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Handicapped retroviral vectors efficiently transduce foreign genes into hematopoietic stem cells.

机译:残障的逆转录病毒载体可有效地将外源基因导入造血干细胞。

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摘要

Retroviral vectors, designated handicapped, are described. These are genetically defective viruses that allow transfer of nonselectable genes under the transcriptional control of internal promoters. The basic handicapped vector (pHHAM) is derived from Harvey, Abelson, and Moloney murine retroviruses. It contains a 327-base-pair deletion in the 3' long terminal repeat that spans enhancer and promoter sequences. The deletion is successfully transferred to the 5' long terminal repeat after reverse transcription of viral RNA, yielding a provirus incapable of synthesizing viral transcripts. HHAM viruses containing the mouse c-myc gene under the control of immunoglobulin kappa chain gene regulatory elements, along with a selectable gene (neo) driven by a weak promoter (tk), were stably transmitted to cultured mouse B cells. The donor c-myc gene was transcribed from the kappa promoter in these cells. Helper-free virus-producing cell lines were generated at titers favorable for the efficient introduction of HHAM viruses, even without selection, into hematopoietic stem cells from mouse bone marrow. When returned to unirradiated congenic recipient mice, the cells were capable of long-term reconstitution of the myeloid and lymphoid lineages of W/Wv mutants and the lymphoid system of scid mutants.
机译:描述了指定为残疾人的逆转录病毒载体。这些是遗传缺陷病毒,可在内部启动子的转录控制下转移非选择基因。基本残障载体(pHHAM)衍生自Harvey,Abelson和Moloney鼠逆转录病毒。它在跨越增强子和启动子序列的3'长末端重复序列中包含一个327个碱基对的缺失。病毒RNA逆转录后,该缺失被成功转移至5'长末端重复序列,产生了无法合成病毒转录本的原病毒。包含受免疫球蛋白κ链基因调控元件控制的小鼠c-myc基因的HHAM病毒,以及由弱启动子(tk)驱动的选择基因(neo),均稳定地传播至培养的小鼠B细胞。在这些细胞中,从κ启动子转录供体c-myc基因。产生无助剂的病毒产生细胞系,其滴度有利于将HHAM病毒有效地导入小鼠骨髓造血干细胞中,即使未经选择也是如此。当返回未经辐照的同类小鼠时,细胞能够长期重建W / Wv突变体的髓样和淋巴谱系以及scid突变体的淋巴系统。

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