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一例获得性 FXIII 缺乏症伴严重出血症状。

A case of acquired FXIII deficiency with severe bleeding symptoms.

机构信息

Department of Hematology, Kanazawa University Hospital, Kanazawa, Japan.

出版信息

Haemophilia. 2012 Jul;18(4):618-20. doi: 10.1111/j.1365-2516.2012.02763.x. Epub 2012 Feb 22.

Abstract

Acquired factor XIII (FXIII) deficiency due to an autoantibody against FXIII is a very rare, yet potentially life-threatening bleeding disorder. As the standard coagulation tests (prothrombin time and activated partial thromboplastin time) are normal, the specialized tests are required to make an accurate diagnosis. Here, we report a case of acquired FXIII deficiency with severe bleeding symptoms. A 75-year-old man was referred to our hospital because of severe bleeding tendency after a tooth extraction. Laboratory findings showed that routine coagulation studies were normal, but factor XIII (FXIII) activity was low (3%). The presence of FXIII inhibitor was detected with dot blotting studies. Although the bleeding tendency was very severe, it was successfully controlled by infusion of FXIII concentrates combined with immunosuppressive treatment (oral prednisolone). Fibrin cross-linking study showed the significant delay of the γ-chain dimer and α-chain polymer formation. Western blotting revealed the marked decrease in FXIII-A level. The mixing study of FXIII activity measured using amine-incorporation assay showed the incomplete inhibition pattern. There seems to be little agreement as to the treatment strategy of acquired FXIII deficiency. In this patient, the use of FXIII concentrates was very useful in the initial treatment of bleeding symptom. The use of steroids was also effective in increasing FXIII activity without any serious complications.

摘要

获得性因子 XIII(FXIII)缺乏症是一种由针对 FXIII 的自身抗体引起的非常罕见但潜在危及生命的出血性疾病。由于标准凝血试验(凝血酶原时间和活化部分凝血活酶时间)正常,因此需要进行专门的检查以做出准确的诊断。在这里,我们报告一例伴有严重出血症状的获得性 FXIII 缺乏症。一名 75 岁男性因拔牙后严重出血倾向被转至我院。实验室检查结果显示,常规凝血研究正常,但 FXIII(FXIII)活性降低(3%)。通过斑点印迹研究检测到 FXIII 抑制剂的存在。尽管出血倾向非常严重,但通过输注 FXIII 浓缩物联合免疫抑制治疗(口服泼尼松龙)成功控制了出血倾向。纤维蛋白交联研究显示 γ 链二聚体和 α 链聚合物形成明显延迟。Western blot 显示 FXIII-A 水平明显下降。使用胺掺入测定法测量 FXIII 活性的混合研究显示不完全抑制模式。对于获得性 FXIII 缺乏症的治疗策略似乎没有达成共识。在本例患者中,FXIII 浓缩物在出血症状的初始治疗中非常有用。使用类固醇也可有效增加 FXIII 活性,且无任何严重并发症。

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