Synthesis and structure-activity relationships of N-aryl-piperidine derivatives as potent (partial) agonists for human histamine H3 receptor.

Ishikawa M; Furuuchi T; Yamauchi M; Yokoyama F; Kakui N; Sato Y

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Synthesis and structure-activity relationships of N-aryl-piperidine derivatives as potent (partial) agonists for human histamine H3 receptor.

机译：N-芳基-哌啶衍生物作为人组胺H3受体的强效（部分）激动剂的合成及其构效关系。

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4-((1H-imidazol-4-yl)methyl)-1-aryl-piperazine and piperidine derivatives were designed and synthesized as candidate human histamine type 3 agonists. The piperazine derivatives were found to have low (or no) affinity for human histamine H3 receptor, whereas the piperidine derivatives showed moderate to high affinity, and their agonistic activity was greatly influenced by substituents on the aromatic ring. Among the piperidine-containing compounds, 17d and 17h were potent human histamine H3 receptor agonists with high selectivity over the closely related human H4 receptor. Our results indicate that appropriate conformational restriction, that is, by the piperidine spacer moiety, favors specific binding to the human histamine H3 receptor.

机译：设计并合成了4-（（1H-咪唑-4-基）甲基）-1-芳基-哌嗪和哌啶衍生物，作为候选的人类组胺3型激动剂。发现哌嗪衍生物对人组胺H3受体具有低（或没有）亲和力，而哌啶衍生物显示出中等至高亲和力，并且它们的激动活性受芳环上的取代基的影响很大。在含哌啶的化合物中，17d和17h是强效的人类组胺H3受体激动剂，对密切相关的人类H4受体具有高选择性。我们的结果表明适当的构象限制，即通过哌啶间隔子部分，有利于与人组胺H3受体的特异性结合。

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《Bioorganic and medicinal chemistry》 |2010年第14期|共8页
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Ishikawa M; Furuuchi T; Yamauchi M; Yokoyama F; Kakui N; Sato Y;
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1. Synthesis and structure-activity relationships of N-aryl-piperidine derivatives as potent (partial) agonists for human histamine H3 receptor. [J] . Ishikawa M, Furuuchi T, Yamauchi M, Bioorganic and medicinal chemistry . 2010,第14期

机译：N-芳基-哌啶衍生物作为人组胺H3受体的强效（部分）激动剂的合成及其构效关系。
2. 2D Quantitative Structure Activity Relationship Studies on Structurally Constrained Quinazoline Derivatives as Potent and Selective Histamine H3 Receptor Inverse Agonists [J] . Mahaveer Singh, Sunny Kumar Asian Journal of Chemistry: An International Quarterly Research Journal of Chemistry . 2012,第5期

机译：结构受限的喹唑啉衍生物作为强效和选择性组胺H3受体反向激动剂的二维定量结构活性关系研究
3. Ring-substituted histaprodifen analogues as partial agonists for histamine H(1) receptors: synthesis and structure-activity relationships. [J] . Elz S, Kramer K, Leschke C, European Journal of Medicinal Chemistry: Chimie Therapeutique . 2000,第1期

机译：作为组胺H（1）受体的部分激动剂的环取代的histaprodifen类似物：合成和结构活性关系。
4. Synthesis and Structure-Activity Relationship Studies of Cryptophycins: A Novel Class of Potent Antimitotic Antitumor Depsipeptides [C] . Chuan Shih, Rima S. Al-Awar, Andrew H. Fray, American Chemical Society . 2001

机译：Cryptophycins的合成与结构 - 活性关系研究：一种新型抗氨基型抗溶解症Depsipip肽
5. Synthesis of new glutamate receptor probes: I. Total synthesis of dysiherbaine, a potent glutamate receptor excitotoxin; II. Design and synthesis of dysiherbaine analogues; III. Synthesis and structure-activity relationships of substituted benzothiadiazides and their role as AMPA receptor modulators. [D] . Phillips, Dean Paul. 2001

机译：新型谷氨酸受体探针的合成：I. dysiherbaine的全合成，一种有效的谷氨酸受体兴奋性毒素；二。 dysiherbaine类似物的设计和合成；三，取代的苯并噻二叠氮化物的合成及其构效关系及其作为AMPA受体调节剂的作用。
6. Compared pharmacology of human histamine H3 and H4 receptors: structure–activity relationships of histamine derivatives [O] . Florence Gbahou, Ludwig Vincent, Marie Humbert-Claude, 2006

机译：人类组胺H3和H4受体的药理比较：组胺衍生物的结构-活性关系
7. Synthesis and Structure-Activity Relationships of Conformationally Constrained Histamine H3 Receptor Agonists. [O] . Kitbunnadaj, R., Zuiderveld, O.P., Esch, I.J.P.D., 2003

机译：构象约束的组胺H3受体激动剂的合成和构效关系。

Synthesis and structure-activity relationships of N-aryl-piperidine derivatives as potent (partial) agonists for human histamine H3 receptor.

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