Title of article
Simian virus 40 as a vector: recombinant viruses expressing individual polyoma T antigens
Author/Authors
Hans Türler، نويسنده , , Consuelo Salomon، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 1998
Pages
13
From page
133
To page
145
Abstract
We constructed simian virus 40 (SV40)/polyomavirus recombinants by replacing in SV40 the T antigen coding region with polyoma early region sequences, either cDNAs encoding small, middle or large T antigen or the wild-type sequence coding all three proteins. The recombinants maintained the SV40 late region and origin of replication and were propagated in COS cells yielding recombinant virus preparations with titers of 106–107 infectious particles per milliliter. These viruses were characterized in productive infections of COS cells by analyzing early and late mRNA levels and by following synthesis of polyoma early proteins. In the absence of viral DNA replication, i.e. in infected monkey or mouse cells, expression of the polyoma T antigens was weak. Further experiments indicated that this was mostly due to high genomic instability during amplification, to lower levels of cDNA transcripts as compared to spliced mRNA, and possibly also to lower infectivity of the recombinant virions. It remains to be determined, whether these handicaps are unique to SV40/polyoma recombinants or whether SV40 is in general inadequate as a viral vector.
Keywords
Viral vector , recombination , Simian virus 40 , Polyomavirus , T antigens
Journal title
Virus Research
Serial Year
1998
Journal title
Virus Research
Record number
785091
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