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Cryoglobulinemic disease

机译:低温血球疾病

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"Cryoglobulinemia" refers to the presence of cryoglobulins (immunoglobulins that precipitate at variable temperatures < 37°C [98.6°F]) in serum. Monoclonal cryoglobulinemia (type I) involves a single type of monoclonal immunoglobulin, while mixed cryoglobulinemia involves a mixture either of polyclonal immunoglobulin (Ig) G and monoclonal IgM (type II), or of polyclonal IgG and polyclonal IgM (type III); both monoclonal and polyclonal IgM have rheumatoid factor activity. Cryoglobulinemia is a unique model of human disease for several reasons: (1) cryoglobulins are detected using a simple technical approach that is based on in vitro laboratory observation of cold precipitation in serum; (2) cryoglobulinemic organ damage may be produced by two different etiopathogenic mechanisms (accumulation of cryoglobulins and autoimmune-mediated vasculitic damage); and (3) cryoglobulinemia is associated with a wide range of etiologies, symptoms, and outcomes, and is considered a disease that combines elements of autoimmune and lymphoproliferative diseases. There are three main broad treatment strategies in cryoglobulinemia-conventional immunosuppression, antiviral treatment, and biologic therapy. Some agents, such as corticosteroids and rituximab, have been successfully used in all types of cryoglobulinemia; however, treatment should be modulated according to the underlying associated disease (chronic viral infections, autoimmune diseases, or cancer), the predominant etiopathogenic damage (vasculitis vs hyperviscosity), and the severity of internal organ involvement.
机译:“冰球蛋白血症”是指血清中存在冰球蛋白(在<37°C [98.6°F]的可变温度下沉淀的免疫球蛋白)。单克隆冷球蛋白血症(I型)涉及一种单克隆免疫球蛋白,而混合冷球蛋白血症涉及多克隆免疫球蛋白(Ig)G和单克隆IgM(II型)的混合物,或多克隆IgG和多克隆IgM(III型)的混合物;单克隆和多克隆IgM均具有类风湿因子活性。低温球蛋白血症是人类疾病的独特模型,其原因有以下几个方面:(1)使用一种简单的技术方法检测冷球蛋白,该方法基于体外实验室对血清冷沉淀的观察; (2)低温球蛋白器官的损伤可能是由两种不同的病因机制引起的(冷冻球蛋白的积累和自身免疫介导的血管损伤); (3)低温球蛋白血症与多种病因,症状和结局相关,被认为是结合自身免疫性疾病和淋巴增生性疾病的疾病。冷冻球蛋白血症主要有三种主要的治疗策略:常规免疫抑制,抗病毒治疗和生物治疗。一些药物,例如皮质类固醇和利妥昔单抗,已成功用于所有类型的冷球蛋白血症。但是,应根据潜在的相关疾病(慢性病毒感染,自身免疫性疾病或癌症),主要的病原性损害(血管炎与高黏度)以及内部器官受累的严重程度来调整治疗。

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  • 来源
    《Oncology》 |2013年第11期|共18页
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  • 正文语种 eng
  • 中图分类 肿瘤学;
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