SPLICE SITE SELECTION DOMINATES OVER POLY(A) SITE CHOICE IN RNA PRODUCTION FROM COMPLEX ADENOVIRUS TRANSCRIPTION UNITS

被引：44

作者：

ADAMI, G ^{[1
]}

NEVINS, JR ^{[1
]}

机构：

[1] ROCKEFELLER UNIV, HOWARD HUGHES MED INST, NEW YORK, NY 10021 USA

来源：

EMBO JOURNAL | 1988年 / 7卷 / 07期

关键词：

D O I：

10.1002/j.1460-2075.1988.tb03050.x

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 adenovirus late genes are organized in a complex transcription unit in which the production of multiple RNAs is controlled by specific RNA processing events. Adding to the complexity is the fact that the early E3 transcription unit is wholly contained within the late transcription unit. Within this overlapping region there are splicing events and poly(A) site choices specific to each transcription unit. Early in infection, there is near exclusive use of the E3 splice site with little L4 poly(A) site use whereas the reverse is true late in infection. Using a plasmid containing an intact E3 transcription unit, we demonstrate that the L4 poly(A) site, located in the first E3 intron, it is not used either in a mock-infected cell or a late infected cell; nor is it used if the same transcription unit is driven by the major late promoter. In addition, the nature of the poly(A) site appeared to be unimportant since the E3 poly(A) site was also not used in the intron if inserted in place of the L4 poly(A) site. Thus, splice site selection appears to dominate over poly(A) site choice. This conclusion was confirmed by the observation that deletion of either the E3 splice donor (5''ss) or the E3 splice acceptor (3''ss) allowed the use of the L4 poly(A) site. Finally, the L4 poly(A) site within the E3 intron was also used when additional sequences, including splicing signals from the L4 region and the tripartite leader, was inserted between the promoter and the E3 processing sites. It appears that splicing is the dominant event in governing production of E3/L4 RNAs.

引用

页码：2107 / 2116

页数：10

共 34 条

[1] ADENOVIRUS 5 DNA SEQUENCES PRESENT AND RNA SEQUENCES TRANSCRIBED IN TRANSFORMED HUMAN-EMBRYO KIDNEY-CELLS (HEK-AD-5 OR 293) [J].

AIELLO, L ;

GUILFOYLE, R ;

HUEBNER, K ;

WEINMANN, R .

VIROLOGY, 1979, 94 (02) :460-469

[2] CONTROLS OF RNA SPLICING AND TERMINATION IN THE MAJOR LATE ADENOVIRUS TRANSCRIPTION UNIT [J].

AKUSJARVI, G ;

PERSSON, H .

NATURE, 1981, 292 (5822) :420-426

[3] SYNTHESIS OF SECRETED AND MEMBRANE-BOUND IMMUNOGLOBULIN-MU HEAVY-CHAINS IS DIRECTED BY MESSENGER-RNAS THAT DIFFER AT THEIR 3' ENDS [J].

ALT, FW ;

BOTHWELL, ALM ;

KNAPP, M ;

SIDEN, E ;

MATHER, E ;

KOSHLAND, M ;

BALTIMORE, D .

CELL, 1980, 20 (02) :293-301

[4] TRANSIENT GENE-EXPRESSION CONTROL - EFFECTS OF TRANSFECTED DNA STABILITY AND TRANS-ACTIVATION BY VIRAL EARLY PROTEINS [J].

ALWINE, JC .

MOLECULAR AND CELLULAR BIOLOGY, 1985, 5 (05) :1034-1042

[5] CALCITONIN CALCITONIN GENE-RELATED PEPTIDE TRANSCRIPTION UNIT - TISSUE-SPECIFIC EXPRESSION INVOLVES SELECTIVE USE OF ALTERNATIVE POLYADENYLATION SITES [J].

AMARA, SG ;

EVANS, RM ;

ROSENFELD, MG .

MOLECULAR AND CELLULAR BIOLOGY, 1984, 4 (10) :2151-2160

[6] GENETIC-ANALYSIS OF MESSENGER-RNA SYNTHESIS IN ADENOVIRUS REGION-E3 AT DIFFERENT STAGES OF PRODUCTIVE INFECTION BY RNA-PROCESSING MUTANTS [J].

BHAT, BM ;

WOLD, WSM .

JOURNAL OF VIROLOGY, 1986, 60 (01) :54-63

[7] COMPLEX SPLICING PATTERNS OF RNAS FROM THE EARLY REGIONS OF ADENOVIRUS-2 [J].

CHOW, LT ;

BROKER, TR ;

LEWIS, JB .

JOURNAL OF MOLECULAR BIOLOGY, 1979, 134 (02) :265-303

[8] DNA-SEQUENCE OF THE EARLY E3 TRANSCRIPTION UNIT OF ADENOVIRUS-5 [J].

CLADARAS, C ;

WOLD, WSM .

VIROLOGY, 1985, 140 (01) :28-43

[9] TRANSCRIPTIONAL CONTROL OF THE MOUSE PREALBUMIN (TRANSTHYRETIN) GENE - BOTH PROMOTER SEQUENCES AND A DISTINCT ENHANCER ARE CELL SPECIFIC [J].

COSTA, RH ;

LAI, E ;

DARNELL, JE .

MOLECULAR AND CELLULAR BIOLOGY, 1986, 6 (12) :4697-4708

[10]

DEVEGVAR HEN, 1986, CELL, V47, P259

← 1 2 3 4 →