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一种在U3序列中含有多个A到G转换的禽类变异长末端重复序列的功能和生物学特性。

Functional and biological properties of an avian variant long terminal repeat containing multiple A to G conversions in the U3 sequence.

作者信息

Felder M P, Laugier D, Yatsula B, Dezélée P, Calothy G, Marx M

机构信息

Unité de Recherche Associée 1443 du Centre National de la Recherche Scientifique, Institut Curie, Centre Universitaire, Orsay, France.

出版信息

J Virol. 1994 Aug;68(8):4759-67. doi: 10.1128/JVI.68.8.4759-4767.1994.

Abstract

We previously reported that infection of chicken embryonic neuroretina cells with Rous-associated virus type 1 leads to the frequent occurrence of spliced readthrough transcripts containing viral and cellular sequences. Generation of such chimeric transcripts constitutes a very early step in oncogene transduction. We report, here, the isolation of a c-mil transducing retrovirus, designated IC4, which contains a highly mutated U3 sequence in which 48% of A is converted to G. Functional analysis of this variant U3 indicated that these mutations do not impair viral transcription and replication; however, they abolish functioning of its polyadenylation signal, thus allowing readthrough transcription of downstream cellular sequences. On the basis of these results, we designed a nonreplicative retroviral vector, pIC4Neo, expressing the neomycin resistance (Neo(r)) gene under the control of the IC4 long terminal repeat. Infection of nondividing neuroretina cells with virus produced by a packaging cell line transfected with pIC4Neo occasionally resulted in sustained cell proliferation. Two independent G418-resistant proliferating cultures were found to express hybrid RNAs containing viral and cellular sequences. These sequences were characterized by reverse transcription-PCR and were identified in both cultures, suggesting that proliferation was correlated with a common integration locus. These results indicate that IC4Neo virus functions as a useful insertional mutagen and may allow identification of genes potentially involved in regulation of cell division.

摘要

我们之前报道过,用1型劳斯相关病毒感染鸡胚神经视网膜细胞会频繁产生包含病毒和细胞序列的剪接通读转录本。此类嵌合转录本的产生是致癌基因转导的一个非常早期的步骤。我们在此报告一种c-mil转导逆转录病毒的分离,命名为IC4,它含有一个高度突变的U3序列,其中48%的A被转化为G。对这个变异U3的功能分析表明,这些突变并不损害病毒转录和复制;然而,它们消除了其聚腺苷酸化信号的功能,从而允许下游细胞序列的通读转录。基于这些结果,我们设计了一种非复制性逆转录病毒载体pIC4Neo,它在IC4长末端重复序列的控制下表达新霉素抗性(Neo(r))基因。用转染了pIC4Neo的包装细胞系产生的病毒感染非分裂神经视网膜细胞偶尔会导致细胞持续增殖。发现两个独立的G418抗性增殖培养物表达包含病毒和细胞序列的杂交RNA。通过逆转录-聚合酶链反应对这些序列进行了表征,并在两种培养物中都得到了鉴定,这表明增殖与一个共同的整合位点相关。这些结果表明,IC4Neo病毒作为一种有用的插入诱变剂发挥作用,可能有助于鉴定潜在参与细胞分裂调控的基因。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7d29/236415/88b01f168044/jvirol00017-0068-a.jpg

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