

UhpT^(E350Q)突变与fosA6/5的出现有可能是肺炎克雷伯菌磷霉素耐药的内在机制

目的分析肺炎克雷伯菌磷霉素耐药基因的分布,探讨磷霉素老药新用在该菌的限制机制。方法使用二代测序技术对14株临床高毒性/高粘性肺炎克雷伯菌分离株(HvKP/HmKP)测序绘制基因组草图,基于综合抗生素耐药性数据库CARD中的同源性和SNP模型,通过抗性基因识别软件分析预测磷霉素耐药相关基因uhpT、fosA及其突变;并对GenBank中获得的521条肺炎克雷伯菌全基因组序列进行同步分析验证。结果本研究中14株HvKP/HmKP临床分离株均具有己糖磷酸盐转运蛋白基因(UhpT)突变,其在350aa处谷氨酸突变为谷氨酰胺(UhpT^(E350Q))。12株菌(12/14,85.71%)基因组携带fosA6基因,其余2株菌(14.29%)中携带fosA5基因。GenBank的521株肺炎克雷伯菌基因组序列中,携带UhpT^(E350Q)突变的菌株508株(97.50%),携带fosA6基因的菌株439株(84.26%),携带fosA5基因的菌株80株(15.36%);同时携带UhpT^(E350Q)突变和fosA6/5基因的菌株507株(97.31%);无UhpT^(E350Q)突变、仅fosA6/5基因的菌株12株(2.30%);仅携带UhpT^(E350Q)突变、无fosA6/5基因的菌株1株(0.19%);无UhpT^(E350Q)突变、无fosA6/5基因的菌株1株(0.19%)。结论染色体UhpT^(E350Q)突变与fosA6/5基因在肺炎克雷伯菌染色体中的普遍存在意味着出现转运蛋白突变和产生磷霉素修饰酶,这可能是该菌对磷霉素天然耐药的内在机制,会限制磷霉素在肺炎克雷伯菌,特别是多重耐药的HvKP/HmKP相关抗感染中的临床应用。

磷霉素对万古霉素致肾损伤模型大鼠Keap1-Nrf2/ARE通路的影响

目的探讨磷霉素对万古霉素致肾损伤模型大鼠的保护作用及其机制。方法SD大鼠60只,随机分为模型对照组、正常对照组、磷霉素组和万古霉素联合磷霉素小、中、大剂量组(联合-L、联合-M、联合-H组),每组10只。正常对照组给予等剂量0.9%氯化钠注射液,模型对照组给予万古霉素0.2 g·kg^(-1),磷霉素组给予磷霉素0.25 g·kg^(-1),联合-L组、联合-M组、联合-H组分别给予磷霉素0.125,0.25,0.5 g·kg^(-1),30 min后再给予万古霉素0.2 g·kg^(-1),均腹腔注射,连续21 d。酶联免疫吸附实验(ELISA)测定大鼠尿N-乙酰-β-D-氨基葡萄糖苷酶(NAG)、肾损伤因子1(KIM-1)含量,考马斯亮蓝法测定24 h尿蛋白,反转录-聚合酶链反应(RT-PCR)检测肾组织Kelch样环氧氯丙烷相关蛋白-1(Keap1)、核因子E2相关因子(Nrf2)、抗氧化反应元件(ARE)信号通路Nrf2、Keap1及下游靶蛋白谷胱甘肽过氧化物酶-1(GPX-1)mRNA表达。结果与正常对照组比较,模型对照组24 h尿蛋白、NAG、KIM-1水平显著升高(P<0.05),肾组织Nrf2 mRNA表达升高(P<0.01),Keap1几乎无变化,GPX-1 mRNA表达下降(P<0.01);联合-L组、联合-M组Nrf2、Keap1 mRNA表达明显升高(P<0.01),联合给药组GPX-1 mRNA表达均显著升高(P<0.01)。与模型对照组比较,联合-M组、联合-H组24 h尿蛋白、NAG、KIM-1水平显著下降(P<0.01),且与磷霉素呈剂量依赖性。结论万古霉素可通过影响肾组织Nrf2表达引起肾损伤。磷霉素可能通过激活机体抵抗外界氧化刺激的防御性转导Keap1-Nrf2/ARE信号通路改善万古霉素引起的肾损伤。

