前药
运输机
氨基酸
化学
血脑屏障
跨膜蛋白
氨基酸转运体
生物化学
组合化学
立体化学
生物
基因
受体
中枢神经系统
神经科学
作者
Henna Ylikangas,Kalle Malmioja,Lauri Peura,Mikko Gynther,Emmanuel Nwachukwu,Jukka Leppänen,Krista Laine,Jarkko Rautio,Maija Lahtela‐Kakkonen,Kristiina M. Huttunen,Antti Poso
出处
期刊:ChemMedChem
[Wiley]
日期:2014-09-09
卷期号:9 (12): 2699-2707
被引量:66
标识
DOI:10.1002/cmdc.201402281
摘要
L-Type amino acid transporter 1 (LAT1) is a transmembrane protein expressed abundantly at the blood-brain barrier (BBB), where it ensures the transport of hydrophobic acids from the blood to the brain. Due to its unique substrate specificity and high expression at the BBB, LAT1 is an intriguing target for carrier-mediated transport of drugs into the brain. In this study, a comparative molecular field analysis (CoMFA) model with considerable statistical quality (Q(2) =0.53, R(2) =0.75, Q(2) SE=0.77, R(2) SE=0.57) and good external predictivity (CCC=0.91) was generated. The model was used to guide the synthesis of eight new prodrugs whose affinity for LAT1 was tested by using an in situ rat brain perfusion technique. This resulted in the creation of a novel LAT1 prodrug with L-tryptophan as the promoiety; it also provided a better understanding of the molecular features of LAT1-targeted high-affinity prodrugs, as well as their promoiety and parent drug. The results obtained will be beneficial in the rational design of novel LAT1-binding prodrugs and other compounds that bind to LAT1.
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