2003
DOI: 10.1007/978-3-662-05597-7_8
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The Structure and Function of the Adenovirus Major Late Promoter

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Cited by 36 publications
(43 citation statements)
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“…Prior to DNA replication, the MLP is active at low levels, with transcription proceeding only as far as the L3 region and mRNA production restricted to the L1-52/55K and i leader proteins (5). The specific activation of the MLP requires binding of Ad-infected cell-specific transcription factor complexes to the downstream element (DE) of the MLP (6). The Ad L4-22K protein is thought to be the minimal factor required for MLP activation, but additional components, such as IVa2, are required to obtain the maximum activation observed at late times of infection (7).…”
mentioning
confidence: 99%
“…Prior to DNA replication, the MLP is active at low levels, with transcription proceeding only as far as the L3 region and mRNA production restricted to the L1-52/55K and i leader proteins (5). The specific activation of the MLP requires binding of Ad-infected cell-specific transcription factor complexes to the downstream element (DE) of the MLP (6). The Ad L4-22K protein is thought to be the minimal factor required for MLP activation, but additional components, such as IVa2, are required to obtain the maximum activation observed at late times of infection (7).…”
mentioning
confidence: 99%
“…The IVa2 protein interacts with the L1 52/55-kDa protein (14), another viral gene product involved in the packaging process (13,15). Interestingly, the core sequences of the packaging domain are also found in the DE elements (34), transcriptional elements located downstream of the Ad major late promoter (MLP) (33). The IVa2 protein was shown to bind these sequences and transactivate the MLP (20,32).…”
mentioning
confidence: 99%
“…Because both E3 genes or fiber genes are only expressed during replication cycle after infection of adenovirus (29,30), it would be expected that the transgene can be only expressed in tumor cells if oncolytic adenovirus is applied. To fully evaluate therapeutic potential of oncolytic adenoviral vector carrying this novel expression system, we have constructed novel doublecontrolled oncolytic adenovirus, in which 6.7K/gp19K of E3 genes was replaced with potent antitumor gene mda-7/IL-24.…”
mentioning
confidence: 99%