磷霉素联合多黏菌素B对碳青霉烯类耐药肠杆菌目细菌的体外抗菌活性分析

目的分析磷霉素联合多黏菌素B对碳青霉烯类耐药肠杆菌目细菌(carbapenem-resistant Enterobacterales,CRE)的体外抗菌活性。方法收集2020~2022年西安交通大学第二附属医院分离的CRE 78株,其中碳青霉烯类耐药大肠埃希菌(carbapenem-resistant Escherichia coli,CREC)32株、碳青霉烯类耐药肺炎克雷伯菌(carbapenem-resistant Klebsiella pneumonia,CRKP)46株;碳青霉烯类敏感肠杆菌目细菌(carbapenem-sensitive Enterobacterales,CSE)132株,其中碳青霉烯类敏感大肠埃希菌(carbapenem-sensitive Escherichia coli,CSEC)72株、碳青霉烯类敏感肺炎克雷伯菌(carbapenem-sensitive Klebsiella pneumonia,CSKP)60株。采用琼脂稀释法和肉汤微量稀释法(broth microdilution,BMD)分别测定磷霉素和多黏菌素B的最低抑菌浓度(minimum inhibitory concentration,MIC),采用肉汤微量稀释棋盘法测定CRE对磷霉素联合多黏菌素B的最低抑菌浓度,并计算部分抑菌浓度指数(fractional inhibitory concentration index,FIC),判定其联合效应。结果78株CRE中28株对磷霉素耐药,总耐药率为35.90%(28/78),其中6株同时还对多黏菌素B耐药,总耐药率为7.69%(6/78)。132株CSE中18株仅对磷霉素耐药,总耐药率为13.64%(18/132);未检测到对多黏菌素B耐药。多黏菌素B联合磷霉素对CREC为相加作用,对CRKP为协同作用。结论磷霉素和多黏菌素B单药耐药率均明显升高,二者联合用药可有效降低耐药率,提供一种新的治疗思路。

亚胺培南联合磷霉素对多重耐药鲍曼不动杆菌的试验研究

目的探索以亚胺培南为基础用药,对临床分离多重耐药鲍曼不动杆菌(MDR-AB)的体内外抗菌方法。方法用微量肉汤稀释法及棋盘法测定7株临床分离的MDR-AB对亚胺培南、磷霉素、阿米卡星、替加环素、多粘菌素B 5种抗菌药物的最低抑菌浓度(MIC)及联合MIC,并计算部分抑菌浓度指数(FICI)。用时间杀菌曲线法判断亚胺培南联合磷霉素的杀菌效果。选取菌株AB6624、AB0153构建体外生物膜模型,结晶紫染色法半定量生物膜。激光共聚焦显微镜观察使用亚胺培南联合磷霉素对生物膜细菌的杀伤作用。流式细胞仪检测亚胺培南及磷霉素单药与联合用药对细菌活性氧(ROS)表达的影响。建立大蜡螟感染模型,记录亚胺培南及磷霉素单药与联合用药时大蜡螟存活率。结果亚胺培南联合磷霉素对5株MDR-AB具有协同作用;亚胺培南联合磷霉素对菌株AB6624、AB0153分别在4、8 h的菌落数较单药组降低>2log 10 CFU/mL;亚胺培南联合磷霉素抑制菌株生物膜形成并对菌株AB0153生物膜结构具有破坏作用;亚胺培南联合磷霉素可以提高菌株AB0153胞内ROS水平,差异具有统计学意义(P<0.05);与对照组相比,亚胺培南联合磷霉素处理组大蜡螟生存率提高(中位生存时间96 h),差异具有统计学意义(P=0.022)。结论亚胺培南联合磷霉素对MDR-AB具有协同作用,并可能通过抑制生物膜形成及提高细菌胞内ROS水平发挥作用。

磷霉素氨基葡萄糖盐β-CD包合物的制备与研究

目的 制备磷霉素氨基葡萄糖盐(FA)-β-环糊精(β-CD)包合物,解决磷霉素氨基葡萄糖盐高温不稳定、引湿性强的问题。方法 采用冷冻干燥法制备FA-β-CD包合物,以包合率和收率为评价指标,单因素考察投料质量比、包合时间、包合温度对包合效果的影响;通过红外光谱分析、X-射线衍射法对FA-β-CD包合物进行鉴定;对FA、FA-β-CD包合物以及β-CD进行抗菌活性测试;对FA和FA-β-CD包合物及其溶液在不同温度下进行稳定性考察。结果冷冻干燥法制备FA-β-CD包合物的最佳工艺为m(β-CD)∶m(FA)=1.25∶1,包合时间为2h,包合温度为20℃;抗菌活性测试和稳定性考察结果均表明β-CD能够较好的保护FA。结论冷冻干燥法可以成功制备FA-β-CD包合物,并能提高FA的稳定性。

磷霉素氨丁三醇散联合止痛化症胶囊治疗慢性盆腔炎的临床疗效研究

目的了解磷霉素氨丁三醇散联合止痛化症胶囊治疗慢性盆腔炎的临床疗效。方法采用随机数字表法将我院收治的84例慢性盆腔炎患者分为治疗组与对照组各42例。对照组给予止痛化症胶囊口服,3粒/次,3次/d,连用15 d;治疗组在对照组的基础上给予磷霉素氨丁三醇散,3 g/d,连用7 d。治疗结束后对两组患者的疗效进行评价比较。结果 (1)治疗组治疗前、后的症状积分分别为(19.05±3.04)分、(4.29±1.21)分,对照组分别为(18.96±3.87)分、(8.52±3.47)分,治疗前差异无统计学意义(P>0.05),治疗后差异有统计学意义(P<0.05)。(2)治疗组治疗后痊愈、显效、有效、无效分别为10例(23.8%)、16例(38.1%)、12例(28.6%)、4例(9.5%),对照组分别为6例(14.3%)、12例(28.6%)、14例(33.3%)、10例(23.8%),两组比较差异有统计学意义(P<0.05)。两组患者均未发生严重不良反应。结论磷霉素氨丁三醇散联合止痛化症胶囊治疗慢性盆腔炎的疗效优于单用止痛化症胶囊,疗效确切显著,不良反应少。