A STUDY OF THE DIMER FORMATION OF ROUS-SARCOMA VIRUS-RNA AND OF ITS EFFECT ON VIRAL PROTEIN-SYNTHESIS INVITRO

被引:180
|
作者
BIETH, E
GABUS, C
DARLIX, JL
机构
[1] Centre de Recherches de Biochimie, Génétique Cellulaires du CNRS, 31062 Toulouse
来源
NUCLEIC ACIDS RESEARCH | 1990年 / 18卷 / 01期
关键词
D O I
10.1093/nar/18.1.119
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
The genetic material of all retroviruses examined so far is an RNA dimer where two identical RNA subunits are joined at their 5' ends by a structure named dimer linkage structure (DLS). Since the precise location and structure of the DLS as well as the mechanism and role(s) of RNA dimerization remain unclear, we analysed the dimerization process of Rous sarcoma virus (RSV) RNA. For this purpose we set up an in vitro model for RSV RNA dimerization. Using this model RSV RNA was shown to form dimeric molecules and this dimerization process was greatly activated by nucleocapsid protein (NCp12) of RSV. Furthermore, RSV RNA dimerization was performed in the presence of complementary 5'32P-DNA oligomers in order to probe the monomer and dimer forms of RSV RNA. Data indicated that the DLS of RSV RNA probably maps between positions 544-564 from the 5'end. In an attempt to define sequences needed for the dimerization of RSV RNA, deletion mutageneses were generated in the 5' 600 nt. The results showed that the dimer promoting sequences probably are located within positions 208-270 and 400-600 from the 5' end and hence possibly encompassing the cis-acting elements needed for the specific encapsidation of RSV genomic RNA. Also it is reported that synthesis of the polyprotein precursor Pr76gag is inhibited upon dimerization of RSV RNA. These results suggest that dimerization and encapsidation of genome length RSV RNA might be linked in the course of virion formation since they appear to be under the control of the same cis elements, E and DLS, and the transacting factor nucleocapsid protein NCp12. © 1990 Oxford University Press.
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页码:119 / 127
页数:9
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