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首页> 外文期刊>Bioorganic and medicinal chemistry >Synthesis and vasodilator effects of rutaecarpine analogues which might be involved transient receptor potential vanilloid subfamily, member 1 (TRPV1).
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Synthesis and vasodilator effects of rutaecarpine analogues which might be involved transient receptor potential vanilloid subfamily, member 1 (TRPV1).

机译:芸香果碱类似物的合成和血管舒张作用,可能涉及瞬时受体电位类香草素亚家族,成员1(TRPV1)。

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摘要

Rutaecarpine is the major alkaloid component of Wu-Chu-Yu, a well known Chinese herbal drug. It has been reported that rutaecarpine causes the vasodilator, hypotensive effects by stimulation of CGRP synthesis and release via activation of TRPV1. In present study, 23 rutaecarpine analogues were designed and synthesized. Then, the vasodilator effects of theses compounds were screened by rat aortic ring experiment. The result showed that the 14-N atom of rutaecarpine might be the key site for the activity. The 5-carbonyl might make lower contribution to the effect. And simple substitute in indole-ring or quinazoline-ring would not enhance the vasodilator effect unless in proper position with proper group. One of these compounds, 10-methylrutaecarpine, exhibited similar effect with rutaecarpine. Further functional experiments showed its vasodilator and hypotensive effect were related to the stimulation of CGRP release via activation of TRPV1. The vasodilator effects of these compounds were evaluated and the structure-activity relationship was elucidated for the first time. The results suggested a new direction of valuable TRPV1 agonist as anti-hypertensive drugs.
机译:Rutaecarpine是著名的中草药Wu-Chu-Yu的主要生物碱成分。据报道,芸香果碱通过刺激CGRP的合成引起血管舒张,降压作用,并通过激活TRPV1而释放。在本研究中,设计并合成了23种芸香菜碱类似物。然后,通过大鼠主动脉环实验筛选了这些化合物的血管舒张作用。结果表明,芸苔芸香碱的14-N原子可能是该活性的关键部位。 5-羰基可能对该作用的贡献较小。除非在适当的位置与适当的基团配合使用,否则简单地取代吲哚环或喹唑啉环不会增强血管舒张作用。这些化合物之一10-甲基rutaecarpine与rutaecarpine表现出相似的作用。进一步的功能实验表明其血管舒张作用和降压作用与通过激活TRPV1刺激CGRP释放有关。评价了这些化合物的血管舒张作用,并首次阐明了结构-活性关系。结果提示了有价值的TRPV1激动剂作为抗高血压药物的新方向。

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