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Murine hematopoietic reconstitution after tagging and selection of retrovirally transduced bone marrow cells

机译:逆转录病毒转导的骨髓细胞的标记和选择后的小鼠造血重建

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摘要

A major problem facing the effective treatment of patients with cancer is how to get the specific antitumor agent into every tumor cell. In this report we describe the use of a strategy that, by using retroviral vectors encoding a truncated human CD5 cDNA, allows the selection of only the infected cells, and we show the ability to obtain, before bone marrow transplantation, a population of 5-fluouraci-treated murine bone marrow cells that are 100% marked. This marked population of bone marrow cells is able to reconstitute the hematopoietic system in lethally irradiated mice, indicating that the surface marker lacks deleterious effects on the functionality of bone marrow cells. No gross abnormalities in hematopoiesis were detected in mice repopulated with CD5-expressing cells. Nevertheless, a significant proportion of the hematopoietic cells no longer expresses the surface marker CD5 in the 9-month-old recipient mice. This transcriptional inactivity of the proviral long terminal repeat (LTR) was accompanied by de novo methylation of the proviral sequences. Our results show that the use of the CD5 as a retrovirally encoded marker enables the rapid, efficient, and nontoxic selection in vitro of infected primary cells, which can entirely reconstitute the hematopoietic system in mice. These results should now greatly enhance the power of studies aimed at addressing questions such as generation of cancer-negative hematopoiesis.
机译:有效治疗癌症患者面临的主要问题是如何将特定的抗肿瘤剂引入每个肿瘤细胞。在本报告中,我们描述了一种策略的使用,该策略通过使用编码截短的人CD5 cDNA的逆转录病毒载体,仅允许选择受感染的细胞,并且我们展示了在骨髓移植之前获得5个群体的能力。经氟尿酸处理的鼠骨髓细胞100%标记。骨髓细胞的这种显着种群能够重建经致死剂量照射的小鼠中的造血系统,表明该表面标志物对骨髓细胞的功能缺乏有害作用。在再表达CD5的细胞中,未发现造血功能的明显异常。尽管如此,在9个月大的受体小鼠中,相当一部分造血细胞不再表达表面标志物CD5。原病毒长末端重复序列(LTR)的这种转录失活伴随着原病毒序列的从头甲基化。我们的研究结果表明,将CD5用作逆转录病毒编码的标记,可以在体外快速,有效和无毒地选择受感染的原代细胞,从而可以完全重建小鼠的造血系统。这些结果现在应该大大增强旨在解决诸如癌症阴性的造血功能等问题的研究能力。

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