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摘要:
FTY720 and IMMH002,prodrugs for sphingosine-1-phosphate receptor 1 (S1P1) agonists,show inadequate and inconsistent levels of phosphorylation in humans compared to that in rats.In this study,FTY720 or IMMH002 analogues (21-24) were designed and synthesized with modified head pieces to improve the biotransformation of the prodrugs to the active phosphorylated forms.Target compounds were synthesized via a convergent route using the key and optically pure building block 9,which was first synthesized via asymmetrically catalyzed amination.The phosphorylation rates of these analogues in rat or human blood were compared.The new methyl-substituted analogue compound 21 showed higher phosphorylation rates in both rats and humans than the parent compound,whereas compound 23 showed improvements in rats,but not in humans.In pharmacokinetics studies of rats,compounds 21 and 23 both had higher levels of phosphorylation than FTY720 and IMMH002.Thus,our study not only yielded new compounds with therapeutic potential,but also showed species differences between rats and humans in response to the structural modifications,which might be useful for predicting the biotransformation behavior and efficacy of this class of prodrugs in the clinic.
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篇名 Design and synthesis of selective sphingosine-1-phosphate receptor 1 agonists with increased phosphorylation rates
来源期刊 药学学报(英文版) 学科
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年,卷(期) 2020,(6) 所属期刊栏目 Short communication
研究方向 页码范围 1134-1142
页数 9页 分类号
字数 语种 英文
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药学学报(英文版)
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2211-3835
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