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Maternally transferred anti-factor VIII IgG reduce the anti-factor VIII humoral immune response in factor VIII-deficient mice

机译:母源转移的抗VIII因子IgG可降低VIII因子缺陷型小鼠的VIII抗体液免疫反应

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摘要

Replacement therapy with exogenous factor VIII (FVIII) to treat haemorrhages or used in prophylaxis induces inhibitory anti-FVIII immunoglobulin G (IgG) in some patients with haemophilia A. Therapeutic strategies to prevent the onset of the deleterious anti-FVIII immune response are still lacking. Maternal IgG is transferred to the offspring during fetal and neonatal life. While protecting the offspring from bacterial and viral infections, maternal IgG may alter the repertoires of T and B lymphocytes, and may impair vaccination in early infancy. Using haemophilic mice, we demonstrate that the transfer of maternal anti-FVIII IgG modulates the onset of anti-FVIII inhibitory IgG in early adulthood. The protective effect is reproduced upon reconstitution of naive mice with anti-FVIII IgG, suggesting that the reduced ability to mount an anti-FVIII immune response is the result of an interference between circulating anti-FVIII IgG and the administered FVIII rather than to a profound remodelling of lymphocyte repertoires occurring during the ontogeny of the immune system.
机译:在一些A型血友病患者中,用外源性因子VIII(FVIII)替代疗法来治疗出血或用于预防可诱导抑制性抗FVIII免疫球蛋白G(IgG)的出现。仍然缺乏防止有害的抗FVIII免疫应答发作的治疗策略。 。在胎儿和新生儿生命中,母体IgG会转移到后代。在保护后代免受细菌和病毒感染的同时,母体IgG可能会改变T和B淋巴细胞的组成,并可能损害婴儿早期的疫苗接种。使用嗜血性小鼠,我们证明母体抗FVIII IgG的转移在成年初期可以调节抗FVIII抑制性IgG的发作。当用抗FVIII IgG的天真小鼠重建后,就会产生保护作用,这表明降低抗FVIII免疫反应的能力是循环的抗FVIII IgG与所用FVIII之间干扰的结果,而不是对免疫系统发育过程中发生的淋巴细胞组成的重塑。

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