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在含有带启动子的外源DNA的回收逆转录病毒载体中的高频缺失。

High-frequency deletion in recovered retrovirus vectors containing exogenous DNA with promoters.

作者信息

Emerman M, Temin H M

出版信息

J Virol. 1984 Apr;50(1):42-9. doi: 10.1128/JVI.50.1.42-49.1984.

Abstract

We previously described infectious retrovirus vectors constructed from spleen necrosis virus which contain the herpes simplex virus thymidine kinase gene and the mouse alpha-globin gene (K. Shimotohno and H. M. Temin, Nature [London] 299:255-268, 1982). In the present study we report that when TK- chicken cells infected with a virus containing the mouse alpha-globin promoter and other 5' noncoding sequences in addition to the alpha-globin coding sequences were selected for thymidine kinase (TK) activity, all virus-producing TK+ cell clones shed virus with a deletion. These deletions were of different sizes and included the mouse alpha-globin coding sequences and the mouse alpha-globin transcriptional promoter. One of the deleted viruses was molecularly cloned. DNA sequencing showed that the deleted sequences are flanked by a short direct repeat. This deleted virus was also shown to have an advantage over the nondeleted parent both in multiplication and in its specific TK-transforming unit titer. In contrast to the results described above, TK+ cell clones established with viruses that contained only the coding sequences from the mouse alpha-globin gene did not delete and were stable over many cell passages. The implications of the high-frequency deletion of the viruses with internal promoters are discussed in terms of the evolution of retroviruses and the construction of retrovirus vectors.

摘要

我们之前描述了由脾坏死病毒构建的感染性逆转录病毒载体,其包含单纯疱疹病毒胸苷激酶基因和小鼠α-珠蛋白基因(K. 下户野和H. M. 特明,《自然》[伦敦]299:255 - 268, 1982)。在本研究中,我们报告称,当用一种除α-珠蛋白编码序列外还含有小鼠α-珠蛋白启动子和其他5'非编码序列的病毒感染的TK - 鸡细胞被选择用于胸苷激酶(TK)活性时,所有产生病毒的TK + 细胞克隆释放的病毒都有缺失。这些缺失大小各异,包括小鼠α-珠蛋白编码序列和小鼠α-珠蛋白转录启动子。其中一种缺失病毒被进行了分子克隆。DNA测序表明,缺失序列两侧有一个短的直接重复序列。还显示这种缺失病毒在增殖及其特定的TK转化单位滴度方面都比未缺失的亲本病毒具有优势。与上述结果相反,用仅包含小鼠α-珠蛋白基因编码序列的病毒建立的TK + 细胞克隆没有缺失,并且在许多细胞传代过程中都很稳定。从逆转录病毒的进化和逆转录病毒载体的构建方面讨论了具有内部启动子的病毒高频缺失的意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/eee3/255579/3f2ff5151b02/jvirol00133-0052-a.jpg

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