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首页> 外文期刊>Infection and immunity >Opsonic Antibodies to the Surface M Protein of Group A Streptococci in Pooled Normal Immunoglobulins (IVIG): Potential Impact on the Clinical Efficacy of IVIG Therapy for Severe Invasive Group A Streptococcal Infections
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Opsonic Antibodies to the Surface M Protein of Group A Streptococci in Pooled Normal Immunoglobulins (IVIG): Potential Impact on the Clinical Efficacy of IVIG Therapy for Severe Invasive Group A Streptococcal Infections

机译:混合正常免疫球蛋白(IVIG)中A组链球菌表面M蛋白的调理性抗体:对IVIG治疗严重A组链球菌感染的临床疗效的潜在影响

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摘要

The surface M protein of group A streptococci (GAS) is one of the major virulence factors for this pathogen. Antibodies to the M protein can facilitate opsonophagocytosis by phagocytic cells present in human blood. We investigated whether pooled normal immunoglobulin G (IVIG) contains antibodies that can opsonize and enhance the phagocytosis of type M1 strains of GAS and whether the levels of these antibodies vary for different IVIG preparations. We focused on the presence of anti-M1 antibodies because the M1T1 serotype accounts for the majority of recent invasive GAS clinical isolates in our surveillance studies. The level of anti-M1 antibodies in three commercial IVIG preparations was determined by enzyme-linked immunosorbent assay (ELISA), and the opsonic activity of these antibodies was determined by neutrophil-mediated opsonophagocytosis of a representative M1T1 isolate. High levels of opsonic anti-M1 antibodies were found in all IVIG preparations tested, and there was a good correlation between ELISA titers and opsonophagocytic activity. However, there was no significant difference in the levels of opsonic anti-M1 antibodies among the various IVIG preparations or lots tested. Adsorption of IVIG with M1T1 bacteria removed the anti-M1 opsonic activity, while the level of anti-M3 opsonophagocytosis was unchanged. Plasma was obtained from seven patients with streptococcal toxic shock syndrome who received IVIG therapy, and the level of anti-M1 antibodies was assessed before and after IVIG administration. A significant increase in the level of type M1-specific antibodies was found in the plasma of all patients who received IVIG therapy (P < 0.006). The results reveal another potential mechanism by which IVIG can ameliorate severe invasive group A streptococcal infections.
机译:A组链球菌(GAS)的表面M蛋白是该病原体的主要毒力因子之一。 M蛋白的抗体可促进人血中吞噬细胞的调理吞噬作用。我们调查了合并的正常免疫球蛋白G(IVIG)是否包含可以调理和增强GAS M1型菌株吞噬作用的抗体,以及这些抗体的水平对于不同的IVIG制剂是否有所不同。我们专注于抗M1抗体的存在,因为在我们的监测研究中,M1T1血清型占最近侵入性GAS临床分离株的大部分。通过酶联免疫吸附测定(ELISA)确定三种商业IVIG制剂中抗M1抗体的水平,并通过中性粒细胞介导的代表性M1T1分离物的调理吞噬作用确定这些抗体的调理活性。在所有测试的IVIG制剂中发现了高水平的调理抗M1抗体,并且ELISA滴度和调理吞噬活性之间存在良好的相关性。但是,在各种IVIG制剂或测试批次中,调理抗M1抗体的水平没有显着差异。 IVIG被M1T1细菌吸附消除了抗M1调理活性,而抗M3调理吞噬作用的水平未改变。从接受IVIG治疗的7名链球菌中毒性休克综合征患者中获取血浆,并在IVIG给药前后评估抗M1抗体的水平。在接受IVIG治疗的所有患者的血浆中均发现M1型特异性抗体水平显着增加( P <0.006)。结果揭示了IVIG可以改善严重的A组侵袭性链球菌感染的另一种潜在机制。

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