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首页> 外文期刊>Clinical Pharmacology and Therapeutics >Effects of supportive treatment such as antioxidant or leukotriene receptor antagonist drugs on inflammatory and respiratory parameters in asthma patients.
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Effects of supportive treatment such as antioxidant or leukotriene receptor antagonist drugs on inflammatory and respiratory parameters in asthma patients.

机译:支持治疗(例如抗氧化剂或白三烯受体拮抗剂)对哮喘患者炎症和呼吸参数的影响。

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In this study, prospectively, we aimed to determine the effects of the different treatment alternatives on the oxidant system and inflammatory and clinic determinants during the stable period of 1 month following an asthmatic attack. Thirty-one patients (22 female, nine male) were randomly divided into three groups following the stabilization of an acute asthma attack. The control group that is an additional group to the three patient groups consisted of 10 healthy volunteers (five female, five male). The following protocols were used for 4 weeks: Group I: short-acting inhaler beta2 mimetic as required (treatment A)+800 mug inhaler budesonide (treatment B)+leukotriene receptor antagonist; Group II: treatment A and B; Group III: treatment A and B+vitamin E. The serum levels before and after treatment of eosinophilic cationic protein (ECP), leukotriene E4 (LTE(4)), and malondialdehyde (MDA) were determined. The values before and after treatment were statistically compared both with each other and controlvalues. Pretreatment ECP, LTE(4), and MDA levels for the three groups were significantly higher compared with post-treatment levels (P<0.05 to P<0.001) and the control levels (P<0.01 to P<0.001). However, when post-treatment levels were compared with those of the control group, no significant differences were found (P>0.05). Lack of significant variation was observed when the pre- and post-treatment differences in the three groups were compared for each one of ECP, LTE(4), and MDA levels (P>0.05). Leukotriene receptor antagonist or antioxidant agents added to standard asthma treatment did not make a significant contribution on ECP, LTE(4), and MDA levels and respiratory parameters such as spirometric function tests. Etiologic factors and/or the possible changes in different pathogenetic ways of the inflammation process may have been responsible for nonsignificant intertreatment difference in the biomarker levels. The result confirms that suppressing the inflammation in asthma enables the entire inflammatory pathologic process to be controlled.
机译:前瞻性地,在这项研究中,我们旨在确定哮喘发作后的1个月稳定期内,不同治疗方法对氧化剂系统以及炎症和临床决定因素的影响。在急性哮喘发作稳定后,将31例患者(22例女性,9例男性)随机分为三组。作为三个患者组的补充组的对照组包括10名健康志愿者(5名女性,5名男性)。使用以下方案治疗4周:第I组:根据需要使用短效吸入器beta2模拟物(治疗A)+ 800杯吸入式布地奈德(治疗B)+白三烯受体拮抗剂;第二组:治疗A和B;第三组:治疗A和B +维生素E。确定了嗜酸性阳离子蛋白(ECP),白三烯E4(LTE(4))和丙二醛(MDA)治疗前后的血清水平。将治疗前后的值与对照值进行统计学比较。三组的治疗前ECP,LTE(4)和MDA水平均显着高于治疗后水平(P <0.05至P <0.001)和对照组水平(P <0.01至P <0.001)。然而,当将治疗后水平与对照组进行比较时,没有发现显着差异(P> 0.05)。比较ECP,LTE(4)和MDA中每一种的三组治疗前后的差异,观察到没有显着差异(P> 0.05)。标准哮喘治疗中添加的白三烯受体拮抗剂或抗氧化剂对ECP,LTE(4)和MDA水平以及呼吸参数(如肺功能测定)没有显着影响。病因和/或炎症过程不同致病方式的可能变化可能是造成生物标志物水平之间无显着差异的原因。该结果证实,抑制哮喘中的炎症能够控制整个炎症病理过程。

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