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Absolute Bioavailability, Tissue Distribution, and Excretion of Erinacine S in Hericium erinaceus Mycelia

机译:猴头菇菌丝体中灵芝碱S的绝对生物利用度,组织分布和排泄

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Erinacine S, so far known to have been produced only in Hericium erinaceus mycelia, has just recently been discovered and is able to reduce amyloid plaque growth and improve neurogenesis in aged brain of rats. However, few investigations have been conducted on the absorption, distribution, and excretion study of Erinacine S. This study aimed to investigate the absolute bioavailability, tissue distribution, and excretion of Erinacine S in H. Erinaceus mycelia in eight-week old Sprague-Dawley rats. After oral administration and intravenous administration of 2.395 g/kg body weight of the H. erinaceus mycelia extract (equivalent to 50 mg/kg body weight Erinacine S) and 5 mg/kg of Erinacine S, respectively, the absolute bioavailability was estimated as 15.13%. In addition, Erinacine S was extensively distributed in organs such as brain, heart, lung, liver, kidney, stomach, small intestine, and large intestine. The maximum concentration of Erinacine S was observed in the stomach, 2 h after the oral administration of H. erinaceus mycelia extract, whereas the maximum amount of Erinacine S found in other tissues were seen after 8 h. Total amount of unconverted Erinacine S eliminated in feces and urine in 24 h was 0.1% of the oral dosage administrated. This study is the first to show that Erinacine S can penetrate the blood–brain barrier of rats and thus support the development of H. erinaceus mycelia, for the treatment of neurological diseases.
机译:迄今为止,已知仅在猴头菇菌丝体中产生的Erinacine S最近才被发现,它能够减少淀粉样蛋白斑块的生长并改善大鼠衰老脑中的神经发生。但是,很少有关于Erinacine S的吸收,分布和排泄研究的研究。该研究旨在调查八周大的Sprague-Dawley的H. Erinaceus菌丝体中Erinacine S的绝对生物利用度,组织分布和排泄。大鼠。口服和静脉内注射2.395 g / kg体重的猴头菌菌丝体提取物(相当于50 mg / kg体重的Erinacine S)和5 mg / kg的Erinacine S后,绝对生物利用度估计为15.13 %。此外,Erinacine S广泛分布于脑,心脏,肺,肝,肾,胃,小肠和大肠等器官。口服猴头菌菌丝体提取物2小时后,在胃中观察到最大的Erinacine S浓度,而8小时后在其他组织中发现了最大量的ErinacineS。在24小时内从粪便和尿液中消除的未转化的Erinacine S总量为口服剂量的0.1%。这项研究是第一个表明Erinacine S可以穿透大鼠的血脑屏障,从而支持erinaceus菌丝体的发展,从而治疗神经系统疾病的研究。

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