Cdc6 Stability Is Regulated by the Huwe1 Ubiquitin Ligase after DNA Damage

Hall, Jonathan; Kow, Evelyn; Nevis, Kathleen R.; Lu, Chiajung Karen; Luce, K. Scott; Zhong, Qing; Cook, Jeanette Gowen

doi:10.1091/mbc.e07-02-0173

Cited by 124 publications

(151 citation statements)

References 61 publications

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“…Evidence exists that Cdc6 is involved in the surveillance of the replication process during S phase via the checkpoint kinase Chk1, 28,40 and it was also shown, that Cdc6 is degraded in response to induced DNA damage during all cell cycle phases. 41 If Cdc6 plays a role in these processes it must either remain available in the cell nucleus during S phase at low levels, or it relocates to the cell nucleus in response to signals induced by stalled replication forks or extrinsic DNA damage. Future work is required to examine these aspects of Cdc6 regulation and their functional consequences.…”

Section: Discussionmentioning

confidence: 99%

Spatio-temporal regulation of the human licensing factor Cdc6 in replication and mitosis

et al. 2015

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To maintain genome stability, the thousands of replication origins of mammalian genomes must only initiate replication once per cell cycle. This is achieved by a strict temporal separation of ongoing replication in S phase, and the formation of pre-replicative complexes in the preceding G1 phase, which "licenses" each origin competent for replication. The contribution of the loading factor Cdc6 to the timing of the licensing process remained however elusive due to seemingly contradictory findings concerning stabilization, degradation and nuclear export of Cdc6. Using fluorescently tagged Cdc6 (Cdc6-YFP) expressed in living cycling cells, we demonstrate here that Cdc6-YFP is stable and chromatin-associated during mitosis and G1 phase. It undergoes rapid proteasomal degradation during S phase initiation followed by active export to the cytosol during S and G2 phases. Biochemical fractionation abolishes this nuclear exclusion, causing aberrant chromatin association of Cdc6-YFP and, likely, endogenous Cdc6, too. In addition, we demonstrate association of Cdc6 with centrosomes in late G2 and during mitosis. These results show that multiple Cdc6-regulatory mechanisms coexist but are tightly controlled in a cell cycle-specific manner.

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Section: Discussionmentioning

confidence: 99%

Spatio-temporal regulation of the human licensing factor Cdc6 in replication and mitosis

et al. 2015

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“…Mule is a HECT domain-containing ubiquitin ligase that ubiquitinates and degrades multiple cellular substrates (Adhikary et al 2005;Chen et al 2005;Hall et (Fig. 4A).…”

Section: Mule Binds and Ubiquitinates Hdac2mentioning

confidence: 99%

“…Mule was first identified as a ubiquitin ligase for an anti-apoptotic Bcl-2 family protein, Mcl-1 (Zhong et al 2005). Mule is also known as ARF-BP1, Ureb1, LASU1, HUWE1, or HectH9, and promotes ubiquitin-proteasomal degradation of multiple substrates, including p53, c-Myc, Cdc6, histones, N-Myc, Miz1, TopBP1, and Polb (Adhikary et al 2005;Chen et al 2005;Zhong et al 2005;Hall et al 2007;Liu et al 2007;Herold et al 2008;Zhao et al 2008;Parsons et al 2009;Yang et al 2010). However, whether any of these existing or unidentified substrates mediate the major function of Mule in the DNA damage response remains elusive.…”

mentioning

confidence: 99%

Mule determines the apoptotic response to HDAC inhibitors by targeted ubiquitination and destruction of HDAC2

Zhang¹,

Kan²,

Huang³

et al. 2011

Genes Dev.

