首页> 美国卫生研究院文献>Antioxidants >Flunixin Meglumine Reduces Milk Isoprostane Concentrations in Holstein Dairy Cattle Suffering from Acute Coliform Mastitis
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Flunixin Meglumine Reduces Milk Isoprostane Concentrations in Holstein Dairy Cattle Suffering from Acute Coliform Mastitis

机译:Flunixin Meglumine减少荷斯坦乳制品牛奶异前甲酸浓度患有急性大肠菌症的牛奶牛奶

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摘要

Dysfunctional inflammation contributes significantly to the pathogenesis of coliform mastitis and the classical pro-inflammatory enzyme cyclooxygenase-2 (COX-2) is the target of medical intervention using the non-steroidal anti-inflammatory drug (NSAID) flunixin meglumine (FM). Inhibition of COX-2 by FM can decrease concentrations of pro-inflammatory fatty acid-based mediators called eicosanoids, providing antipyretic and analgesic effects in dairy cows suffering from coliform mastitis. However, approximately 50% of naturally occurring coliform mastitis with systemic involvement results in death of the animal, even with NSAID treatment. Inadequate antioxidant potential (AOP) to neutralize reactive oxygen species (ROS) produced during excessive inflammation allows for oxidative stress (OS), contributing to tissue damage during coliform mastitis. Biomarkers of lipid peroxidation by ROS, called isoprostanes (IsoP), were used in humans and cattle to quantify the extent of OS. Blood IsoP were shown to be elevated and correlate with oxidant status during acute coliform mastitis. However, the effect of FM treatment on oxidant status and markers of OS has not been established. Blood IsoP concentrations were used to quantify systemic OS, whereas milk was used to assess local OS in the mammary gland. Results indicate that FM treatment had no effect on blood markers of inflammation but reduced the oxidant status index (OSi) by increasing blood AOP from pre- to post-FM treatment. Milk AOP significantly increased from pre- to post-FM treatment, whereas ROS decreased, resulting in a decreased OSi from pre- to post-FM treatment. The only blood IsoP concentration that was significantly different was 5-iso-iPF2α-VI, with a decreased concentration from pre- to post-FM treatment. Conversely, milk 5-iso-iPF2α-VI, 8,12-iso-iPF2α-VI, and total IsoP concentrations were decreased following FM treatment. These results indicated that administration of FM did improve systemic and local oxidant status and reduced local markers of OS. However, differential effects were observed between those animals that survived the infection and those that died, indicating that pre-existing inflammation and oxidant status greatly affect efficacy of FM and may be the key to reducing severity and mortality associated with acute coliform infections. Supplementation to improve AOP and anti-inflammatory mediator production may significantly improve efficacy of FM treatment.
机译:功能失调的炎症有助于显著到大肠菌乳腺炎的发病机制和经典促炎酶环氧合酶-2(COX-2)是医疗干预的使用非甾体抗炎药(NSAID)氟尼辛葡甲胺(FM)的目标。通过FM COX-2的抑制可降低促炎性基于脂肪酸的介质称为类二十烷酸,从而提供从大肠菌患乳腺炎奶牛解热镇痛作用的浓度。然而,天然存在的大肠菌群大约为50%,动物的死亡累及全身结果乳腺炎,甚至NSAID治疗。不足的抗氧化能力(AOP),以中和过量的炎症过程中产生的活性氧物质(ROS)允许氧化应激(OS),大肠菌乳腺炎期间促进组织的损伤。由ROS脂质过氧化的生物标记物,被称为异前列烷(ISOP),在人类和牲畜被用来量化OS的程度。血液ISOP被证明在急性乳腺炎大肠菌中升高和关联与氧化剂状态。然而,FM治疗对氧化状态和OS的标志物的影响尚未确定。血ISOP浓度用于定量全身OS,而牛奶是用来评估在乳腺本地操作系统。结果表明,超短波治疗对炎症的血液指标没有影响,但是从之前到之后的FM治疗增加血液AOP减少氧化剂状态指数(OSI)。牛奶AOP从之前到之后的FM治疗显著增加,而ROS明显降低,导致从之前到之后的FM治疗降低OSi的。这是显著不同的唯一血ISOP浓度为5异iPF2α-VI,其浓度从之前到之后的FM治疗降低。相反,牛奶5-异iPF2α-VI,8,12 - 异iPF2α-VI,和总ISOP浓度以下FM治疗明显降低。这些结果表明FM的给药确实改善全身和局部的氧化状态和OS的减少本地标记。然而,死亡幸存的感染的动物和那些之间观察差的影响,表明预先存在的炎症和氧化状态极大地影响FM的疗效和可能的关键是降低急性大肠菌群感染相关的严重程度和死亡率。补充改善AOP和抗炎介质产生可显著改善FM治疗的效果。

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