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首页> 外文期刊>Respiratory Research >Ablation of SP-A has a negative impact on the susceptibility of mice to Klebsiella pneumoniae infection after ozone exposure: sex differences
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Ablation of SP-A has a negative impact on the susceptibility of mice to Klebsiella pneumoniae infection after ozone exposure: sex differences

机译:SP-A的消融对臭氧暴露后小鼠对肺炎克雷伯菌的敏感性具有负面影响:性别差异

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BackgroundSurfactant protein A (SP-A) enhances phagocytosis of bacteria, including Klebsiella pneumoniae, by alveolar macrophages. Ozone, a major air pollutant, can cause oxidation of surfactant and may influence lung immune function. Immune function may also be affected by sex-specific mechanisms. We hypothesized that ablation of SP-A has a negative impact on the susceptibility of mice to Klebsiella pneumoniae infection after ozone exposure, and that sex differences in the effect of ozone do exist.MethodsMale and female SP-A (-/-) mice on the C57BL/6J background were exposed to ozone or to filtered air (FA) used as a control and then infected intratracheally with K. pneumoniae bacteria. Survival rate was monitored during a 14-day period. In addition, protein oxidation levels and in vivo phagocytosis were checked 1 h after inoculation of PBS used as a sham control and after inoculation of K. pneumoniae bacteria in PBS, respectively.ResultsWe found: 1) ozone exposure followed by K. pneumoniae infection decreases survival and alveolar macrophage phagocytic function of SP-A (-/-) mice compared to filtered air exposure (p < 0.05), and females are more affected than males; 2) SP-A (-/-) mice (exposed either to ozone or FA) are more susceptible to infection with K. pneumoniae than wild type (WT) mice regarding their survival rate and macrophage phagocytic function; the phagocytic function of FA SP-A(-/-) is similar to that of ozone exposed WT. 3) ozone exposure appears to increase infiltration of PMNs, total protein, and SP-A oxidation in WT mice; infiltration of PMNs and total protein oxidation appears to be more pronounced in female mice in response to ozone; 4) ozone exposure increases SP-A oxidation in WT females significantly more than in males.ConclusionAbsence (i.e. ablation of SP-A in SP-A (-/-) mice) or reduction of functional activity of SP-A (i.e. oxidation of SP-A in WT mice) increases the susceptibility of mice to experimental pneumonia after ozone exposure, and in both cases females are more affected by ozone exposure than males.
机译:背景技术表面活性剂蛋白A(SP-A)通过肺泡巨噬细胞增强细菌(包括肺炎克雷伯菌)的吞噬作用。臭氧是主要的空气污染物,会导致表面活性剂氧化并影响肺部免疫功能。免疫功能也可能受到性别特异性机制的影响。我们假设SP-A的消融对暴露于臭氧的小鼠对肺炎克雷伯菌的敏感性有负面影响,并且确实存在臭氧作用的性别差异。将C57BL / 6J背景暴露于臭氧或用作对照的过滤空气(FA)中,然后气管内感染肺炎克雷伯菌。在14天内监测生存率。此外,分别在作为假对照的PBS接种后1 h和在PBS中接种肺炎克雷伯菌后,分别检查了蛋白质的氧化水平和体内吞噬作用。结果我们发现:1)臭氧暴露继之以肺炎克雷伯菌感染减少与过滤空气接触相比,SP-A(-/-)小鼠的存活率和肺泡巨噬细胞吞噬功能(p <0.05),雌性比雄性受影响更大; 2)就存活率和巨噬细胞吞噬功能而言,SP-A(-/-)小鼠(暴露于臭氧或FA中)比野生型(WT)小鼠更易感染肺炎克雷伯菌。 FA SP-A(-/-)的吞噬功能类似于暴露于臭氧的WT。 3)臭氧暴露似乎增加了WT小鼠中PMN,总蛋白和SP-A氧化的渗透;在对臭氧的反应中,雌性小鼠中PMN的渗透和总蛋白氧化似乎更为明显。 4)臭氧暴露对野生雌性小鼠的SP-A氧化作用明显大于雄性。结论缺失(即SP-A(-/-)小鼠的SP-A消融)或SP-A的功能活性降低(即SP-A的氧化) WT小鼠中的SP-A会增加小鼠在暴露于臭氧后对实验性肺炎的敏感性,在两种情况下,雌性都比雄性更易受到臭氧的影响。

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