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关节腔内移植的人骨髓来源克隆间充质干细胞的药代动力学及体内转归

Pharmacokinetics and in vivo fate of intra-articularly transplanted human bone marrow-derived clonal mesenchymal stem cells.

作者信息

Shim Gayong, Lee Sangbin, Han Jeonghoon, Kim Gunwoo, Jin Hyerim, Miao Wenjun, Yi Tac-Ghee, Cho Yun Kyoung, Song Sun Uk, Oh Yu-Kyoung

机构信息

1 Research Institute of Pharmaceutical Sciences, College of Pharmacy, Seoul National University , Seoul, Republic of Korea.

出版信息

Stem Cells Dev. 2015 May 1;24(9):1124-32. doi: 10.1089/scd.2014.0240. Epub 2015 Jan 21.

DOI:10.1089/scd.2014.0240
PMID:25519508
Abstract

In this study, we report the pharmacokinetics and in vivo fate of intra-articularly transplanted human mesenchymal stem cells (MSCs) in comparison with those of intravenously administered cells. Bone marrow-derived human clonal mesenchymal stem cells (hcMSCs) were transplanted to nude mice through intravenous or intra-articular routes. The numbers of hcMSCs in blood and tissue samples were measured by the quantitative real-time-polymerase chain reaction (qPCR) with human Alu (hAlu) as a detection marker. Following intra-articular transplantation, the blood levels of hcMSCs peaked 8 h postdose and gradually diminished, showing a 95-fold higher mean residence time than hcMSCs delivered through the intravenous route. Unlike intravenously administered hcMSCs, intra-articularly injected hcMSCs were mainly retained at injection joint sites where their levels 8 h postdose were 116-fold higher than those in muscle tissues. Regardless of injection routes, biodistribution patterns did not significantly differ between normal and osteoarthritis-induced mice. Quantitative analysis using hAlu-specific qPCR revealed that hcMSC levels in joint tissues were significantly higher than those in muscle tissues 120 days postdose. These dramatic differences in kinetic behavior and fate of intra-articularly transplanted hcMSCs compared with intravenously administered hcMSCs may provide insights useful for the development of human MSCs for arthritis therapeutics.

摘要

在本研究中,我们报告了关节内移植的人间充质干细胞(MSCs)的药代动力学和体内转归,并与静脉注射细胞进行了比较。将骨髓来源的人克隆间充质干细胞(hcMSCs)通过静脉或关节内途径移植到裸鼠体内。以人Alu(hAlu)作为检测标记,通过定量实时聚合酶链反应(qPCR)测定血液和组织样本中的hcMSCs数量。关节内移植后,hcMSCs的血药浓度在给药后8小时达到峰值,随后逐渐下降,其平均驻留时间比静脉途径给药的hcMSCs高95倍。与静脉注射的hcMSCs不同,关节内注射的hcMSCs主要保留在注射关节部位,给药后8小时其水平比肌肉组织中的水平高116倍。无论注射途径如何,正常小鼠和骨关节炎诱导小鼠之间的生物分布模式没有显著差异。使用hAlu特异性qPCR进行的定量分析显示,给药后120天关节组织中的hcMSC水平显著高于肌肉组织中的水平。与静脉注射的hcMSCs相比,关节内移植的hcMSCs在动力学行为和转归上的这些显著差异可能为开发用于关节炎治疗的人MSCs提供有用的见解。

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