治疗甲状腺眼病的新疗法

A. Kamboj, Andrew R. Harrison, A. Mokhtarzadeh
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摘要

甲状腺眼病(TED)是一种免疫介导的疾病,具有一系列不同的表现,可能对视力和生活质量产生不利影响。随着人们对这种疾病复杂发病机理认识的不断深入,具有新分子靶点的疗法也在不断发展,为改善患者预后带来了希望。作为甲状腺眼病自身免疫和自身炎症途径的介质,不同的传统和生物免疫抑制剂已被研究。特普鲁单抗是一种抗IGF-1R单克隆抗体,最近已成为活动性中重度TED的一线疗法,与安慰剂相比,该药在突眼、复视、临床活动评分和生活质量方面均有统计学意义的显著改善。目前正在研究的其他几种旨在抑制 IGF-1R 的药物具有不同的给药方式:VRDN-001(静脉注射)、VRDN-002 或 VRDN-003(皮下注射)、lonigutamab(皮下注射)和 linsitinib(口服)。Tocilizumab是一种白细胞介素6单克隆抗体,在治疗多种自身免疫性和炎症性疾病中发挥了作用,可能有望用于治疗TED。治疗 TED 的另一个新生物靶点是新生儿 Fc 受体,抑制该受体有可能降低免疫球蛋白的循环和抗体水平;针对这一靶点的药物包括单克隆抗体和抗体片段。最后,降血脂药物可能是 TED 相关炎症的介质。目前正在研究的旨在降低 TED 相关眼部发病率的药物包括 IGF-1R、白细胞介素 6 和新生儿 Fc 受体。随着新型免疫学方法的出现,TED 的治疗范围也在不断扩大。
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Emerging therapies in the medical management of thyroid eye disease
Thyroid eye disease (TED) is an immune-mediated disorder associated with a heterogenous array of manifestations that may unfavorably impact vision and quality of life. As understanding of this entity’s complex pathogenesis has evolved, so have therapies with novel molecular targets offering promise for improved patient outcomes.Emerging immunologic therapies for the management of thyroid eye disease have diverse mechanisms of actions and routes of administration. Different conventional and biological immunosuppressive agents have been studied as mediators of the autoimmune and autoinflammatory pathways in thyroid eye disease. Teprotumumab – an anti-IGF-1R monoclonal antibody that has recently emerged as a first-line therapy for active, moderate-to-severe TED – has demonstrated statistically significant improvements in proptosis, diplopia, clinical activity score, and quality of life compared to placebo. Currently under investigation are several other agents, with varying administration modalities, that aim to inhibit IGF-1R: VRDN-001 (intravenous), VRDN-002 or VRDN-003 (subcutaneous), lonigutamab (subcutaneous), and linsitinib (oral). Tocilizumab, a monoclonal antibody of interleukin 6, has played a role in the management of multiple autoimmune and inflammatory conditions and may offer promise in TED. Another incipient biologic target for TED management is the neonatal Fc receptor, inhibition of which has potential to decrease recycling of immunoglobulin and antibody levels; agents addressing this target including monoclonal antibodies as well as antibody fragments. Finally, hypolipidemic agents may play a role as mediators of TED-associated inflammation.Among the agents under investigation that aim to decrease ocular morbidity associated with TED are agents that IGF-1R, interleukin 6, and the neonatal Fc receptor. The management of TED continues to expand with novel immunologic approaches for disease therapy.
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