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Echinacea in infection.

机译:紫锥菊感染。

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摘要

Ongoing studies have developed strategies for identifying key bioactive compounds and chemical profiles in Echinacea with the goal of improving its human health benefits. Antiviral and antiinflammatory-antipain assays have targeted various classes of chemicals responsible for these activities. Analysis of polar fractions of E. purpurea extracts showed the presence of antiviral activity, with evidence suggesting that polyphenolic compounds other than the known HIV inhibitor, cichoric acid, may be involved. Antiinflammatory activity differed by species, with E. sanguinea having the greatest activity and E. angustifolia, E. pallida, and E. simulata having somewhat less. Fractionation and studies with pure compounds indicate that this activity is explained, at least in part, by the alkamide constituents. Ethanol extracts from Echinacea roots had potent activity as novel agonists of TRPV1, a mammalian pain receptor reported as an integrator of inflammatory pain and hyperalgesia and a prime therapeutic target for analgesic and antiinflammatory drugs. One fraction from E. purpurea ethanol extract was bioactive in this system. Interestingly, the antiinflammatory compounds identified to inhibit prostaglandin E(2) production differed from those involved in TRPV1 receptor activation.
机译:正在进行的研究已经制定了识别紫锥菊中关键生物活性化合物和化学特征的策略,目的是改善其对人类健康的益处。抗病毒和抗炎-抗疼痛测定针对的是负责这些活动的各种类别的化学物质。对紫花大肠杆菌提取物极性组分的分析显示存在抗病毒活性,有证据表明,除了已知的HIV抑制剂菊花酸之外,还可能涉及多酚化合物。抗炎活性因物种而异,其中血叶大肠杆菌的活性最大,而大叶大肠杆菌、苍白大肠杆菌和拟桉大肠杆菌的活性稍低。纯化合物的分馏和研究表明,这种活性至少部分地由碱酰胺成分解释。紫锥菊根的乙醇提取物作为 TRPV1 的新型激动剂具有强大的活性,TRPV1 是一种哺乳动物疼痛受体,据报道是炎症性疼痛和痛觉过敏的整合剂,也是镇痛和抗炎药的主要治疗靶点。来自紫花大肠杆菌乙醇提取物的一种馏分在该系统中具有生物活性。有趣的是,被鉴定出抑制前列腺素E(2)产生的抗炎化合物与参与TRPV1受体激活的抗炎化合物不同。

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