2003
DOI: 10.1093/nar/gkg827
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ssDNA-dependent colocalization of adeno-associated virus Rep and herpes simplex virus ICP8 in nuclear replication domains

Abstract: The subnuclear distribution of replication complex proteins is being recognized as an important factor for the control of DNA replication. Herpes simplex virus (HSV) single-strand (ss)DNA-binding protein, ICP8 (infected cell protein 8) accumulates in nuclear replication domains. ICP8 also serves as helper function for the replication of adeno-associated virus (AAV). Using quantitative 3D colocalization analysis we show that upon coinfection of AAV and HSV the AAV replication protein Rep and ICP8 co-reside in H… Show more

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Cited by 26 publications
(48 citation statements)
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“…To confirm the finding from the IP experiments, 3D deconvolution fluorescence microscopy with quantitative colocalization was carried out with WT1 and the HA-tagged hnRNP-U constructs (Heilbronn et al, 2003). Acquisition of the Z-axis stacks (0.2 mcm) of the images in either fluorescence channel was performed followed by Imaris-Colocalization quantitative analysis.…”
Section: Antibody (C Es Cells; D M15 Cells) (E)mentioning
confidence: 89%
“…To confirm the finding from the IP experiments, 3D deconvolution fluorescence microscopy with quantitative colocalization was carried out with WT1 and the HA-tagged hnRNP-U constructs (Heilbronn et al, 2003). Acquisition of the Z-axis stacks (0.2 mcm) of the images in either fluorescence channel was performed followed by Imaris-Colocalization quantitative analysis.…”
Section: Antibody (C Es Cells; D M15 Cells) (E)mentioning
confidence: 89%
“…In analogy to the HSV-1 ori-binding protein UL9 [146], Rep probably triggers the assembly of the replication machinery by binding to the RBSs within the AAV-2 oris. In the next step, Rep68 and Rep78 are thought to recruit ICP8 through a direct protein-protein interaction, which in turn stimulates Rep DNA-binding and nicking activity [147,148]. The Rep68/78-ICP8 complex is then thought to recruit the helicase-primase complex, as well as the DNA polymerase holoenzyme.…”
Section: Hsv-1-based Gene Therapy Vectorsmentioning
confidence: 99%
“…Among the HSV-1 replication factors involved in AAV-2 replication, ICP8 can certainly be considered a key helper factor, since its presence is crucial to processive AAV-2 DNA replication. The function of ICP8 presumably lies in its ability to stabilize ssDNA and to hold the replication fork in an extended conformation [149], as well as in its ability to act as a scaffolding protein for the recruitment of the helicase-primase complex and the polymerase holoenzyme [90,147]. Consistent with a key role in the helper activity, the mere addition of purified ICP8 to extracts from uninfected HeLa cells is sufficient to support in vitro AAV-2 DNA replication [148].…”
Section: Hsv-1-based Gene Therapy Vectorsmentioning
confidence: 99%
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