2007
DOI: 10.1074/jbc.m702328200
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Carboxyl-terminal Proteolytic Processing of CUX1 by a Caspase Enables Transcriptional Activation in Proliferating Cells

Abstract: Proteolytic processing at the end of the G 1 phase generates a CUX1 isoform, p110, which functions either as a transcriptional activator or repressor and can accelerate entry into S phase. Here we describe a second proteolytic event that generates an isoform lacking two active repression domains in the COOH terminus. This processing event was inhibited by treatment of cells with synthetic and natural caspase inhibitors. In vitro, several caspases generated a processed isoform that co-migrated with the in vivo … Show more

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Cited by 43 publications
(55 citation statements)
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“…Multiple CUX1 isoforms have been described, two of which are ubiquitously expressed 2,22,[24][25][26][27] (reviewed in REF. 28).…”
Section: Molecular and Cellular Functions Of Cux1mentioning
confidence: 99%
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“…Multiple CUX1 isoforms have been described, two of which are ubiquitously expressed 2,22,[24][25][26][27] (reviewed in REF. 28).…”
Section: Molecular and Cellular Functions Of Cux1mentioning
confidence: 99%
“…Using transcription and cellbased assays, a role for p110 CUX1 was shown in many cellular processes, notably in cell cycle progression and cell proliferation 21,22 , strengthening of the spindle assembly checkpoint 19 , establishment of a transcriptional programme that enables efficient DNA damage responses 23 , and cell migration and invasion 13,42 . In addition, from RNA interference (RNAi)-mediated knockdown and genetic inactivation, CUX1 was shown to be required for the resistance to apoptotic signals in pancreatic cancer cells 14 , the repression cytokine genes associated with M1 macrophages 43 , and dendrite branching and spine development in cortical neurons 34 .…”
Section: The Knudson Two-hit Modelmentioning
confidence: 99%
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