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Recombinantly engineered human proteins: transforming the treatment of psoriasis.

机译:重组工程化的人类蛋白质:改变牛皮癣的治疗方法。

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摘要

Psoriasis is a chronic, inflammatory disease with lesions that produce considerable physical discomfort and often lead to substantial disruption in patients' daily activities. The use of currently available, nonspecific, systemic immunosuppressive therapies for patients with moderate to severe psoriasis is limited by an inability to maintain disease remission safely. Advances in recombinant DNA technology paralleled with increased understanding of the immunopathology of psoriasis have led to the development of numerous biologic agents for the treatment of this disease. These new biologic therapies target specific steps in psoriasis pathology, including direct effects on T cells, T cell activation, T cell migration, and cellular production and secretion of cytokines. By selectively targeting the activities of T cells that are directly involved in psoriasis pathogenesis, these novel agents offer improved safety profiles and enhanced efficacy. In this article, the mechanisms of T cell pathogenicity that guided the development of these new biologic therapies are reviewed along with clinical data on the progress of these agents.
机译:牛皮癣是一种慢性炎性疾病,其病变会引起相当大的身体不适,并经常导致患者日常活动的严重中断。对于中度至重度牛皮癣患者,目前无法使用的非特异性全身免疫抑制疗法的使用受到局限,原因是无法安全地维持疾病的缓解。重组DNA技术的进步与对牛皮癣免疫病理学认识的增强相结合,导致了许多用于治疗这种疾病的生物制剂的开发。这些新的生物疗法针对牛皮癣病理学的特定步骤,包括对T细胞,T细胞活化,T细胞迁移以及细胞产生和分泌细胞因子的直接作用。通过选择性靶向直接参与牛皮癣发病机制的T细胞的活性,这些新型药物可改善安全性并提高疗效。在本文中,对指导这些新的生物疗法发展的T细胞致病性机制以及这些药物进展的临床数据进行了综述。

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