2016
DOI: 10.1172/jci86114
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RBPJ maintains brain tumor–initiating cells through CDK9-mediated transcriptional elongation

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Cited by 58 publications
(69 citation statements)
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“…Although no stratified clinical trial to assess GSI for the treatment of proneural GBMs has been carried out, identification of the molecular mechanism of GSI resistance in GBM has the potential to help develop novel therapies for this deadly disease. In the current issue, Xie et al elegantly demonstrate that a mediator of Notch signaling, RBPJ, is overexpressed in GSI-resistant BTICs preferentially in proneural GBMs and is required for BTIC propagation both in vitro and in vivo (25). The results of this study are of substantial clinical relevance, because a mechanism of GSI resistance in BTICs has been identified, thereby providing a new approach to target GSI-resistant tumor cells in general.…”
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confidence: 65%
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“…Although no stratified clinical trial to assess GSI for the treatment of proneural GBMs has been carried out, identification of the molecular mechanism of GSI resistance in GBM has the potential to help develop novel therapies for this deadly disease. In the current issue, Xie et al elegantly demonstrate that a mediator of Notch signaling, RBPJ, is overexpressed in GSI-resistant BTICs preferentially in proneural GBMs and is required for BTIC propagation both in vitro and in vivo (25). The results of this study are of substantial clinical relevance, because a mechanism of GSI resistance in BTICs has been identified, thereby providing a new approach to target GSI-resistant tumor cells in general.…”
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confidence: 65%
“…Indeed, loss of RBPJ has been shown to induce expression of several Notch target genes, either in the presence or absence of NICD, and increase tumorigenesis in breast cancer and Burkitt lymphoma cells (37). In contrast, Xie et al show that knockdown of RBPJ only derepresses a few Notch target genes, such as HES5, but induces apoptosis in BTICs (25). One possible reason for these opposite effects from knockdown of RBPJ in tumor cells is that the breast cancer cells and Burkitt lymphoma cells used were dependent on Notch signaling to grow (37), whereas the BTICs used by Xie et al were already independent of Notch signaling for their growth (GSI-resistant cells) (Figure 1).…”
Section: 1mentioning
confidence: 99%
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