抗艰难梭菌的保护性抗体存在于静脉注射免疫球蛋白中,并在给药后保留在人体内

O. Negm, B. MacKenzie, Mohamed R. Hamed, O.A.J. Ahmad, C. Shone, David Paul Humphreys, K. Acharya, Christine E. Loscher, I. Marszalowska, M. Lynch, Mark Wilcox, Tanya Monaghan
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引用次数: 18

摘要

在健康人群中,针对艰难梭菌(CD)毒素A和B的血清抗体的普遍存在,促使人们对静脉注射免疫球蛋白(IVIg)在经历严重或复发性艰难梭菌感染(CDI)的个体中的治疗活性进行评估。尽管有一些有希望的病例报告,但IVIg在CDI中的明确临床作用仍不清楚。相互矛盾的结果可能归因于对最佳剂量、给药时间和患者选择缺乏共识,以及商业制剂之间特异性抗体含量的可变性。本研究的目的是回顾性调查三种IVIg市售制剂治疗严重或复发性CDI的疗效。在随后的机制研究中,使用蛋白质微阵列和毒素中和试验,分析了所有IVIg制剂在体外对CD抗原的特异性结合和中和抗体(NAb),以及IVIg输注后体内抗毒素NAb的存在。41%(17例中的10例)的CDI患者对IVIg有治疗反应。在IVIg制剂之间以及IVIg给药前后的患者血清中,观察到针对7种CD抗原的多同型特异性抗体和毒素中和效果的显著差异。这些结果扩展了我们目前对乳糜泻人群免疫的理解,并支持在乳糜泻疫苗中包含表面层蛋白和二元毒素抗原。未来的策略可以通过在分离前使用蛋白质微阵列预先选择具有最高水平抗CD抗体和/或抗毒素中和能力的供体血浆/血清来提高IVIg治疗反应率。
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Protective antibodies against Clostridium difficile are present in intravenous immunoglobulin and are retained in humans following its administration
The prevalence of serum antibodies against Clostridium difficile (CD) toxins A and B in healthy populations have prompted interest in evaluating the therapeutic activity of intravenous immunoglobulin (IVIg) in individuals experiencing severe or recurrent C. difficile infection (CDI). Despite some promising case reports, a definitive clinical role for IVIg in CDI remains unclear. Contradictory results may be attributed to a lack of consensus regarding optimal dose, timing of administration and patient selection as well as variability in specific antibody content between commercial preparations. The purpose of this study was to investigate retrospectively the efficacy of three commercial preparations of IVIg for treating severe or recurrent CDI. In subsequent mechanistic studies using protein microarray and toxin neutralization assays, all IVIg preparations were analysed for specific binding and neutralizing antibodies (NAb) to CD antigens in vitro and the presence of anti‐toxin NAbs in vivo following IVIg infusion. A therapeutic response to IVIg was observed in 41% (10 of 17) of the CDI patients. Significant variability in multi‐isotype specific antibodies to a 7‐plex panel of CD antigens and toxin neutralization efficacies were observed between IVIg preparations and also in patient sera before and after IVIg administration. These results extend our current understanding of population immunity to CD and support the inclusion of surface layer proteins and binary toxin antigens in CD vaccines. Future strategies could enhance IVIg treatment response rates by using protein microarray to preselect donor plasma/serum with the highest levels of anti‐CD antibodies and/or anti‐toxin neutralizing capacities prior to fractionation.
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