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流感病毒cDNA中的核苷酸序列异质性和序列重排

Nucleotide-sequence heterogeneity and sequence rearrangements in influenza virus cDNA.

作者信息

Fields S, Winter G

出版信息

Gene. 1981 Nov;15(2-3):207-14. doi: 10.1016/0378-1119(81)90130-x.

Abstract

Double-stranded cDNA has been synthesized from influenza virus RNA and cloned into derivatives of the bacteriophage M13 for sequence analysis. The characterization of over 200 clones has permitted an analysis both of nucleotide sequence heterogeneity and of clones containing unusual rearrangements of sequence. Heterogeneity, due to genetic variability in the RNA population and to in vitro synthetic errors, was detected at the low level of one nucleotide difference per 3 700 nucleotides. By contrast, gross sequence rearrangements were identified in eight clones. Inversions of sequence within the same cDNA molecule were the predominant type of rearrangement, and three mechanisms for producing such inversions are discussed. In addition, we observed rarer clones containing sequence from one RNA molecule joined to that from another molecule.

摘要

已从流感病毒RNA合成双链cDNA,并将其克隆到噬菌体M13的衍生物中进行序列分析。对200多个克隆的表征使得能够对核苷酸序列异质性以及包含序列异常重排的克隆进行分析。由于RNA群体中的遗传变异性和体外合成错误导致的异质性,在每3700个核苷酸中一个核苷酸差异的低水平上被检测到。相比之下,在八个克隆中鉴定出了明显的序列重排。同一cDNA分子内的序列倒位是重排的主要类型,并讨论了产生这种倒位的三种机制。此外,我们观察到更罕见的克隆,其包含来自一个RNA分子的序列与来自另一个分子的序列相连。

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