Di Cao, Zhengjiao Wang, Xiuting Shen, Xiaojun Song, Zhongxiang Zhao
{"title":"异外皂苷A1在正常及抗生素治疗大鼠体内代谢及药代动力学研究","authors":"Di Cao, Zhengjiao Wang, Xiuting Shen, Xiaojun Song, Zhongxiang Zhao","doi":"10.1177/09731296231198608","DOIUrl":null,"url":null,"abstract":"Background Ilexsaponin A 1 (IA 1 ) is a bioactive triterpene saponin derived from natural medicinal plants. IA 1 exhibits anti-inflammatory and proangiogenic activities and improves intestinal barrier function. It has been reported that IA 1 could be metabolized into a dominant metabolite, ilexgenin A (IA) by β-glucosidase enzymes in intestinal microflora. Materials and Methods Herein, an accurate, sensitive, and selective method based on ultra-performance liquid chromatography coupled with mass spectrometry was established to simultaneously profile the metabolism and pharmacokinetic behaviors of IA 1 in normal and antibiotic-treated rat plasma after intragastric administration of IA 1 . The precursor-to-product ion pairs of IA and IA 1 were m/ z 501.32↓439.32 and m/ z 663.38↓501.32, respectively. For method validation, the specificity, matrix effect, accuracy, precision, and stability of the pharmacokinetic study were measured, and a calibration curve was created. The collaborative pharmacological target pathways of IA 1 and its metabolite IA were investigated using network pharmacology tools. Results The validated analytical method was successfully utilized to investigate the pharmacokinetics of IA 1 in normal and antibiotic-treated rats. The bioavailability of IA 1 and conversion from IA 1 to IA were significantly inhibited by antibiotic-treated rats after oral administration of IA 1 . Fragment ions at m/z 483.3155, 455.3159, 439.3233, 421.3136, 395.3362, 152.9952, 113.0256, and 71.0531 were characteristic of the IA 1 moiety. IA 1 was metabolized in rat plasma by biotransformation routes involving deglycosylation, decarboxylation, isomerization, hydrogenation, dehydrogenation, and oxidation. Considering database analysis, IA and IA 1 play synergistic role in common pharmacological pathways, such as hypertrophic cardiomyopathy and dilated cardiomyopathy. Conclusion The experiments illustrated that β-glucosidase activity inhibited by antibiotics suppressed the hydrolysis reaction of IA 1 in the intestinal tract. IA 1 and IA play a synergistic role in exerting effects.","PeriodicalId":19895,"journal":{"name":"Pharmacognosy Magazine","volume":"137 2","pages":"0"},"PeriodicalIF":0.6000,"publicationDate":"2023-10-31","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Metabolic and Pharmacokinetic Investigation of Ilexsaponin A<sub>1</sub> in Normal and Antibiotic-treated Rats\",\"authors\":\"Di Cao, Zhengjiao Wang, Xiuting Shen, Xiaojun Song, Zhongxiang Zhao\",\"doi\":\"10.1177/09731296231198608\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"Background Ilexsaponin A 1 (IA 1 ) is a bioactive triterpene saponin derived from natural medicinal plants. IA 1 exhibits anti-inflammatory and proangiogenic activities and improves intestinal barrier function. It has been reported that IA 1 could be metabolized into a dominant metabolite, ilexgenin A (IA) by β-glucosidase enzymes in intestinal microflora. Materials and Methods Herein, an accurate, sensitive, and selective method based on ultra-performance liquid chromatography coupled with mass spectrometry was established to simultaneously profile the metabolism and pharmacokinetic behaviors of IA 1 in normal and antibiotic-treated rat plasma after intragastric administration of IA 1 . The precursor-to-product ion pairs of IA and IA 1 were m/ z 501.32↓439.32 and m/ z 663.38↓501.32, respectively. For method validation, the specificity, matrix effect, accuracy, precision, and stability of the pharmacokinetic study were measured, and a calibration curve was created. The collaborative pharmacological target pathways of IA 1 and its metabolite IA were investigated using