Synthesis of new 8(S)-HETE analogs and their biological evaluation as activators of the PPAR nuclear receptors

LiutkusM.; CaijoF.; GirardA.-L.; AyralE.; AudinotV.; BoutinJ.A.; RenardP.; CaignardD.H.; DacquetC.; KtorzaA.; MossetP.; GréeR.

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Synthesis of new 8(S)-HETE analogs and their biological evaluation as activators of the PPAR nuclear receptors

机译：新的8（S）-HETE类似物的合成及其作为PPAR核受体激活剂的生物学评估

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Structural modifications around 8-HETE (8-hydroxyeicosatetraenoic acid), a natural agonist of the PPAR (peroxisome proliferator-activated receptor) nuclear receptors have led previously to the identification of a promising analog, the quinoline S 70655. Series of novel quinoline or benzoquinoline derivatives were designed through the modification of this lead. Variations of the nature of the aromatic core and of the side chains were carried out. The SAR studies indicated the high sensitivity of the upper acid chain to modifications as well as the strong effect of the length and size of the lipophilic side chain. They afforded several new promising PPARα/γ dual agonists with a high PPARα activity in vitro.

机译：围绕8-HETE（8-羟基二十碳四烯酸）（PPAR（过氧化物酶体增殖物激活的受体）天然受体激动剂）的结构修饰先前已导致鉴定出有前途的类似物喹啉S70655。新型喹啉或苯并喹啉系列通过修改该引线设计衍生工具。进行了芳族核和侧链的性质变化。 SAR研究表明，上部酸链对修饰的高度敏感性以及亲脂性侧链的长度和大小的强烈影响。他们提供了几种新的有希望的体外具有高PPARα活性的PPARα/γ双激动剂。

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《Journal of enzyme inhibition and medicinal chemistry.》 |2010年第5期|共20页
作者
LiutkusM.; CaijoF.; GirardA.-L.; AyralE.; AudinotV.; BoutinJ.A.; RenardP.; CaignardD.H.; DacquetC.; KtorzaA.; MossetP.; GréeR.;
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正文语种 eng
中图分类酶;
关键词
3-chloro-2- quinolinecarboxaldehyde; Benzoquinoline; Dual agonists; PPARs; Quinoline;

机译：3-氯-2-喹啉甲醛;苯并喹啉;双重激动剂;PPARs;喹啉;

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专利

1. Synthesis of new 8(S)-HETE analogs and their biological evaluation as activators of the PPAR nuclear receptors [J] . LiutkusM., CaijoF., GirardA.-L., Journal of enzyme inhibition and medicinal chemistry. . 2010,第5期

机译：新的8（S）-HETE类似物的合成及其作为PPAR核受体激活剂的生物学评估
2. Synthesis of new 8( S )-HETE analogs and their biological evaluation as activators of the PPAR nuclear receptors [J] . Journal of enzyme inhibition and medicinal chemistry. . 2010,第5期

机译：新的8（溶液的模拟和它们作为PPAR核受体的活化剂的生物学评估的合成
3. Synthesis of aromatic analogs of 8(S)-HETE and their biological evaluation as activators of the PPAR nuclear receptors [J] . Caijo F, Mosset P, Gree R, European journal of organic chemistry . 2006,第9期

机译：8（S）-HETE芳香类似物的合成及其作为PPAR核受体活化剂的生物学评估
4. Synthesis and Biological Assessment of Insulin-Like Analogs with Differential Activity at the Insulin and IGF-1 Receptors [C] . Richard D. DiMarchi, Jie Han, Amy Hoffman American Peptide Symposium . 2006

机译：胰岛素和IGF-1受体差异活性的胰岛素样类似物的合成与生物学评估
5. Development of novel nicotinic receptor mediated therapeutic agents: Synthesis and biological evaluation of novel epibatidine analogs and the first total synthesis of (+/-)-anabasamine and related analogs. [D] . DiMaggio, Stassi Catherine. 2003

机译：新型烟碱样受体介导的治疗剂的开发：新型表巴替丁类似物的合成和生物学评估以及（+/-）-安巴胺和相关类似物的第一个全合成。
6. Bcl3 Interacts Cooperatively with Peroxisome Proliferator-Activated Receptor Gamma (PPARγ) Coactivator 1α To Coactivate Nuclear Receptors Estrogen-Related Receptor α and PPARα [O] . John Yang, R. Sanders Williams, Daniel P. Kelly 2009

机译：Bcl3与过氧化物酶体增殖物激活受体γ（PPARγ）共激活因子1α协同相互作用以共激活核受体雌激素相关受体α和PPARα
7. Synthesis of new 8(S)-HETE analogs and their biological evaluation as activators of the PPAR nuclear receptors. [O] . Liutkus, Mélanie, Caijo, Frédéric, Girard, Anne-Lise, 2010

机译：新的8（S）-HETE类似物的合成及其作为PPAR核受体激活剂的生物学评估。

Synthesis of new 8(S)-HETE analogs and their biological evaluation as activators of the PPAR nuclear receptors

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