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卡拉胶在小鼠体内的药代动力学、组织分布和亚急性毒性。

Pharmacokinetics, tissue distribution, and subacute toxicity of oral carrageenan in mice.

机构信息

College of Pharmaceutical Science, Soochow University, Suzhou 215123, PR China.

College of Pharmaceutical Science, Soochow University, Suzhou 215123, PR China.

出版信息

Int J Biol Macromol. 2024 May;266(Pt 1):130725. doi: 10.1016/j.ijbiomac.2024.130725. Epub 2024 Mar 14.

DOI:10.1016/j.ijbiomac.2024.130725
PMID:38490394
Abstract

Carrageenan (CGN) is a typical sulfated polysaccharide widely applied in the food and pharmaceutical industries. Its in vivo behavior plays vital roles in understanding structural and biological functional relationships. The lack of UV chromophores in highly sulfated polysaccharides presents a challenge for their in vivo behavior studies. Therefore, this study aimed to develop a fast and effective quantitative fluorescence method for investigating the pharmacokinetics and tissue distribution of CGN. Fluorescence isothiocyanate labeling of CGN (FCGN) and microplate reader-based measurements were developed and validated to study its pharmacokinetics. These results showed that the FCGN concentration peaked at 3 h, the mean residence time was 36.6 h, and the clearance rate was 0.1 L/h/kg. Most of the FCGN was excreted in the feces, while 9.2 % was excreted in the urine, suggesting absorption and metabolism. The pharmacokinetic parameters indicated that the FCGN was absorbed quickly, eliminated slowly, and could remain in the body for a sustained profile. Moreover, ex vivo imaging and quantification of FCGN in tissues revealed that FCGN accumulated in the liver and kidney. Furthermore, oral administration of CGN or KOs for 14 days led to changes in liver and kidney indices. Histological analysis of significant organs revealed hepatocyte necrosis in the liver, renal tubular vacuolization in the kidney, and incomplete colonic epithelial cells. The KOs had a more significant effect on inflammatory cell infiltration than did CGNs. These in vivo findings laid the foundation for the study and application of CGN in food and pharmaceutical applications.

摘要

卡拉胶(CGN)是一种典型的硫酸化多糖,广泛应用于食品和制药行业。其体内行为在理解结构和生物功能关系方面起着至关重要的作用。高度硫酸化多糖缺乏紫外发色团,这给其体内行为研究带来了挑战。因此,本研究旨在开发一种快速有效的定量荧光法来研究 CGN 的药代动力学和组织分布。开发并验证了 CGN 的荧光异硫氰酸酯标记(FCGN)和微孔板读数测量方法,以研究其药代动力学。结果表明,FCGN 浓度在 3 小时时达到峰值,平均驻留时间为 36.6 小时,清除率为 0.1 L/h/kg。大部分 FCGN 从粪便中排出,而 9.2%从尿液中排出,表明吸收和代谢。药代动力学参数表明,FCGN 吸收迅速,消除缓慢,在体内能持续存在。此外,FCGN 在组织中的离体成像和定量分析表明,FCGN 在肝脏和肾脏中积累。此外,连续口服 CGN 或 KOs 14 天导致肝脏和肾脏指数发生变化。对重要器官的组织学分析显示,肝脏中有肝细胞坏死,肾脏中有肾小管空泡化,结肠上皮细胞不完全。KOs 对炎性细胞浸润的影响比 CGNs 更为显著。这些体内发现为 CGN 在食品和制药应用中的研究和应用奠定了基础。

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