Division of Haematology, SA Pathology, South Australia, Australia.
Semin Thromb Hemost. 2009 Nov;35(8):769-77. doi: 10.1055/s-0029-1245109. Epub 2010 Feb 18.
Acquired hemophilia A (AH) is a rare and serious acquired bleeding disorder where prompt and correct diagnosis is crucial, and immune suppression is often required for factor VIII (FVIII) autoantibody eradication. The acquired FVIII deficiency usually manifests as bruises and bleeding, and treatment such as FVIII has limited efficacy because of the neutralizing FVIII inhibitor. Expensive bypassing agents such as recombinant activated factor VII (rFVIIa) may be required to treat clinically significant bleeding. This report summarizes the experience related to AH from a large Australian hemophilia center based in South Australia. We identified 25 patients retrospectively over 12 years (1997 to 2008) and reviewed diagnostic features, treatment for bleeds and to eradicate the autoantibody, treatment response, and survival outcomes. The incidence in South Australia was 1.20 cases per million/year with a median age of 78 years with an approximately equivalent sex ratio (12 males versus 13 females); median FVIII and inhibitor titer were 2.5 IU/dL and 11.0 BU/mL, respectively. Twenty-four patients were evaluated further. Thirteen patients (54%) required hemostatic agents, and rFVIIa was used in seven for major bleeds, of which four were limb or life threatening. Eighteen patients were treated by hematologists with immune suppression, and combination steroid and azathioprine was used most commonly to eradicate autoantibody; 15 of these 18 achieved remission (i.e., 83% response rate). Two patients had persistent low-titer inhibitor when treatments were withdrawn, and one died of a fatal bleed shortly after starting treatment. One had spontaneous remission. Five patients (33%) relapsed, three in less than 6 months after starting treatment; all were retreated successfully. Rituximab was used in six patients for high-titer inhibitor, second relapse, two life-threatening bleeds, underlying lymphoma, and steroid intolerance, respectively. Overall mortality was 25% ( N = 6), five of whom were not treated. Advanced age and lack of treatment were predictive of poor survival outcomes. The very elderly (>75 years of age) may warrant a different treatment modality such as rituximab, which is potentially more tolerable and efficacious.
获得性血友病 A (AH) 是一种罕见且严重的获得性出血性疾病,及时正确的诊断至关重要,通常需要免疫抑制来消除因子 VIII (FVIII) 自身抗体。获得性 FVIII 缺乏症通常表现为瘀伤和出血,由于存在中和 FVIII 抑制剂,FVIII 等治疗方法的疗效有限。可能需要昂贵的旁路制剂,如重组激活因子 VII (rFVIIa) 来治疗具有临床意义的出血。本报告总结了澳大利亚南澳大利亚一家大型血友病中心的 AH 相关经验。我们回顾性地在 12 年内(1997 年至 2008 年)确定了 25 名患者,并回顾了诊断特征、出血治疗和消除自身抗体、治疗反应和生存结局。南澳大利亚的发病率为每百万分之 1.20,中位年龄为 78 岁,男女比例大致相等(12 名男性对 13 名女性);中位 FVIII 和抑制剂滴度分别为 2.5IU/dL 和 11.0BU/mL。进一步评估了 24 名患者。13 名患者(54%)需要止血剂,7 名患者因大出血使用 rFVIIa,其中 4 名患者为肢体或危及生命的出血。18 名患者由血液学家进行免疫抑制治疗,最常用的是联合使用类固醇和硫唑嘌呤来消除自身抗体;18 名患者中有 15 名(83%的反应率)达到缓解。2 名患者停药后持续存在低滴度抑制剂,1 名患者在开始治疗后不久死于致命性出血。1 名患者自发缓解。5 名患者(33%)复发,其中 3 名在开始治疗后不到 6 个月复发;所有患者均成功再次治疗。利妥昔单抗用于 6 名患者治疗高滴度抑制剂、第二次复发、两次危及生命的出血、潜在淋巴瘤和类固醇不耐受。总体死亡率为 25%( N = 6),其中 5 名患者未接受治疗。高龄和缺乏治疗是预后不良的预测因素。非常高龄(>75 岁)可能需要不同的治疗方式,如利妥昔单抗,其潜在更耐受且有效。
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