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AFT024基质细胞系支持多能人类造血祖细胞在体外长期维持植入状态。

The AFT024 stromal cell line supports long-term ex vivo maintenance of engrafting multipotent human hematopoietic progenitors.

作者信息

Nolta J A, Thiemann F T, Arakawa-Hoyt J, Dao M A, Barsky L W, Moore K A, Lemischka I R, Crooks G M

机构信息

Division of Research Immunology and Bone Marrow Transplantation, Childrens Hospital Los Angeles, Los Angeles, CA 90027, USA.

出版信息

Leukemia. 2002 Mar;16(3):352-61. doi: 10.1038/sj.leu.2402371.

Abstract

The immortalized murine stromal cell line AFT024 has been reported to maintain human hematopoietic progenitors in an undifferentiated state in vitro. In the current studies the beige/nude/xid (bnx) mouse in vivo xenograft model was used to examine the engraftment and multilineage generative potential of human hematopoietic progenitors after 2-3 weeks growth on AFT024 stroma, in comparison to primary stromal monolayers derived from post-natal human bone marrow. Eight to 12 months after transplantation of human CD34+CD38- cells from umbilical cord blood, cultured on AFT024 vs human stroma for 2-3 weeks, the murine bone marrow was harvested and analyzed for the presence of human myeloid and lymphoid cells. The mean percent engraftment of total human hematopoietic cells in the murine marrow was significantly higher after co-cultivation on AFT024 than on human stroma. Human myeloid and lymphoid lineage cells were detected in all mice. However, engraftment of myeloid lineage cells (CD33+), B lymphoid (CD19+), and T lymphoid cells (CD4+and CD8+) were significantly higher after co-cultivation of the human cells on AFT024 than on human stroma, prior to transplantation. Interestingly, the length of time in culture did not significantly affect the engraftment of the myeloid and T lymphoid lineage progenitors, but the percentage of B lymphoid lineage engraftment decreased significantly between 2 and 3 weeks of co-cultivation on both types of stroma. Cells with a primitive phenotype (CD45+/CD34-/CD38- and CD45+/CD34-/lin-) and cells with the capacity to generate secondary human CFU after recovery from the bnx bone marrow were maintained at significantly higher levels during culture on AFT024 stroma than on human stroma. The current studies demonstrate that the AFT024 murine stromal cell line supports the ex vivo survival and maintenance of human hematopoietic progenitors that are capable of long-term multilineage reconstitution for 2-3 weeks ex vivo, to levels superior to those that can be obtained using human stromal cells.

摘要

据报道,永生化小鼠基质细胞系AFT024可在体外使人类造血祖细胞维持在未分化状态。在当前研究中,使用米色/裸鼠/ xid(bnx)小鼠体内异种移植模型,来检测人类造血祖细胞在AFT024基质上生长2 - 3周后与源自出生后人骨髓的原代基质单层相比的植入情况和多谱系生成潜力。将来自脐带血的人类CD34 + CD38-细胞在AFT024或人类基质上培养2 - 3周后进行移植,8至12个月后,收获小鼠骨髓并分析其中人类髓系和淋巴系细胞的存在情况。与在人类基质上共培养相比,在AFT024上共培养后,小鼠骨髓中人类造血细胞的平均植入百分比显著更高。在所有小鼠中均检测到人类髓系和淋巴系细胞。然而,在移植前,人类细胞在AFT024上共培养后,髓系细胞(CD33 +)、B淋巴细胞(CD19 +)和T淋巴细胞(CD4 +和CD8 +)的植入明显高于在人类基质上。有趣的是,培养时间长短对髓系和T淋巴细胞系祖细胞的植入没有显著影响,但在两种基质上共培养2至3周期间,B淋巴细胞系植入的百分比显著下降。具有原始表型(CD45 + / CD34 - / CD38 -和CD45 + / CD34 - / lin -)的细胞以及从bnx骨髓恢复后能够产生次级人类集落形成单位的细胞,在AFT024基质上培养期间维持的水平明显高于在人类基质上。当前研究表明,AFT024小鼠基质细胞系支持人类造血祖细胞在体外存活和维持2 - 3周,这些祖细胞能够进行长期多谱系重建,且水平优于使用人类基质细胞所能获得的水平。

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