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Partial immune reconstitution of X-linked hyper IgM syndrome with recombinant CD40 ligand

机译:X连锁的高IgM综合征与重组CD40配体的部分免疫重建

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摘要

X-linked hyper IgM syndrome (XHM) is a combined immune deficiency disorder caused by genetic alterations in CD40 ligand. The purpose of this study was to investigate the safety and efficacy of recombinant CD40 ligand (rCD40L) in the treatment of the disease. Three children were administered rCD40L subcutaneously 3 times per week at 0.03 mg/kg for 22 weeks, and after a 12-week drug-free interval, the dose was increased to 0.05 mg/kg for an additional 22 weeks of treatment. Although specific antibody responses to T cell–dependent antigens was lacking, administration of rCD40 resulted in acquisition of the capacity to mount cutaneous delayed type hypersensitivity reactions that disappeared during the drug-free interval as well as the postbiologic follow-up period. With rCD40L treatment, patient T cells developed a new capacity to respond to T-cell mitogens with synthesis of IFN-γ and TNF-α. Intracellular cytokine staining studies showed that both CD4+ and CD8+ T cells participated in this response. Finally, CD40L therapy was associated with changes in lymph node size and architecture based on comparison of biopsies taken before and after therapy. This clinical study showed that rCD40L is capable of improving T cell–immune function in patients with XHM.
机译:X连锁性高IgM综合征(XHM)是由CD40配体的遗传改变引起的综合性免疫缺陷疾病。这项研究的目的是研究重组CD40配体(rCD40L)在疾病治疗中的安全性和有效性。 3名儿童以0.03 mg / kg的剂量每周皮下注射rCD40L 3次,共22周,在无药间隔12周后,剂量增加至0.05 mg / kg,再进行22周的治疗。尽管缺乏对T细胞依赖性抗原的特异性抗体反应,但是rCD40的使用导致获得了皮肤延迟型超敏反应的能力,这种反应在无药间隔以及生物学后的随访期间消失了。通过rCD40L治疗,患者的T细胞发展出了一种新的能力,可以通过合成IFN-γ和TNF-α来响应T细胞的有丝分裂原。细胞内细胞因子染色研究表明CD4 + 和CD8 + T细胞均参与了该反应。最后,根据治疗前后进行的活检比较,CD40L治疗与淋巴结大小和结构改变有关。这项临床研究表明,rCD40L能够改善XHM患者的T细胞免疫功能。

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