Department of Internal Medicine, Lehigh Valley Health Network, Allentown, PA, USA.
Department of Hematology and Oncology, Lehigh Valley Health Network, Allentown, PA, USA.
Am J Case Rep. 2020 May 7;21:e922326. doi: 10.12659/AJCR.922326.
BACKGROUND Acquired hemophilia A (AHA) is a rare autoimmune disease caused by immunoglobulins that bind and inactive factor VIII, thereby predisposing to life-threatening bleeding. Bleeding is typically stabilized by utilizing bypassing agents, such as recombinant factor VIIa (rVIIa). Select case reports have demonstrated the success of alternative prophylaxis for clearance of factor VIII inhibitors through the use of emicizumab, a current FDA approved medication for treatment of congenital hemophilia A. In this case report we present the efficacy of utilizing emicizumab as a prophylactic agent in a patient that was unable to tolerate first-line therapy for prophylaxis. CASE REPORT A 91-year-old male presented for ongoing hematuria for 5 weeks with prior workup unrevealing. He was given a day's course of recombinant factor VIIa to stabilize his bleeding and was started on cyclophosphamide and prednisone after a revealing hematological workup including activated partial thromboplastin time (aPTT) >100 seconds and factor VIII inhibitor level of 44 BU/mL. He continued to require VIIa infusions to control his bleeding and was started on emicizumab once stabilized. His bleeding remained controlled and his inhibitor decreased after 6 months of therapy with repeat factor VIII inhibitor level of 1.9 BU/mL. CONCLUSIONS The success of utilizing emicizumab for bleeding prophylaxis in AHA is demonstrated by this patient's resolution of bleeding. The high frequency of dosing and higher risk for thrombosis with factor VIIa, in conjunction with our patient's medical history and ease of administration, make emicizumab an ideal agent for bleeding prophylaxis while awaiting clearance of factor VIII inhibitors.
获得性血友病 A(AHA)是一种罕见的自身免疫性疾病,由结合并失活因子 VIII 的免疫球蛋白引起,从而易发生危及生命的出血。通过使用旁路制剂,如重组因子 VIIa(rVIIa),通常可以稳定出血。一些病例报告已经证明,通过使用emicizumab(一种目前获得 FDA 批准用于治疗先天性血友病 A 的药物)清除因子 VIII 抑制剂,替代预防的方法是有效的。在本病例报告中,我们介绍了在无法耐受一线预防治疗的患者中,将 emicizumab 用作预防剂的疗效。
一名 91 岁男性因持续血尿 5 周就诊,此前的检查未发现异常。他接受了为期一天的 rVIIa 治疗以稳定出血,并在进行了包括活化部分凝血活酶时间(aPTT)>100 秒和因子 VIII 抑制剂水平为 44 BU/mL 的血液学检查后,开始使用环磷酰胺和泼尼松治疗。他继续需要 VIIa 输注来控制出血,并在稳定后开始使用 emicizumab。在接受治疗 6 个月后,他的出血得到控制,抑制剂水平下降,重复因子 VIII 抑制剂水平为 1.9 BU/mL。
通过该患者出血的缓解,证明了使用 emicizumab 进行 AHA 出血预防的成功。与因子 VIIa 相比,emicizumab 的高剂量频率和更高的血栓形成风险,结合我们患者的病史和给药的便利性,使其成为因子 VIII 抑制剂清除期间出血预防的理想药物。