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The dilemma of treating hepatitis C virus-associated cryoglobulinemia

机译:治疗丙型肝炎病毒相关乳蛋白血症的困境

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Purpose of review The present review focuses on the new therapeutic opportunities offered by the combination of biological drugs, mainly Rituximab, with direct-acting antiviral agents (DAAs). Recent findings Hepatitis C virus (HCV) is known to be the etiologic agent in the majority of patients with mixed cryoglobulinemia syndrome. Clinical research has been focused on antiviral drugs and, more recently, on the new, highly potent DAAs. New DAAs assure sustained virologic response (SVR) rates greater than 90% with relief of mild-to-moderate symptoms. Mixed cryoglobulinemia may present with multiorgan vasculitis involving kidneys, joints, skin, and peripheral nerves. Data on DAAs efficacy in HCV-associated cryoglobulinemic vasculitis are disappointing possibly because of the inability of these drugs to suppress the immune-mediated process once it has been triggered. Immunosuppression has often been employed in the past as a first-line therapy in cryoglobulinemic vasculitis despite the potential risk of the infection exacerbation. However, more manageable Rituximab-based therapeutic approaches have been more recently used without increase of viral load. Rituximab substantially changed the outcome of HCV-associated cryoglobulinemic vasculitis by providing long-term remission. A combination schedule of DAAs and Rituximab may result in eradication of both cryoglobulinemic vasculitis and HCV infection.
机译:审查目的目前的审查重点介绍了生物药物,主要是Rituximab的新的治疗机会,具有直接作用的抗病毒药物(DAAS)。最近发现丙型肝炎病毒(HCV)是众所周知的大多数患有混合冷冻蛋白血症综合征患者的病因试剂。临床研究一直专注于抗病毒药物,最近,在新的高度有效的DAA上。新的DAAS确保持续的病毒学反应(SVR)率大于90%,缓解温和至中等症状。混合的干酪蛋白血症可能存在涉及肾脏,关节,皮肤和周围神经的多功能血管炎。关于HCV相关的干燥致血管膜炎的DAAs疗效数据可能是由于这些药物不能在触发后抑制免疫介导的过程而令人失望。除了潜在的感染情况恶化的潜在风险,免疫抑制通常在过去作为冷冻纤维素血管炎的一线治疗。然而,最近使用了更易于扫描的利妥昔单抗的治疗方法而不会增加病毒载荷。 Rituximab通过提供长期缓解基本上改变了HCV相关的色糊精血管炎的结果。 DAAs和Rituximab的组合时间表可能导致无胶质血管血管血管炎和HCV感染的根除。

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