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在一名患有先天性重度A型血友病且预后因素较差的儿科患者中,使用血浆源性FVIII浓缩物和静脉注射免疫球蛋白成功诱导免疫耐受。

Successful immune tolerance induction with a plasma-derived FVIII concentrate and intravenous immunoglobulins in a pediatric patient with congenital severe hemophilia A and poor prognostic factors.

作者信息

de Cos Carmen, Rodríguez-Martorell Javier

机构信息

aDepartment of Hematology and Hemotherapy, Hospital Universitario Puerta del Mar, Cádiz bDepartment of Hematology and Hemotherapy, Hospital Universitario Virgen del Rocío, Sevilla, Spain.

出版信息

Blood Coagul Fibrinolysis. 2014 Jan;25(1):77-80. doi: 10.1097/MBC.0b013e328364f992.

Abstract

We present the case of a pediatric patient born in July 1991, diagnosed with severe hemophilia A at 8 months of life after a hemarthrosis. He was treated with regular factor replacement therapy on-demand until an inhibitor was detected (1.75-2.5 BU) at the age of 6. The patient started an immunotolerance induction (ITI) program, which was discontinued 3 months later because of parental decision based on inhibitor persistence (3.75-6.75 BU). On-demand treatment with recombinant activated FVII in bleeding episodes was applied. Titer peaked 13 months later (37 BU). On May 2003 (age 11), rescue ITI with plasma-derived FVIII (Fanhdi, 100 IU/kg per 24 h daily) and intravenous immunoglobulin (IVIg) (Flebogamma, 1 g/kg per 24 h for 2 days every 3 weeks) was started. Inhibitor eradication was achieved after 16 months of ITI. The patient continued with FVIII+IVIg treatment for 3 additional months when he was switched to FVIII prophylaxis (40 IU/kg 3 times a week). At present, the patient is inhibitor-free.

摘要

我们报告一例1991年7月出生的儿科患者,该患者在8个月大时因关节积血被诊断为重度甲型血友病。他接受按需定期凝血因子替代治疗,直到6岁时检测到抑制物(1.75 - 2.5 BU)。患者开始免疫耐受诱导(ITI)方案,但3个月后因家长基于抑制物持续存在(3.75 - 6.75 BU)的决定而停药。出血发作时应用重组活化FVII进行按需治疗。13个月后抑制物滴度达到峰值(37 BU)。2003年5月(11岁),开始采用血浆源性FVIII(Fanhdi,每24小时100 IU/kg每日)和静脉注射免疫球蛋白(IVIg)(Flebogamma,每24小时1 g/kg,每3周连用2天)进行挽救性ITI。ITI 16个月后成功根除抑制物。患者继续接受FVIII + IVIg治疗3个月,之后改为FVIII预防治疗(每周3次,每次40 IU/kg)。目前,该患者无抑制物。

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