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Peripheral Serotonin Synthesis as a New Drug Target

机译:外周血清素合成作为一种新药靶标

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The first step in serotonin (5-HT) biosynthesis is catalyzed by tryptophan hydroxylase (TPH). There are two independent sources of the monoamine that have distinct functions: first, the TPH1-expressing enterochromaffin cells (ECs) of the gut; second, TPH2-expressing serotonergic neurons. TPH1-deficient mice revealed that peripheral 5-HT plays important roles in platelet function and in inflammatory and fibrotic diseases of gut, pancreas, lung, and liver. Therefore, TPH inhibitors were developed which cannot pass the blood-brain barrier to specifically block peripheral 5-HT synthesis. They showed therapeutic efficacy in several rodent disease models, and telotristat ethyl is the first TPH inhibitor to be approved for the treatment of carcinoid syndrome. We review this development and discuss further therapeutic options for these compounds.
机译:血清素(5-HT)生物合成的第一步是由色氨酸羟化酶(TPH)催化。 单胺有两个独立的来源,具有不同的功能:第一,表达TPH1表达肠道的肠溶肠道细胞(ECS); 二,TPH2表达血清奈良菌神经元。 TPH1缺陷小鼠揭示了外周5-HT在血小板功能和肠道,胰腺,肺和肝脏的炎症和纤维化疾病中起重要作用。 因此,开发了TPH抑制剂,其不能通过血脑屏障,特别是嵌段外周5-HT合成。 它们在几种啮齿动物疾病模型中表现出治疗效果,并且Thotristat乙基是批准的TPH抑制剂用于治疗毒素综合征。 我们审查了这一发展,并讨论了这些化合物的进一步治疗选择。

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