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Actual status of antiinterleukin-1 therapies in rheumatic diseases

机译:风湿性疾病中抗白介素1疗法的实际状况

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PURPOSE OF REVIEW: Several studies have evaluated the efficacy and safety of novel therapeutic options targeting interleukin-1 (IL-1), which not only plays a significant role in rheumatoid arthritis, but also in other rheumatic diseases, for which only limited therapeutical options exist. RECENT FINDINGS: Three different strategies have been pursued and evaluated in the past years: preventing IL-1 binding by occupying IL-1 receptors with anakinra, an imitation of the naturally occurring IL-1 receptor antagonist, anakinra; development of the fully human monoclonal anti-IL-1β antibody canakinumab; and synthesis of the dimeric fusion protein rilonacept, consisting of the ligand-binding domain of interleukin-1 receptor type I and its accessory protein, bound to human IgG1. Each of these three anti-IL-1 agents proved efficacy in distinct clinical situations and disease entities. SUMMARY: Owing to the observation that IL-1 is not only involved in signaling processes resulting in autoimmune and crystal-induced joint destruction but also in several hereditary autoinflammatory syndromes, its value both in pathophysiology as well as for novel advances in medication has significantly improved in the past years leading to an enrichment of the current therapeutic armamentarium for the affected patients.
机译:审查的目的:几项研究评估了针对白介素-1(IL-1)的新型治疗选择的疗效和安全性,白介素-1(IL-1)不仅在类风湿性关节炎中起着重要作用,而且在其他风湿性疾病中也起着重要作用,而对于这些风湿性疾病,只有有限的治疗选择存在。最近的发现:在过去的几年中,已经采取了三种不同的策略并对其进行了评估:通过用anakinra占据IL-1受体来阻止IL-1结合,anakinra是对天然存在的IL-1受体拮抗剂anakinra的模仿;全人抗IL-1β单克隆抗体canakinumab的开发;二聚体融合蛋白rilonacept的合成,该蛋白由与人IgG1结合的I型白介素1受体的配体结合结构域及其辅助蛋白组成。这三种抗IL-1药物中的每一种在不同的临床情况和疾病实体中均证明有效。摘要:由于观察到IL-1不仅参与导致自身免疫和晶体诱导的关节破坏的信号传导过程,而且还参与多种遗传性自发炎综合征,因此其在病理生理学以及药物新进展中的价值均得到了显着提高在过去的几年中,为受影响的患者提供了丰富的治疗用武器。

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