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Humanized anti-CD4 monoclonal antibody therapy of autoimmune and inflammatory disease

机译:人源化抗CD4单克隆抗体治疗自身免疫性和炎症性疾病

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摘要

We have investigated the biological and therapeutic properties of a humanized anti-CD4 MoAb, hlgGl-CD4, in patients with refractory psoriasis and rheumatoid arthritis (RA). hIgGl-CD4 is a modulating, non-depleting MoAb, which induced a first-dose reaction in most patients treated. It provided brief symptomatic relief in both conditions, and psoriasis appeared easier to control with conventional agents after MoAb therapy. At the doses used, hIgGl-CD4 did not synergize therapeutically with the pan-lymphocyte MoAb CAMPATH-1H (C1H) in patients with RA treated sequentially with both agents. There were no serious adverse effects definitely attributable to therapy. Our results are compared with those of other CD4 MoAb studies, and factors influencing the outcome of therapy are discussed.
机译:我们已经研究了难治性牛皮癣和类风湿关节炎(RA)患者的人源化抗CD4 MoAb,hlgG1-CD4的生物学和治疗特性。 hIgG1-CD4是一种调节性的,不消耗性的MoAb,可在大多数接受治疗的患者中引起首次剂量反应。在两种情况下,它都能提供短暂的症状缓解,并且在使用MoAb治疗后,使用常规药物似乎更容易控制牛皮癣。在所使用的剂量下,在先后用两种药物治疗的RA患者中,hIgG1-CD4与泛淋巴细胞MoAb CAMPATH-1H(C1H)在治疗上均无协同作用。没有明显可归因于治疗的严重不良反应。我们的结果与其他CD4 MoAb研究的结果进行了比较,并讨论了影响治疗结果的因素。

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