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使用胰岛素样生长因子结合蛋白-2 增强的间充质细胞共培养物,在免疫缺陷小鼠中进行体外扩增和未扩增脐带血细胞的共移植。

Cotransplantation of ex vivo expanded and unexpanded cord blood units in immunodeficient mice using insulin growth factor binding protein-2-augmented mesenchymal cell cocultures.

机构信息

Cancer and Stem Cell Biology Program, Duke-National University of Singapore Graduate Medical School, Singapore.

出版信息

Biol Blood Marrow Transplant. 2012 May;18(5):674-82. doi: 10.1016/j.bbmt.2012.01.001. Epub 2012 Jan 9.

Abstract

Ex vivo expansion of cord blood (CB) hematopoietic stem cells and cotransplantation of 2 CB units (CBUs) could enhance the applicability of CB transplantation in adult patients. We report an immunodeficient mouse model for cotransplantation of ex vivo expanded and unexpanded human CB, showing enhanced CB engraftment and provide proof of concept for this transplantation strategy as a means of overcoming the limiting cell numbers in each CBU. CBUs were expanded in serum-free medium supplemented with stem cell factor, Flt-3 ligand, thrombopoietin, and insulin growth factor binding protein-2 together with mesenchymal stromal cell coculture. Unexpanded and expanded CB cells were cotransplanted by tail vein injection into 45 sublethally irradiated nonobese diabetic SCID-IL2γ(-/-) (NSG) mice. Submandibular bleeding was performed monthly, and mice were sacrificed 4 months after transplantation to analyze for human hematopoietic engraftment. Expansion of non-CD34(+) selected CB cells yielded 40-fold expansion of CD34(+) cells and 3.1-fold expansion of hematopoietic stem cells based on limiting dilution analysis of NSG engraftment. Mice receiving expanded grafts exhibited 4.30% human cell repopulation, compared with 0.92% in mice receiving only unexpanded grafts at equivalent starting cell doses, even though the unexpanded graft predominated in long-term hematopoiesis (P = .07). Ex vivo expanded grafts with lower initiating cell doses also showed equivalent engraftment to unexpanded grafts with higher cell dose (8.0% versus 7.9%; P = .93). In conclusion, ex vivo expansion resulted in enhanced CB engraftment despite eventual rejection by the unexpanded CBU.

摘要

体外扩增脐血(CB)造血干细胞并共移植 2 个 CB 单位(CBU)可以增强 CB 移植在成年患者中的适用性。我们报告了一个免疫缺陷小鼠模型,用于共移植体外扩增和未扩增的人 CB,显示出增强的 CB 植入,并为这种移植策略提供了概念验证,作为克服每个 CBU 中细胞数量限制的一种手段。CBU 在无血清培养基中扩增,补充有干细胞因子、Flt-3 配体、血小板生成素和胰岛素生长因子结合蛋白-2,并与间充质基质细胞共培养。未扩增和扩增的 CB 细胞通过尾静脉注射共移植到 45 只亚致死剂量照射的非肥胖糖尿病 SCID-IL2γ(-/-)(NSG)小鼠中。每月进行下颌下出血,移植后 4 个月处死小鼠,分析人造血植入情况。非-CD34(+)选择的 CB 细胞扩增产生了 CD34(+)细胞的 40 倍扩增和基于 NSG 植入的造血干细胞的 3.1 倍扩增。与仅接受未扩增移植物的小鼠(0.92%)相比,接受扩增移植物的小鼠表现出 4.30%的人细胞再群体,即使未扩增移植物在长期造血中占主导地位(P=0.07)。即使起始细胞剂量较低的扩增移植物也显示出与起始细胞剂量较高的未扩增移植物相当的植入(8.0%与 7.9%;P=0.93)。总之,尽管未扩增的 CBU 最终被排斥,但体外扩增导致 CB 植入增强。

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