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Inhibition of Moloney murine leukemia virus-induced leukemia in transgenic mice expressing antisense RNA complementary to the retroviral packaging sequences.

机译:在表达与逆转录病毒包装序列互补的反义RNA的转基因小鼠中抑制莫洛尼氏鼠白血病病毒诱导的白血病。

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摘要

Recombinant plasmids pLP psi as and pCP psi as were constructed by positioning the Moloney murine leukemia virus (M-MuLV) proviral packaging (psi) sequences in reverse orientation under the transcriptional regulation of lymphotropic promoter/regulatory elements from the M-MuLV long terminal repeat or the cytomegalovirus immediate-early region. Linear fragments containing the antisense psi and the appropriate transcriptional regulatory sequences from these plasmids were introduced into the mouse germ line by zygote microinjection. The chromosomal integration, germ-line transmission, and lymphocyte-directed expression of the antisense psi RNA were confirmed. Control (nontransgenic) and transgenic mice containing either the pLP psi as or the pCP psi as sequences were infected with M-MuLV on the day of birth and assayed for signs of leukemia between 12 and 14 weeks of age with standard assay procedures. While 31% (11 of 36) of the control, nontransgenic, mice developed leukemia, none of the antisense psi transgenic mice developed any symptoms of leukemia. The pCP psi as sequences were also introduced into mouse NIH 3T3 cells and stably transformed cell lines were isolated. When infected with M-MuLV these cells were shown to produce virus devoid of packaged viral RNA.
机译:重组质粒pLP psi as和pCP psi as是通过在M-MuLV长末端重复序列的淋巴启动子/调控元件的转录调控下将莫洛尼氏鼠白血病病毒(M-MuLV)原病毒包装(psi)序列反向定位而构建的或巨细胞病毒的早期区域。通过合子显微注射将含有反义psi和来自这些质粒的适当转录调控序列的线性片段引入小鼠种系。证实了反义psi RNA的染色体整合,种系传递和淋巴细胞定向表达。含有pLP psi as或pCP psi as序列的对照(非转基因)和转基因小鼠在出生当天被M-MuLV感染,并通过标准检测程序检测了12至14周龄之间的白血病迹象。对照非转基因小鼠中有31%(36个中的11个)发生了白血病,而反义psi转基因小鼠均未出现任何白血病症状。将pCP psi作为序列也引入小鼠NIH 3T3细胞中,并分离出稳定转化的细胞系。当感染M-MuLV时,这些细胞显示出可产生无包装病毒RNA的病毒。

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  • 作者

    Han, L; Yun, J S; Wagner, T E;

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  • 年度 1991
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  • 原文格式 PDF
  • 正文语种 en
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