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Challenges in the search for drugs to treat central nervous system disorders.

机译:寻找治疗中枢神经系统疾病的药物面临的挑战。

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摘要

The history of drug discovery spans approximately 200,000 years. For much of this time, the identification of therapeutic agents was empirical, with the shift to a more hypothesis-driven approach occurring in the late 19th century. Since then, the objective has changed from identifying an active drug and its mechanism of action to determining therapeutic potential only after identifying drug-like compounds that interact with a target site. Although the emphasis on target identification, or "targephilia," has yielded novel drugs, overall it appears to have slowed the drug discovery process, especially for compounds used in treating central nervous system (CNS) disorders. This is because the "targephilic" approach requires a good understanding of target physiology and its integration with the target organ, with a hierarchical integration from in vitro cellular and functional tissue studies to animal models that reasonably predict human responses. Because the majority of CNS drugs were discovered empirically, drug discovery in this area appears less amenable to target-based approaches than it seems for other types of therapeutics. Improving the success rate in CNS drug discovery requires a more pharmacometric-based approach, with a renewed emphasis on defining basic CNS function in intact animals and a more systematic in vivo screening of novel structures. Efforts must also be directed toward defining the sites of action of existing CNS drugs to aid in the design of second-generation agents with improved efficacy and safety.
机译:药物发现的历史大约有20万年。在这段时间的大部分时间里,治疗剂的鉴定都是凭经验进行的,在19世纪后期,人们转向了更多的假设驱动的方法。从那时起,目标已从鉴定一种活性药物及其作用机理转变为仅在鉴定与靶位点相互作用的类药物化合物后才确定治疗潜力。尽管对目标识别或“ targephilia”的重视已产生了新药,但总体看来,它已减慢了药物发现过程的速度,特别是对于用于治疗中枢神经系统(CNS)疾病的化合物。这是因为“亲友性”方法需要对靶标生理及其与靶标器官的整合有充分的了解,并且需要进行从体外细胞和功能组织研究到合理预测人类反应的动物模型的层次化整合。由于大多数中枢神经系统药物是凭经验发现的,因此与其他类型的治疗方法相比,该领域的药物发现似乎不适合基于靶标的方法。提高中枢神经系统药物发现的成功率,需要一种更加基于药理学的方法,重点是在完整动物中定义中枢神经系统的基本功能,以及对新结构进行更系统的体内筛选。还必须努力确定现有CNS药物的作用部位,以帮助设计具有更高功效和安全性的第二代药物。

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