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首页> 外文期刊>BMC Infectious Diseases >Combined therapy with ceftriaxone and doxycycline does not improve the outcome of meningococcal meningitis in mice compared to ceftriaxone monotherapy
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Combined therapy with ceftriaxone and doxycycline does not improve the outcome of meningococcal meningitis in mice compared to ceftriaxone monotherapy

机译:与头孢曲松和强霉素的联合治疗没有改善小鼠脑膜炎球菌脑膜炎的结果与头孢曲松单药治疗相比

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Meningococcal meningitis (MM) is a life-threatening disease associated with approximately 10% case fatality rates and neurological sequelae in 10–20% of the cases. Recently, we have shown that the matrix metalloproteinase (MMP) inhibitor BB-94 reduced brain injury in a mouse model of MM. The present study aimed to assess whether doxycycline (DOX), a tetracycline that showed a neuroprotective effect as adjuvant therapy in experimental pneumococcal meningitis (PM), would also exert a beneficial effect when given as adjunctive therapy to ceftriaxone (CRO) in experimental MM. BALB/c mice were infected by the intracisternal route with a group C Neisseria meningitidis strain. Eighteen h post infection (hpi), animals were randomised for treatment with CRO [100?mg/kg?subcutaneously (s.c.)], CRO plus DOX (30?mg/kg?s.c.) or saline (control?s.c.). Antibiotic treatment was repeated 24 and 40 hpi. Mouse survival and clinical signs, bacterial counts in cerebella, brain damage, MMP-9 and cyto/chemokine levels were assessed 48 hpi. Analysis of bacterial load in cerebella indicated that CRO and CRO?+?DOX were equally effective at controlling meningococcal replication. No differences in survival were observed between mice treated with CRO (94.4%) or CRO?+?DOX (95.5%), (p??0.05). Treatment with CRO?+?DOX significantly diminished both the number of cerebral hemorrhages (p?=?0.029) and the amount of MMP-9 in the brain (p?=?0.046) compared to untreated controls, but not to CRO-treated animals (p??0.05). Levels of inflammatory markers in the brain of mice that received CRO or CRO?+?DOX were not significantly different (p??0.05). Overall, there were no significant differences in the parameters assessed between the groups treated with CRO alone or CRO?+?DOX. Treatment with CRO?+?DOX showed similar bactericidal activity to CRO in vivo, suggesting no antagonist effect of DOX on CRO. Combined therapy significantly improved mouse survival and disease severity compared to untreated animals, but addition of DOX to CRO did not offer significant benefits over CRO monotherapy. In contrast to experimental PM, DOX has no adjunctive activity in experimental MM.
机译:脑膜炎球菌脑膜炎(mm)是一种危及生命的疾病,其患者有关的危及疾病,病例患者的10-20%的病例患者和神经系统后遗症相关。最近,我们已经表明,基质金属蛋白酶(MMP)抑制剂BB-94降低了MM的小鼠模型中的脑损伤。本研究旨在评估豆蔻素(DOX),一种四环素,所述四环素在实验性肺炎脑膜炎(PM)中显示出神经保护作用的辅助治疗,当作为实验MM的辅助治疗(CRO)作为辅助治疗时,也会发挥有益效果。 Balb / C小鼠被脑内途径感染了C neisseria Meningitidis菌株。感染后十八h后(HPI),动物随机用CRO [100〜Mg / kg吗?皮下(S.C.)],CRO加入(30?Mg / kgαs.C。)或盐水(对照?S.C。)。抗生素治疗重复24和40 HPI。小鼠存活和临床症状,在48 HPI中评估了脑损伤,脑损伤,MMP-9和CYTO /趋化因子水平的细菌计数。小脑细菌载荷分析表明CRO和CRO?+?DOX同样有效地控制脑膜炎球菌复制。在用CRO(94.4%)或CRO + + + +(95.5%)处理的小鼠之间没有在小鼠之间观察到存活差异(p?> 0.05)。用CROα+ +?DOX显着降低了脑出血(P?= 0.029)的数量和大脑中的MMP-9量(P?= 0.046),而不是未处理的对照,但不适用于CRO治疗动物(p?> 0.05)。接受CRO或CRO的小鼠脑中炎症标志物的水平α+?DOX没有显着差异(p?> 0.05)。总体而言,在单独使用CRO或CRO的基团之间评估的参数没有显着差异或CRO?+?DOX。用CRO治疗+ +?DOX在体内向CRO的杀菌活性显示出类似的杀菌活性,表明DOX对CRO的拮抗作用。与未经处理的动物相比,组合治疗显着提高了小鼠生存和疾病严重程度,但对CRO的加入DOX没有提供对CRO单药治疗的显着益处。与实验PM相比,DOX在实验MM中没有辅助活性。

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