The Amino-Terminal Transforming Region of Simian Virus 40 Large T and Small t Antigens Functions as a J Domain

Srinivasan, Ashok; McClellan, Amie J.; Vartikar, Jai V.; Marks, Ian M.; Cantalupo, Paul G.; Li, Yun; Whyte, Peter; Rundell, Kathleen; Brodsky, Jeffrey L.; Pipas, James M.

doi:10.1128/mcb.17.8.4761

Cited by 216 publications

(280 citation statements)

References 59 publications

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“…The K1 ± JS225 cell line expresses high levels of the protein, consistent with the fact that it contains higher levels of B-myb mRNA than the other two K1-expressing lines, indicating a direct correlation between the level of T antigen and the level of B-myb mRNA. Although dl1135 was not expressed at high levels, it was present; this is consistent with the ®ndings of others that dl1135 is expressed at around 15% of the level of wild-type T antigen (Srinivasan et al, 1997). These results raise the intriguing possibility that dl1135 T antigen can interact productively with p130 and that K1 T antigen also interacts with p130.…”

Section: Dl1135 T Antigen Interacts Productively With P130supporting

confidence: 90%

“…Dl1135 was previously found to be inactive in all transformation assays Michalovitz et al, 1987;Yaciuk et al, 1991;Symonds et al, 1993;Srinivasan et al, 1997). Our results showing that it was unable to immortalize REFs directly but could maintain the growth of tsa14 cells, suggests that some of the functions initially required to immortalize REFs may not be required once the immortal state has been established.…”

Section: Activities Dependent Upon the Amino Terminusmentioning

confidence: 58%

“…When T antigen binds these pocket proteins, they are unable to interact with, and repress the activity of, the transcription factor E2F, so E2F-dependent transcription proceeds and the cell enters the cell cycle. It has been suggested that an intact J domain is required to disrupt a pocket protein-E2F complex (Srinivasan et al, 1997;Stubdal et al, 1997;Zalvide et al, 1998), and that this function can only be supplied in cis (Stubdal et al, 1997). Others have found that the J domain can be supplied in trans (Montano et al, 1990;Porras et al, 1996), either by another T molecule, or by the homologus region from small t antigen.…”

Section: Introductionmentioning

confidence: 99%

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Different functions are required for initiation and maintenance of immortalization of rat embryo fibroblasts by SV40 large T antigen

et al. 1999

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We have used two di erent, but complementary assays to characterize functions of SV40 T antigen that are necessary for its ability to immortalize rat embryo ®broblasts. In accordance with previous work, we found that several functions were required. These include activities that map to the p53 binding domain and the amino terminal 176 amino acids which contain the J domain as well as the CR1 and CR2 domain required for binding and sequestering the RB family of pocket proteins. Moreover, we found that even though activities dependent only upon the amino terminus were su cient for immortalization they were unable to maintain it. This suggests that immortalization by these amino terminal functions requires either additional events or immortalization of a subset of cells within the heterogeneous rat embryo ®broblast population. We further found that an activity dependent upon amino acids 17 ± 27 which remove a portion of the CR1 domain and the predicted a-1 helix of the J domain was not necessary to maintain growth but was required for direct immortalization suggesting that at least one of the functions required initially was not required to maintain the immortal state. This represents the ®rst demonstration that some of the functions required for maintenance of the immortal state di er from those required for initiation of immortalization.

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Section: Dl1135 T Antigen Interacts Productively With P130supporting

confidence: 90%

Section: Activities Dependent Upon the Amino Terminusmentioning

confidence: 58%

Section: Introductionmentioning

confidence: 99%

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Different functions are required for initiation and maintenance of immortalization of rat embryo fibroblasts by SV40 large T antigen

et al. 1999

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“…SV40, JCV and BKV large T-antigens share a >70% amino-acid sequence homology and are depicted in Figure 1. All these three large T-antigens possess a J domain, the homologous of a region conserved among all cellular DnaJ/Hsp40 molecular chaperones, essential for chaperone activity and for the interaction with the DnaK homolog Hsp70/Hsc70 chaperone machinery Kelley and Georgopoulos, 1997;Srinivasan et al, 1997). Simian virus 40, JCV and BKV large T-antigen (LT-Ag) also possess the LxCxE motif, through which they physically interact with all the members of the RB family proteins (Dahiya et al, 2000), which in turn bind to the viral factors through their 'pocket' domain (Paggi et al, 1996;Helt and Galloway, 2003).…”

Section: Polyomavirus Large T-antigenmentioning

confidence: 99%

“…The N-terminal portion contains three important functional domains, namely CR1, J-domain and CR2 (Powell et al, 1999). The CR1, comprised within the J-domain (residues 1-82), is necessary for SV40 LT-Agmediated transformation capabilities (Srinivasan et al, 1997); CR2 physically contains the LxCxE motif (residues 103-107) and is thus responsible for the binding with pRb, p107 and pRb2/p130 (Zalvide and DeCaprio, 1995;Kim et al, 2001). From a functional point of view, while the LxCxE motif serves to the physical docking of SV40 LT-Ag to the RB family proteins, the J-domain results indispensable for the inactivation of the ability of each member of the pRb family to induce G1 arrest (Zalvide et al, 1998).…”

Section: Polyomavirus Large T-antigenmentioning

confidence: 99%