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人脂肪间充质干细胞在新型异种移植模型中的体内分布

In vivo distribution of human adipose-derived mesenchymal stem cells in novel xenotransplantation models.

作者信息

Meyerrose Todd E, De Ugarte Daniel A, Hofling A Alex, Herrbrich Phillip E, Cordonnier Taylor D, Shultz Leonard D, Eagon J Chris, Wirthlin Louisa, Sands Mark S, Hedrick Marc A, Nolta Jan A

机构信息

Washington University School of Medicine, Division of Oncology, Hematopoietic Development and Malignancy Section, St. Louis, Missouri 63110, USA.

出版信息

Stem Cells. 2007 Jan;25(1):220-7. doi: 10.1634/stemcells.2006-0243. Epub 2006 Sep 7.

Abstract

The potential for human adipose-derived mesenchymal stem cells (AMSC) to traffic into various tissue compartments was examined using three murine xenotransplantation models: nonobese diabetic/severe combined immunodeficient (NOD/SCID), nude/NOD/SCID, and NOD/SCID/MPSVII mice. Enhanced green fluorescent protein was introduced into purified AMSC via retroviral vectors to assist in identification of cells after transplantation. Transduced cells were administered to sublethally irradiated immune-deficient mice through i.v., intraperitoneal, or subcutaneous injection. Up to 75 days after transplantation, tissues were harvested and DNA polymerase chain reaction (PCR) was performed for specific vector sequences as well as for human Alu repeat sequences. Duplex quantitative PCR using human beta-globin and murine rapsyn primers assessed the contribution of human cells to each tissue. The use of the novel NOD/SCID/MPSVII mouse as a recipient allowed rapid identification of human cells in the murine tissues, using an enzyme reaction that was independent of surface protein expression or transduction with an exogenous transgene. For up to 75 days after transplantation, donor-derived cells were observed in multiple tissues, consistently across the various administration routes and independent of transduction parameters. Tissue localization studies showed that the primary MSC did not proliferate extensively at the sites of lodgement. We conclude that human AMSC represent a population of stem cells with a ubiquitous pattern of tissue distribution after administration. AMSC are easily obtained and highly amenable to current transduction protocols for retroviral transduction, making them an excellent avenue for cell-based therapies that involve a wide range of end tissue targets.

摘要

利用三种小鼠异种移植模型,即非肥胖糖尿病/严重联合免疫缺陷(NOD/SCID)小鼠、裸鼠/NOD/SCID小鼠和NOD/SCID/MPSVII小鼠,研究了人脂肪来源间充质干细胞(AMSC)进入各种组织区室的潜力。通过逆转录病毒载体将增强型绿色荧光蛋白导入纯化的AMSC中,以协助移植后细胞的鉴定。将转导的细胞通过静脉内、腹腔内或皮下注射给予亚致死剂量照射的免疫缺陷小鼠。移植后长达75天,收集组织并进行DNA聚合酶链反应(PCR),检测特定载体序列以及人Alu重复序列。使用人β-珠蛋白和小鼠rapsyn引物进行双重定量PCR,评估人细胞对各组织的贡献。使用新型NOD/SCID/MPSVII小鼠作为受体,通过一种独立于表面蛋白表达或外源转基因转导的酶反应,能够快速鉴定小鼠组织中的人细胞。移植后长达75天,在多种组织中均观察到供体来源的细胞,在各种给药途径中均一致,且与转导参数无关。组织定位研究表明,原发性间充质干细胞在植入部位并未广泛增殖。我们得出结论,人AMSC代表了一群干细胞,给药后具有普遍的组织分布模式。AMSC易于获取,并且高度适合当前用于逆转录病毒转导的转导方案,使其成为涉及广泛终末组织靶点的基于细胞治疗的理想途径。

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