Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
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Drug
Enzyme
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Query: UMLS:C0001486 (
Adenovirus
)
3,125
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The EIa region of an
Adenovirus
5 recombinant has been substituted by a modular gene encoding
dihydrofolate reductase
(
DHFR
). In this recombinant, the mouse
DHFR
cDNA was positioned behind sequences of the major late promoter and the complete tripartite leader. The leader sequences end in the normal 5' splice site (SS) of the third leader, so that RNA splicing joins the tripartite leader to a 3' splice site immediately upstream of the
DHFR
cDNA. At late stages of infection, high levels of
DHFR
mRNAs were synthesized. At early times in the late stage, this mRNA was efficiently translated; however, at later times translation of
DHFR
decreased probably due to poor competition with other late mRNAs. Synthesis of DHFR protein from an analogous
Adenovirus
5 recombinant containing only the first late leader was studied in parallel. Equivalent levels of
DHFR
mRNA were expressed after infection with this recombinant virus; however, the efficiency of
DHFR
translation was at least 20 fold lower than that of the
DHFR
mRNA containing the tripartite leader. This suggests that the tripartite leader sequence is important for translation in the late stage of infection. As reported previously, the Ad5 recombinant containing only the first leader vastly overexpresses polypeptide IX from a novel mRNA, formed by the splicing of the first leader in the modular
DHFR
gene to the 3' splice site in the EIb region. Cells infected with this recombinant synthesize very little normal mRNA from the EIb region. Here, we demonstrated that coinfection of 293 cells with this recombinant and wild type
Adenovirus
5 also results in decreased EIb mRNA synthesis. We propose that the overproduction of polypeptide IX suppresses mRNA expression from the EIb and IX promoter sites, probably by an autoregulation loop active during lytic growth.
...
PMID:Effect of the tripartite leader on synthesis of a non-viral protein in an adenovirus 5 recombinant. 383 74
Infection of human cells by adenovirus results in multiple alterations of host gene expression. To examine the effects of viral infection on the expression of a single gene, a line of human cells was developed which is resistant to growth in methotrexate and which contains amplified RNA and protein specific for
dihydrofolate reductase
(
DHFR
). Cytogenetic evidence indicated the presence of amplified DNA.
Adenovirus infection
of these cells caused an induction and subsequent decline in the synthesis of DHFR protein. The maximum
DHFR
induction occurred 16 to 19 h after infection and reached a level 2.5-fold greater than that observed in uninfected cells. Induction of DHFR protein synthesis was accompanied by concomitant increases in the level of steady-state
DHFR
-specific cytoplasmic RNA. The relative rate of
DHFR
mRNA production (i.e., the appearance of
DHFR
-specific mRNA sequences in the cytoplasm) also increased 2.5-fold during induction. Later in infection, the relative rate of DHFR protein synthesis declined, reaching a level below that observed in uninfected cells. This decline was accompanied by a similar decline in the steady-state levels of
DHFR
RNA and in the relative rate of synthesis of
DHFR
mRNA. These data suggest that adenovirus infection controls
DHFR
gene expression by increasing and subsequently decreasing the relative rate at which
DHFR
-specific mRNA sequences appear in the cytoplasm and enter the pool of mRNA available for translation.
...
PMID:Control of cellular gene expression during adenovirus infection: induction and shut-off of dihydrofolate reductase gene expression by adenovirus type 2. 686 43
