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临床认可的款冬属杂种植物提取物 Ze 339 对涉及组胺处理的肠道机制的影响。

Impact of the clinically approved Petasites hybridus extract Ze 339 on intestinal mechanisms involved in the handling of histamine.

机构信息

Biopharmacy, Department of Pharmaceutical Sciences, University of Basel, Basel, Switzerland.

Max Zeller & Söhne AG, Medical Department, Seeblickstrasse 4, 8590 Romanshorn, Switzerland.

出版信息

Biomed Pharmacother. 2022 Apr;148:112698. doi: 10.1016/j.biopha.2022.112698. Epub 2022 Feb 8.

DOI:10.1016/j.biopha.2022.112698
PMID:35149385
Abstract

In patients with histamine intolerance accumulated or ingested histamine causes a broad range of undesirable symptoms. Food-derived histamine is degraded by intestinal diamine oxidase (DAO) and histamine-N-methyltransferase (HNMT), while the organic cation transporter 3 (OCT3) contributes to the transcellular flux of histamine. Anecdotal evidence from patients with HIT suggests an improvement of symptoms related to histamine intolerance after intake of Ze 339, a lipophilic CO-extract prepared from the leaves of Petasites hybridus. Thus, it was the aim of this study to investigate the influence of Ze 339 on DAO, HNMT and OCT3 using Caco-2 and MDCKII cells. Even though Ze 339 reduced mRNA levels of HNMT and DAO, there was no change in protein expression. Ze 339 changed neither the basal release nor the enzymatic activity of DAO. Testing the interaction of Ze 339 with the transcellular histamine transport, we observed a significant increase in the basal to apical flux in presence of high Ze 339 concentrations at the early phases of the experiment. Testing the influence of Ze 339 on OCT3-mediated histamine uptake in overexpressing MDCKII cells revealed a dose-dependent inhibition with an estimated IC of 26.9 ug/mL for the extract. In conclusion, we report an effect of Ze 339 on transcellular histamine transport, where inhibition of OCT3 may contribute.

摘要

在组胺不耐受患者中,积累或摄入的组胺会引起广泛的不适症状。食物来源的组胺被肠道二胺氧化酶(DAO)和组氨酸-N-甲基转移酶(HNMT)降解,而有机阳离子转运蛋白 3(OCT3)有助于组胺的跨细胞转运。来自组胺不耐受患者的轶事证据表明,摄入从杂种千里光叶中提取的亲脂性 CO 提取物 Ze 339 后,与组胺不耐受相关的症状得到改善。因此,本研究旨在使用 Caco-2 和 MDCKII 细胞研究 Ze 339 对 DAO、HNMT 和 OCT3 的影响。尽管 Ze 339 降低了 HNMT 和 DAO 的 mRNA 水平,但蛋白表达没有变化。Ze 339 既没有改变 DAO 的基础释放,也没有改变其酶活性。在实验早期,当 Ze 339 浓度较高时,测试 Ze 339 与跨细胞组胺转运的相互作用,我们观察到基础到顶端的通量显著增加。在过表达 MDCKII 细胞中测试 Ze 339 对 OCT3 介导的组胺摄取的影响,发现提取物对 OCT3 的抑制作用呈剂量依赖性,估计 IC 为 26.9μg/mL。总之,我们报告了 Ze 339 对跨细胞组胺转运的影响,其中 OCT3 的抑制可能起作用。

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