Effect of the tripartite leader on synthesis of a non-viral protein in an adenovirus 5 recombinant

doi:10.1093/nar/13.3.841

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Nucleic Acids Research, 1985, Vol. 13, No. 3 841-857
© 1985

Articles

Effect of the tripartite leader on synthesis of a non-viral protein in an adenovirus 5 recombinant

Kathleen L. Berkner⁺ and Phillip A. Sharp

Center for Cancer Research, and Department of Biology, Massachusetts Institute of Technology Cambridge, MA 02139, USA

Received October 29, 1984. Revised December 31, 1984. Accepted December 31, 1984.

The EIa region of an Adenovirus 5 recombinant has been substitutedby a modular gene encoding dihydrofolate reductase (DHFR). Inthis recombinant, the mouse DHFR cDNA was positioned behindsequences of the major late promoter and the complete tripartiteleader. The leader sequences end in the normal 5' splice site(SS) of the third leader, so that RNA splicing joins the tripartiteleader to a 3' splice site immediately upstream of the DHFRcDNA. At late stages of infection, high levels of DHFR mRNAswere synthesized. At early times in the late stage, this mRNAwas efficiently translated; however, at later times translationof DHFR decreased probably due to poor competition with otherlate mRNAs. Synthesis of DHFR protein from an analogous Adenovirus5 recombinant containing only the first late leader was studiedin parallel. Equivalent levels of DHFR mRNA were expressed afterinfection with this recombinant virus; however, the efficiencyof DHFR translation was at least 20 fold lower than that ofthe DHFR mRNA containing the tripartite leader. This suggeststhat the tripartite leader sequence is important for translationin the late stage of infection. As reported previously, theAd5 recombinant containing only the first leader vastly overexpressespolypeptlde IX from a novel mRNA, formed by the splicing ofthe first leader in the modular DHFR gene to the 3' splice sitein the EIb region. Cells infected with this recombinant synthesizevery little normal mRNA from the EIb region. Here, we demonstratedthat coinfection of 293 cells with this recombinant and wildtype Adenovirus 5 also results in decreased EIb mRNA synthesis.We propose that the overproduction of polypeptide IX suppressesmRNA expression from the EIb and IX promoter sites, probablyby an autoregulation loop active during lytic growth.

⁺Present address: Zymogenetics, 2121 North 35th Street, Seattle,WA 98103, USA

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