2007
DOI: 10.1038/sj.cr.7310145
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Cell polarity protein Par3 complexes with DNA-PK via Ku70 and regulates DNA double-strand break repair

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Cited by 48 publications
(36 citation statements)
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“…Recently, Fang and colleagues have shown that Par-3 is also present in the nucleus and directly binds to the Ku heterodimer. This interaction is enhanced when cells are exposed to genotoxic stress (g-irradiation or the anticancer agent etoposide phosphate), and knockdown of the protein by RNAi delays the DNA repair response and significantly decreases cell survival in response to ionizing radiation (Fang et al, 2007;Lees-Miller, 2007). These data demonstrate that there is an active crosstalk between the DNA repair machinery and proteins that are traditionally considered to be cytosolic and membrane related, such as Par-3 and small GTPases of the Rho family.…”
Section: Fig 5 Rhoa Activation and Actin Stress Fiber Formation Upomentioning
confidence: 70%
“…Recently, Fang and colleagues have shown that Par-3 is also present in the nucleus and directly binds to the Ku heterodimer. This interaction is enhanced when cells are exposed to genotoxic stress (g-irradiation or the anticancer agent etoposide phosphate), and knockdown of the protein by RNAi delays the DNA repair response and significantly decreases cell survival in response to ionizing radiation (Fang et al, 2007;Lees-Miller, 2007). These data demonstrate that there is an active crosstalk between the DNA repair machinery and proteins that are traditionally considered to be cytosolic and membrane related, such as Par-3 and small GTPases of the Rho family.…”
Section: Fig 5 Rhoa Activation and Actin Stress Fiber Formation Upomentioning
confidence: 70%
“…28 We confirmed here, by confocal microscopy, that PAR-3 is expressed by hCMEC/D3 cells and partly localized at cell-cell junctions, together with ZO-1, a prototype TJ-associated protein; a proportion of PAR-3 was also detected in the cytosol and nucleus, in line with previous reports in different cell types. 29,30 We established here, by quantitative confocal microscopy analysis of Podxl and P-gp expression in individual cells, that hCMEC/D3 cells are polarized on Transwell inserts (Figure 2), as previously reported by electron microscopy monitoring of P-gp expression. 23 We further demonstrated that siRNA-mediated PAR-3 knockdown largely prevented the apicobasal-polarized expression of these proteins.…”
Section: Discussionmentioning
confidence: 98%
“…For example, apical polarity is present in S1 acini but not in RT4-2 spheroids. Interestingly, PAR3, a tight junction protein involved in apical polarity, was shown to regulate DSB repair by interacting with the Ku70-Ku80 heterodimer (also known as XRCC6-XRCC5) in the nucleus (Fang et al, 2007), and a number of other apical polarity complex proteins can influence chromatin organization (reviewed by Lelièvre, 2010). These observations suggest that both basal and apical poles of the polarity axis influence nuclear functions.…”
Section: Discussionmentioning
confidence: 99%