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Development of small-molecule therapies for autoimmune diseases.

机译:开发用于自身免疫性疾病的小分子疗法。

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Until the recent advent of genetically engineered drugs, small molecules constituted the predominant method of treatment for autoimmune diseases. Both modalities have advantages and disadvantages; while protein-based therapeutics interfere very selectively with the function of their biological targets, they have to be administered subcutaneously or intravenously. Small molecules have the potential for oral administration. Due to their cell permeability, they can interact with extra- and intracellular targets, thus opening opportunities for interfering with novel biochemical pathways. We herein describe the preclinical stages of typical small-molecule research programmes and outline hurdles that may have to be overcome. A few examples of small molecules that are currently under clinical evaluation and arose from diverse discovery pathways will be discussed.
机译:直到最近基因工程药物的出现,小分子才成为治疗自身免疫性疾病的主要方法。两种方式都有优点和缺点;尽管基于蛋白质的疗法非常有选择性地干扰其生物学靶标的功能,但必须通过皮下或静脉内给药。小分子具有口服的潜力。由于它们的细胞渗透性,它们可以与细胞外和细胞内靶标相互作用,从而为干扰新的生化途径提供了机会。我们在此描述了典型的小分子研究计划的临床前阶段,并概述了可能必须克服的障碍。将讨论一些小分子的例子,这些小分子目前正在临床评估中,并且源于多种发现途径。

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