network pharmacology tools. Results The validated analytical method was successfully utilized to investigate the pharmacokinetics of IA 1 in normal and antibiotic-treated rats. The bioavailability of IA 1 and conversion from IA 1 to IA were significantly inhibited by antibiotic-treated rats after oral administration of IA 1 . Fragment ions at m/z 483.3155, 455.3159, 439.3233, 421.3136, 395.3362, 152.9952, 113.0256, and 71.0531 were characteristic of the IA 1 moiety. IA 1 was metabolized in rat plasma by biotransformation routes involving deglycosylation, decarboxylation, isomerization, hydrogenation, dehydrogenation, and oxidation. Considering database analysis, IA and IA 1 play synergistic role in common pharmacological pathways, such as hypertrophic cardiomyopathy and dilated cardiomyopathy. Conclusion The experiments illustrated that β-glucosidase activity inhibited by antibiotics suppressed the hydrolysis reaction of IA 1 in the intestinal tract. 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引用次数: 0
摘要
Ilexsaponin a1 (ia1)是从天然药用植物中提取的具有生物活性的三萜皂苷。IA 1具有抗炎和促血管生成活性,改善肠道屏障功能。据报道,肠道菌群中的β-葡萄糖苷酶可将ia1代谢为优势代谢物ilexgenin a (IA)。材料与方法本研究建立了一种基于超高效液相色谱-质谱联用的准确、灵敏、选择性的方法,用于同时测定正常和抗生素治疗大鼠灌胃IA 1后血浆中IA 1的代谢和药代动力学行为。IA和IA 1的前驱物-产物离子对分别为m/ z 501.32↓439.32和m/ z 663.38↓501.32。为验证方法,测定了药代动力学研究的特异性、基质效应、准确度、精密度和稳定性,并建立了校准曲线。利用网络药理学工具研究了IA 1及其代谢物IA的协同药理靶点通路。结果本方法可用于正常大鼠和抗生素治疗大鼠体内IA - 1的药动学研究。经抗生素处理的大鼠口服IA 1后,IA 1的生物利用度和IA 1向IA的转化明显受到抑制。在m/z 483.3155、455.3159、439.3233、421.3136、395.3362、152.9952、113.0256和71.0531处的碎片离子是IA 1片段的特征离子。IA 1在大鼠血浆中通过生物转化途径代谢,包括去糖基化、脱羧化、异构化、氢化、脱氢和氧化。结合数据库分析,IA和IA 1在肥厚型心肌病、扩张型心肌病等常见药理通路中发挥协同作用。结论抗生素抑制β-葡萄糖苷酶活性可抑制肠道IA 1的水解反应。IA 1与IA协同发挥作用。
Metabolic and Pharmacokinetic Investigation of Ilexsaponin A1 in Normal and Antibiotic-treated Rats
Background Ilexsaponin A 1 (IA 1 ) is a bioactive triterpene saponin derived from natural medicinal plants. IA 1 exhibits anti-inflammatory and proangiogenic activities and improves intestinal barrier function. It has been reported that IA 1 could be metabolized into a dominant metabolite, ilexgenin A (IA) by β-glucosidase enzymes in intestinal microflora. Materials and Methods Herein, an accurate, sensitive, and selective method based on ultra-performance liquid chromatography coupled with mass spectrometry was established to simultaneously profile the metabolism and pharmacokinetic behaviors of IA 1 in normal and antibiotic-treated rat plasma after intragastric administration of IA 1 . The precursor-to-product ion pairs of IA and IA 1 were m/ z 501.32↓439.32 and m/ z 663.38↓501.32, respectively. For method validation, the specificity, matrix effect, accuracy, precision, and stability of the pharmacokinetic study were measured, and a calibration curve was created. The collaborative pharmacological target pathways of IA 1 and its metabolite IA were investigated using network pharmacology tools. Results The validated analytical method was successfully utilized to investigate the pharmacokinetics of IA 1 in normal and antibiotic-treated rats. The bioavailability of IA 1 and conversion from IA 1 to IA were significantly inhibited by antibiotic-treated rats after oral administration of IA 1 . Fragment ions at m/z 483.3155, 455.3159, 439.3233, 421.3136, 395.3362, 152.9952, 113.0256, and 71.0531 were characteristic of the IA 1 moiety. IA 1 was metabolized in rat plasma by biotransformation routes involving deglycosylation, decarboxylation, isomerization, hydrogenation, dehydrogenation, and oxidation. Considering database analysis, IA and IA 1 play synergistic role in common pharmacological pathways, such as hypertrophic cardiomyopathy and dilated cardiomyopathy. Conclusion The experiments illustrated that β-glucosidase activity inhibited by antibiotics suppressed the hydrolysis reaction of IA 1 in the intestinal tract. IA 1 and IA play a synergistic role in exerting effects.
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