Novel GlyT1 inhibitor chemotypes by scaffold hopping. Part 1: Development of a potent and CNS penetrant [3.1.0]-based lead

JonesC.K.; ShefflerD.J.; WilliamsR.; JadhavS.B.; FeltsA.S.; MorrisonR.D.; NiswenderC.M.; DanielsJ.S.; ConnP.J.; LindsleyC.W.

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Novel GlyT1 inhibitor chemotypes by scaffold hopping. Part 1: Development of a potent and CNS penetrant [3.1.0]-based lead

机译：新型GlyT1抑制剂通过支架跳跃的化学型。第1部分：开发有效的基于CNS渗透剂[3.1.0]的铅

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This Letter describes the development and SAR of a novel series of GlyT1 inhibitors derived from a scaffold hopping approach that provided a robust intellectual property position, in lieu of a traditional, expensive HTS campaign. Members within this new [3.1.0]-based series displayed excellent GlyT1 potency, selectivity, free fraction, CNS penetration and efficacy in a preclinical model of schizophrenia (prepulse inhibition).

机译：这封信描述了一系列新的GlyT1抑制剂的开发和SAR，这些抑制剂来自脚手架跳跃方法，该方法提供了可靠的知识产权地位，代替了传统的昂贵的HTS运动。这个基于[3.1.0]的新系列中的成员在精神分裂症的临床前模型（脉冲抑制）中显示出出色的GlyT1效能，选择性，游离级分，CNS渗透和功效。

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《Bioorganic and Medicinal Chemistry Letters》 |2014年第4期|共4页
作者
JonesC.K.; ShefflerD.J.; WilliamsR.; JadhavS.B.; FeltsA.S.; MorrisonR.D.; NiswenderC.M.; DanielsJ.S.; ConnP.J.; LindsleyC.W.;
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正文语种 eng
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关键词
GlyT1; Scaffold hopping; Schizophrenia; Transporter;

机译：GlyT1;脚手架跳跃;精神分裂症;转运蛋白;

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1. Novel GlyT1 inhibitor chemotypes by scaffold hopping. Part 1: Development of a potent and CNS penetrant [3.1.0]-based lead [J] . JonesC.K., ShefflerD.J., WilliamsR., Bioorganic and Medicinal Chemistry Letters . 2014,第4期

机译：新型GlyT1抑制剂通过支架跳跃的化学型。第1部分：开发有效的基于CNS渗透剂[3.1.0]的铅
2. Novel GlyT1 inhibitor chemotypes by scaffold hopping. Part 2: Development of a [3.3.0]-based series and other piperidine bioisosteres (vol 24, pg 1062, 2014) [J] . Sheffler Douglas J., Nedelcovych Michael T., Williams Richard, Bioorganic and Medicinal Chemistry Letters . 2017,第9期

机译：通过脚手架跳跃的新型Glyt1抑制剂趋化型。第2部分：开发A [3.3.0]的系列和其他哌啶生物蛋白酶（Vol 24，PG 1062,2014）
3. Novel GlyT1 inhibitor chemotypes by scaffold hopping. Part 2: Development of a [3.3.0]-based series and other piperidine bioisosteres [J] . ShefflerD.J., NedelovychM.T., WilliamsR., Bioorganic and Medicinal Chemistry Letters . 2014,第4期

机译：新型GlyT1抑制剂通过支架跳跃的化学型。第2部分：基于[3.3.0]的系列药物和其他哌啶生物等位基因的开发
4. Development and characterization of potent peptide inhibitors of p60~(C-Src) PTK using pseudosubstrate-based inhibitor design approach [C] . Jayesh R.Kamath, Ruiwu Liu, Amanda M.Enstrom, the International Peptide Symposium . 2001

机译：基于假素抑制剂设计方法的P60〜（C-SRC）PTK有效肽抑制剂的开发与表征
5. Computational ligand-based cns therapeutic design: The search for novel-scaffold norepinephrine transporter inhibitors. [D] . Chaly, Anna. 2012

机译：基于计算配体的cns治疗设计：寻找新型支架去甲肾上腺素转运蛋白抑制剂。
6. Novel GlyT1 inhibitor chemotypes by scaffold hopping. Part 1. Development of a potent and CNS penetrant 3.1.0-based lead [O] . Carrie K. Jones, Douglas J. Sheffler, Richard Williams, -1

机译：新型GlyT1抑制剂通过支架跳跃的化学型。第1部分。开发基于CNS渗透性强的3.1.0的铅
7. Novel GlyT1 inhibitor chemotypes by scaffold hopping. Part 1: Development of a potent and CNS penetrant [3.1.0]-based lead [O] . Jones, Carrie K., Sheffler, Douglas J., Williams, Richard, 2014

机译：新型GlyT1抑制剂通过支架跳跃的化学型。第1部分：开发有效的基于CNS渗透剂[3.1.0]的铅

Novel GlyT1 inhibitor chemotypes by scaffold hopping. Part 1: Development of a potent and CNS penetrant [3.1.0]-based lead

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