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首页> 外文期刊>Journal of thrombosis and haemostasis: JTH >Factor? VIII VIII products and inhibitor development in previously treated patients with severe or moderately severe hemophilia?A: a systematic review
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Factor? VIII VIII products and inhibitor development in previously treated patients with severe or moderately severe hemophilia?A: a systematic review

机译:因素? VIII VIII产品和抑制剂发育在先前治疗严重或中度严重的血友病患者的患者?A:系统审查

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Essentials Data on product‐related immunogenicity in previously treated haemophilia A patients is scarce. A systematic review and meta‐analysis of all currently available evidence was conducted. The overall incidence rate was 2.06 per 1000 person‐years (95% confidence interval: 1.06‐4.01). Some recombinant factor VIII products were associated with increased immunogenicity. Summary Background Patients with severe hemophilia?A who have been treated extensively with factor? VIII products have a low but potentially serious risk of inhibitor development. It is unknown why these patients develop inhibitors, and data on product‐related immunogenicity are scarce. Aims To summarize the currently available evidence on the relationship between inhibitor development and recombinant FVIII product type in previously treated patients ( PTP s) with severe hemophilia?A. Methods Longitudinal studies were included that reported on de?novo inhibitor formation in patients with baseline FVIII activity levels of ?0.02? IU ? mL ?1 who had been treated with FVIII for at least 50?days. Pooled incidence rates of inhibitor development according to product types were calculated with a random intercept Poisson regression model. Results Forty‐one independent cohorts were included; 39 patients developed de?novo inhibitors during 19?157?person‐years of observation. The overall incidence rate was 2.06 per 1000?person‐years, with a 95% confidence interval ( CI ) of 1.06–4.01. According to product type, the pooled incidence rates were 0.99 (95%? CI ?0.37–2.70) per 1000?person‐years for patients treated with Advate, 5.86 (95%? CI ?0.25–134.92) per 1000?person‐years for those treated with Kogenate/Helixate, 1.35 (95%? CI ?0.66–2.77) per 1000?person‐years for those treated with Kogenate? FS /Helixate NexGen, 12.05 (95%? CI ?1.53–94.78) per 1000?person‐years for those treated with Refacto, and 4.64 (95%? CI ?0.82–26.43) per 1000?person‐years for those treated with Refacto? AF . Conclusion These results suggest that some products may be associated with increased immunogenicity. However, the low incidence of inhibitors in PTP s and the differences in study design may cause significant variation in estimates of risk.
机译:在先前处理过的血友病中的产品相关免疫原性的基本数据是稀缺的。对所有现有证据进行系统审查和荟萃分析。总发生率为2.06每1000人 - 年(95%置信区间:1.06-4.01)。一些重组因子VIII产物与增加的免疫原性相关。摘要背景血友病患者(严重血友病患者)是谁被广泛治疗的因素? VIII产品具有低但潜在的抑制剂发育风险。它尚不赘述为什么这些患者发展抑制剂,以及与产品相关的免疫原性的数据很少。旨在总结目前可用的证据,就预先治疗的患者(PTP S)具有严重血友病的抑制剂发育和重组FVIII产品类型之间的关系?a。方法包括纵向研究,报道患者在基线FVIII活性水平的患者中涉及DE?Novo抑制剂形成。?0.02? IU? ML?1曾经用FVIII治疗至少50岁的人。用随机拦截泊松回归模型计算根据产品类型的抑制剂发育的抑制率。结果包括44个独立队列; 39名患者在19岁时开发了DE?Novo抑制剂157?人类的观察年。总发病率为每1000百万的2.06人 - 年,具有1.06-4.01的95%置信区间(CI)。根据产品类型,汇集的发病率为每1000个(95%?CI?0.37-2.70)为每1000?患者治疗的患者,5.86(95%?CI?0.25-134.92)每1000?人数 - 年对于用Kogenerate / Herixate治疗的那些,每1000个(95%?CI?0.66-2.77)为每1000?人类为kuengate治疗的人? FS / HERIXATE NEXGEN,12.05(95%?CI?1.53-94.78)每1000个?对于使用重构处理的人,4.64(95%?CI?0.82-26.43)每1000?人为 - 为受试者治疗重构? AF。结论这些结果表明,一些产品可能与增加的免疫原性相关。然而,PTP中的抑制剂的发病率低以及研究设计的差异可能导致风险估算中的显着变化。

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