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首页> 外文期刊>MEDICC review >Systemic Ozone Therapy by Rectal Insufflation for Immunoglobulin A Deficiency
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Systemic Ozone Therapy by Rectal Insufflation for Immunoglobulin A Deficiency

机译:直肠吹入全身臭氧治疗免疫球蛋白A缺乏症

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SUMMARY INTRODUCTION IgA deficiency is a primary immunodeficiency predominantly due to an antibody defect, for which there is no replacement therapy. Treatment consists of prevention and treatment of infections and other associated conditions. Given the immunomodulatory and regulatory properties of the redox balance of ozone therapy in infectious and inflammatory conditions, evaluation of its effect on IgA deficiency is of interest. OBJECTIVE Assess the benefits and possible adverse effects of ozone treatment in patients with IgA deficiency. METHODS A monocentric randomized controlled phase 2 clinical trial (RPCEC 00000236) was carried out, after approval by the Institutional Ethics Committee of the Roberto Rodríguez Fernández Provincial General Teaching Hospital in Morón, Ciego de ávila Province, Cuba. Included were 40 patients aged 5–50 years, distributed in 2 groups of 20, after agreeing to participate and signing informed consent. The experimental group received 2 cycles of ozone by rectal insufflation for 20 days (5 times a week for 4 weeks each cycle) with a 3-month interval between cycles, for a total of 40 doses, with age-adjusted dose ranges. The control group was treated with leukocyte transfer factor (Hebertrans), 1 U per m2 of body surface area subcutaneously, once weekly for 12 weeks. Frequency of appearance and severity of clinical symptoms and signs of associated diseases, serum immunoglobulin concentrations and balance of pro-oxidant and antioxidant biomarkers were recorded at treatment initiation and one month after treatment completion. Therapeutic response was defined as complete, partial, stable disease or progressive disease. Descriptive statistics and significance were calculated to compare groups and assess effect size. RESULTS One month after treatment completion, 70% of patients in the experimental group experienced significant increases in IgG (p = 0.000) and IgM (p = 0.033). The experimental group also displayed decreased pro-oxidation biomarkers, glutathione modulation and increased antioxidant enzymes, with reduced oxidative stress; none of these occurred in the control group. Complete therapeutic response was achieved in 85% of patients in the experimental group and only 45% in the control group. Mild, transient adverse events were reported in both groups. CONCLUSIONS Ozone therapy by rectal insufflation is a suitable therapeutic option for treating IgA deficiency because it produces antioxidant and immunomodulatory effects and is feasible, safe and minimally invasive. CONTRIBUTION OF THIS RESEARCH This paper introduces in Cuba a new treatment a for IgA deficiency, with immunomodulatory and antioxidant effects offering substantial clinical benefits to patients with this immunodeficiency.
机译:发明概述引言IgA缺乏症是主要由于抗体缺陷的原发性免疫缺陷,对此没有替代疗法。治疗包括预防和治疗感染及其他相关疾病。鉴于臭氧疗法在感染性和炎症性条件下氧化还原平衡的免疫调节和调节特性,评估其对IgA缺乏症的影响是很有意义的。目的评估臭氧治疗对IgA缺乏症患者的益处和可能的不利影响。方法经古巴古巴Ciego de Avila省Morón的RobertoRodríguezFernández省总教学医院机构伦理委员会批准,进行了单中心随机对照2期临床试验(RPCEC 00000236)。在同意参加并签署知情同意书后,包括40位5至50岁的患者,分为2组,每组20个。实验组通过直肠吹入法接受了2个臭氧循环,共20天(每周5次,每个循环4周),每个循环之间间隔3个月,共40剂,并根据年龄调整了剂量范围。对照组皮下注射白细胞转移因子(Hebertrans),每平方米体表面积1 U,每周一次,持续12周。在治疗开始时和治疗结束后一个月,记录出现频率和临床症状的严重程度以及相关疾病的体征,血清免疫球蛋白浓度以及促氧化剂和抗氧化剂生物标志物的平衡。治疗反应定义为完全,部分,稳定疾病或进行性疾病。计算描述性统计数据和显着性以比较各组并评估效果大小。结果治疗完成一个月后,实验组中70%的患者的IgG(p = 0.000)和IgM(p = 0.033)显着增加。实验组还显示出减少的前氧化生物标志物,谷胱甘肽调节和增加的抗氧化酶,并减少了氧化应激。这些都没有发生在对照组中。实验组中85%的患者获得了完全的治疗反应,而对照组中只有45%的患者获得了完全的治疗反应。两组均报告了轻度,短暂的不良事件。结论直肠吹入臭氧疗法是治疗IgA缺乏症的合适治疗选择,因为它产生抗氧化和免疫调节作用,并且可行,安全且微创。该研究的贡献本文在古巴介绍了一种针对IgA缺乏症的新疗法,其具有免疫调节和抗氧化作用,可为患有这种免疫缺陷的患者提供大量的临床益处。

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