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Histone deacetylases (HDACs) are major epigenetic modulators involved in a broad spectrum of human diseases including cancers. Administration of HDAC inhibitors (HDACis) leads to growth inhibition, differentiation, and apoptosis of cancer cells. Understanding the regulatory mechanism of HDACs is imperative to harness the therapeutic potentials of HDACis. Here we show that HDACi-and DNA damage-induced apoptosis are severely compromised in mouse embryonic fibroblasts lacking a HECT domain ubiquitin ligase, Mule (Mcl-1 ubiquitin ligase E3). Mule specifically targets HDAC2 for ubiquitination and degradation. Accumulation of HDAC2 in Mule-deficient cells leads to compromised p53 acetylation as well as crippled p53 transcriptional activation, accumulation, and apoptotic response upon DNA damage and Nutlin-3 treatments. These defects in Mule-null cells can be partially reversed by HDACis and fully rescued by lowering the elevated HDAC2 in Mule-null cells to the normal levels as in wild-type cells. Taken together, our results reveal a critical regulatory mechanism of HDAC2 by Mule and suggest this pathway determines the cellular response to HDACis and DNA damage.

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“…Alternatively, this difference in HUWE1 function is a reflection of its context-and cell-type-dependent specificity in its biological role, which is highlighted by our findings in this report. Similarly, while HUWE1 can facilitate degradation of anti-apoptotic MCL1 [21,24,40], deletion of HUWE1 in the pancreas did not change MCL1 protein expression. This is consistent with the only slight differences in MCL1 that were seen at steady state in B lymphocytes with Huwe1 deletion, suggesting MCL1 regulation is context-specific [18,24].…”

Section: Discussionmentioning

confidence: 84%

“…Apart from p53, HUWE1 has mul tiple other polyubiquitination substrates [18][19][20][21][22]. Among them is MCL1, which belongs to the anti-apoptotic B cell CLL/lymphoma 2 (BCL-2) family of proteins [20].…”

Section: Introductionmentioning

confidence: 99%

Dichotomous role of pancreatic HUWE1/MULE/ARF-BP1 in modulating beta cell apoptosis in mice under physiological and genotoxic conditions

et al. 2014

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Aims/hypothesis Diabetes mellitus represents a significant burden on the health of the global population. Both type 1 and type 2 diabetes share a common feature of a reduction in functional beta cell mass. A newly discovered ubiquitination molecule HECT, UBA and WWE domain containing 1, E3 ubiquitin protein ligase (HUWE1 [also known as MULE or ARF-BP1]) is a critical regulator of p53-dependent apoptosis. However, its role in islet homeostasis is not entirely clear. Methods We generated mice with pancreas-specific deletion of Huwe1 using a Cre-loxP recombination system driven by the Pdx1 promoter (Pdx1cre + Huwe1 fl/fl ) to assess the in vivo role of HUWE1 in the pancreas. Results Targeted deletion of Huwe1 in the pancreas preferentially activated p53-mediated beta cell apoptosis, leading to reduced beta cell mass and diminished insulin exocytosis. These defects were aggravated by ageing, with progressive further decline in insulin secretion and glucose homeostasis in older mice. Intriguingly, Huwe1 deletion provided protection against genotoxicity, such that Pdx1cre + Huwe1 fl/fl mice were resistant to multiple-lowdose-streptozotocin-induced beta cell apoptosis and diabetes. Conclusion/interpretation HUWE1 expression in the pancreas is essential in determining beta cell mass. Furthermore, HUWE1 demonstrated divergent roles in regulating beta cell apoptosis depending on physiological or genotoxic conditions.

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Cdc6 Stability Is Regulated by the Huwe1 Ubiquitin Ligase after DNA Damage

Cited by 124 publications

References 61 publications

Spatio-temporal regulation of the human licensing factor Cdc6 in replication and mitosis

Spatio-temporal regulation of the human licensing factor Cdc6 in replication and mitosis

Mule determines the apoptotic response to HDAC inhibitors by targeted ubiquitination and destruction of HDAC2

Dichotomous role of pancreatic HUWE1/MULE/ARF-BP1 in modulating beta cell apoptosis in mice under physiological and genotoxic conditions

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