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Design and Synthesis of mGlu2 NAMs withImproved Potency and CNS Penetration Based on a Truncated PicolinamideCore

机译：mGlu2 NAMs的设计与合成截短的吡啶甲酰胺改善了药效和中枢神经系统的渗透性核心

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摘要

Herein, we detail the optimization of the mGlu2 negative allosteric modulator (NAM), VU6001192, by a reductionist approach to afford a novel, simplified mGlu2 NAM scaffold. This new chemotype not only affords potent and selective mGlu2 inhibition, as exemplified by VU6001966 (mGlu2 IC50 = 78 nM, mGlu3 IC50 > 30 μM), but also excellent central nervous system (CNS) penetration (Kp = 1.9, Kp,uu = 0.78), a feature devoid in all previously disclosed mGlu2 NAMs (Kps ≈ 0.3, Kp,uus ≈ 0.1). Moreover, this series, based on overall properties, represents an exciting lead series for potential mGlu2 PET tracer development.

机译：在这里，我们详细介绍了通过还原论方法对mGlu2负变构调节剂（NAM）VU6001192的优化，以提供新颖，简化的mGlu2 NAM支架。这种新的化学型不仅提供有效的选择性mGlu2抑制作用（如VU6001966所示（mGlu2 IC50 = 78 nM，mGlu3 IC50> 30μM），而且还具有出色的中枢神经系统（CNS）渗透性（Kp = 1.9，Kp，uu = 0.78）），这是所有先前公开的mGlu2 NAM中都没有的特征（Kps≈0.3，Kp，uus≈0.1）。此外，基于总体性能，该系列代表了潜在的mGlu2 PET示踪剂开发的激动人心的铅系列。

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期刊名称 ACS Medicinal Chemistry Letters
作者
KatrinaA. Bollinger; Andrew S. Felts; Christopher J. Brassard; Julie L. Engers; Alice L. Rodriguez; Rebecca L. Weiner; Hyekyung P. Cho; Sichen Chang; Michael Bubser; Carrie K. Jones; Anna L. Blobaum; Colleen M. Niswender; P. Jeffrey Conn; Kyle A. Emmitte; ⊥; Craig W. Lindsley; *;
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年(卷),期 2017(8),9
年度 2017
页码 919–924
总页数 6
原文格式 PDF
正文语种
中图分类药物化学;
关键词
Negative allosteric modulator (NAM) metabotropic glutamate receptor 2 (mGlu2) depression VU6001966 CNS penetration;

机译：负变构调节剂（NAM）;代谢型谷氨酸受体2（mGlu2）;抑郁症;VU6001966;CNS渗透;

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专利

1. Design and Synthesis of mGlu₂ NAMs with Improved Potency and CNS Penetration Based on a Truncated Picolinamide Core [J] . Katrina A. Bollinger, Andrew S. Felts, Christopher J. Brassard, ACS medicinal chemistry letters . 2017,第9期

机译：基于截短吡啶胺核心的改进效力和CNS渗透的MGLU _{2 Nams的设计与合成}
2. Continued optimization of the M-5 NAM ML375: Discovery of VU6008667,, an M5 NAM with high CNS penetration and a desired short half-life in rat for addiction studies [J] . McGowan Kevin M., Nance Abkellie D., Cho Hykeyung P., Bioorganic and Medicinal Chemistry Letters . 2017,第6期

机译：持续优化M-5 NAM ML375：Vu6008667的发现，M5 Nam，具有高CNS渗透的M5 NAM和大鼠中所需的短半衰期进行成瘾研究
3. Design and Synthesis of N-Aryl Phenoxyethoxy Pyridinones as Highly Selective and CNS Penetrant mGlu₃ NAMs [J] . Julie L. Engers, Katrina A. Bollinger, Rebecca L. Weiner, ACS medicinal chemistry letters . 2017,第9期

机译：N - 亚芳基苯氧氧基吡啶酮的设计和合成作为高度选择性和CNS渗透MGLU _{3 Nams}
4. Design, Synthesis and Structure Characterization of Novel Peptide Template to Probe Melanocortln Receptors Selectivity and Potency [C] . Anamika Singh, Marvin Dirain, Arthur S. Edison American Peptide Symposium . 2011

机译：新型肽模板的设计，合成及结构表征探针黑素灭菌器受体选择性和效力
5. Synthesis and characterization of bivalent P-glycoprotein inhibitors to enhance brain penetration of CNS therapies [D] . Emmert, Dana Marie 2011

机译：二价P-糖蛋白抑制剂的合成与表征，以增强中枢神经系统疗法的大脑渗透能力
6. Continued optimization of the M5 NAM ML375: Discovery of VU6008667 an M5 NAM with high CNS penetration and a desired short half-life in rat for addiction studies [O] . Kevin M. McGowan, Kellie D. Nance, Hykeyung P. Cho, -1

机译：M5 NAM ML375的持续优化：发现VU6008667这是一种具有高CNS渗透性并且在成瘾研究中所需的半衰期短的M5 NAM
7. Continued optimization of the M 5 NAM ML375: Discovery of VU6008667, an M 5 NAM with high CNS penetration and a desired short half-life in rat for addiction studies [O] . Kevin M. McGowan, Kellie D. Nance, Hykeyung P. Cho, 2017

机译：持续优化M 5 NAM ML375：VU6008667的发现，一个高CNS渗透和大鼠中所需的短半衰期，对成瘾研究

Design and Synthesis of mGlu2 NAMs withImproved Potency and CNS Penetration Based on a Truncated PicolinamideCore

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