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干细胞因子、白细胞介素-3和白细胞介素-6促进逆转录病毒介导的基因转移至小鼠造血干细胞中。

Stem cell factor, interleukin-3, and interleukin-6 promote retroviral-mediated gene transfer into murine hematopoietic stem cells.

作者信息

Luskey B D, Rosenblatt M, Zsebo K, Williams D A

机构信息

Howard Hughes Medical Institute, Indiana University School of Medicine, Indianapolis 46202.

出版信息

Blood. 1992 Jul 15;80(2):396-402.

PMID:1378319
Abstract

The efficiency of retroviral-mediated gene transfer into hematopoietic stem cells (HSC) is dependent on the survival and self-renewal of HSC in vitro during retroviral infection. We have examined the effect of prestimulation of bone marrow with various cytokines, including the product of the Steel gene, Steel factor or stem cell factor (SCF) (the ligand for the c-kit receptor) on the efficiency of retroviral transduction of the human adenosine deaminase (hADA) cDNA into murine HSC. Bone marrow cells were prestimulated for 48 hours with hematopoietic growth factors, then cocultivated with the packaging cell line producing the ZipPGK-ADA simplified retrovirus for an additional 48 hours with continued growth factor exposure. Nonadherant cells from these cocultures were injected into lethally irradiated recipients. The content of day 12 colony-forming unit-spleen (CFU-S12) in SCF/interleukin 6 (IL-6)-prestimulated and cocultured bone marrow was more than threefold greater than that of IL-3/IL-6-prestimulated bone marrow cells. All mice receiving bone marrow cells infected with the PGK-ADA virus after prestimulation with IL-3/IL-6 or SCF/IL-6 demonstrated hADA expression in the peripheral blood after full hematopoietic reconstitution. While all recipients of IL-3/IL-6-prestimulated bone marrow expressed hADA at 4 months posttransplant, in three independent experiments examining a total of 33 mice, in most recipients of SCF/IL-6-prestimulated and infected bone marrow cells, the expression of human enzyme was higher than IL-3/IL-6 mice. Southern blot analysis of DNA from hematopoietic tissues from these same mice prepared at least 4 months posttransplantation also demonstrated a higher infection efficiency of HSC as measured by proviral integration patterns and genome copy number analysis. These results suggest that the higher level of hADA expression seen in mice receiving marrow prestimulated with SCF/IL-6 before retroviral infection is due to more efficient infection of reconstituting HSC. Other growth factor combinations were also studied; however, prestimulation with SCF/IL-6 or IL-3/IL-6 appeared optimal. Using retroviral-mediated gene transfer and viral integration patterns, Steel factor (SCF) in combination with IL-6 appears to increase the survival and self-renewal of reconstituting hematopoietic stem cells and proves useful in effecting expression of foreign genes in transplant recipients. Such pretreatment may also be useful in the application of retroviral transfer methods to human cells.

摘要

逆转录病毒介导的基因导入造血干细胞(HSC)的效率取决于逆转录病毒感染期间HSC在体外的存活和自我更新能力。我们研究了用各种细胞因子(包括Steel基因产物、Steel因子或干细胞因子(SCF),即c-kit受体的配体)对骨髓进行预刺激,对人腺苷脱氨酶(hADA)cDNA逆转录病毒转导至小鼠HSC效率的影响。用造血生长因子对骨髓细胞预刺激48小时,然后与产生ZipPGK-ADA简化逆转录病毒的包装细胞系共培养48小时,同时持续给予生长因子。将这些共培养物中的非贴壁细胞注射到接受致死性照射的受体中。SCF/白细胞介素6(IL-6)预刺激并共培养的骨髓中第12天脾集落形成单位(CFU-S12)的含量比IL-3/IL-6预刺激的骨髓细胞高出三倍多。在用IL-3/IL-6或SCF/IL-6预刺激后,所有接受感染PGK-ADA病毒的骨髓细胞的小鼠在完全造血重建后外周血中均表现出hADA表达。虽然所有接受IL-3/IL-6预刺激骨髓的受体在移植后4个月均表达hADA,但在总共33只小鼠的三项独立实验中,在大多数接受SCF/IL-6预刺激并感染骨髓细胞的受体中,人酶的表达高于IL-3/IL-6处理的小鼠。对这些相同小鼠移植后至少4个月制备的造血组织DNA进行的Southern印迹分析也表明,通过前病毒整合模式和基因组拷贝数分析测量,HSC的感染效率更高。这些结果表明,在逆转录病毒感染前接受SCF/IL-6预刺激骨髓的小鼠中观察到的hADA表达水平较高,是由于重建HSC的感染效率更高。还研究了其他生长因子组合;然而,SCF/IL-6或IL-3/IL-6预刺激似乎是最佳的。利用逆转录病毒介导的基因转移和病毒整合模式,Steel因子(SCF)与IL-6联合使用似乎可提高重建造血干细胞的存活和自我更新能力,并证明在使移植受体中外源基因表达方面是有用的。这种预处理在将逆转录病毒转移方法应用于人类细胞方面可能也有用。

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