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重组逆转录病毒介导的基因转移至正常造血细胞。

Recombinant retrovirus-mediated gene transfer to normal haemopoietic cells.

作者信息

Johnson G R

机构信息

Cancer Research Unit, Walter and Eliza Hall Institute of Medical Research, Royal Melbourne Hospital, Victoria, Australia.

出版信息

J Cell Sci Suppl. 1988;10:131-44. doi: 10.1242/jcs.1988.supplement_10.10.

Abstract

Several of parameters seeking to increase the infection frequency of normal haemopoietic cells by recombinant retroviruses containing a drug selectable marker and/or a haemopoietic growth factor gene have been compared. By using bone marrow cells pretreated with 5-fluorouracil, cocultivation of cells for at least 4 days with virus producing fibroblasts, and addition of pokeweed mitogen stimulated spleen cell conditioned medium, from 30 to 100% of haemopoietic spleen colony forming cells (CFU-S) could be infected. Because drug (G-418) selection was found to select subsets of CFU-S, a retrovirus lacking the drug selectable marker Neor, but containing a GM-CSF gene, was used to study the effects of endogenous GM-CSF production on CFU-S differentiation. Infected CFU-S produced equivalent numbers of erythroid and neutrophil-macrophage committed progenitor cells to control uninfected CFU-S. However, the progeny of infected CFU-S produced GM-CSF, some cells grew autonomously and neutrophil numbers were greatly increased at the expense of erythroblasts. These results suggest that unregulated GM-CSF production, although not altering commitment, alters the amplication phase following commitment.

摘要

已对若干旨在通过含有药物选择标记和/或造血生长因子基因的重组逆转录病毒提高正常造血细胞感染频率的参数进行了比较。通过使用经5-氟尿嘧啶预处理的骨髓细胞,将细胞与产生病毒的成纤维细胞共培养至少4天,并添加商陆丝裂原刺激的脾细胞条件培养基,可感染30%至100%的造血脾集落形成细胞(CFU-S)。由于发现药物(G-418)选择会选择CFU-S的亚群,因此使用一种缺乏药物选择标记Neor但含有GM-CSF基因的逆转录病毒来研究内源性GM-CSF产生对CFU-S分化的影响。感染的CFU-S产生的红系和中性粒细胞-巨噬细胞定向祖细胞数量与未感染的对照CFU-S相当。然而,感染的CFU-S的后代产生GM-CSF,一些细胞自主生长,中性粒细胞数量大幅增加,而牺牲了成红细胞。这些结果表明,不受调控的GM-CSF产生虽然不会改变定向,但会改变定向后的扩增阶段。

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