ROC1, a Homolog of APC11, Represents a Family of Cullin Partners with an Associated Ubiquitin Ligase Activity

Ohta, Tomohiko; Michel, Jennifer J. Carlisle; Schottelius, Arndt; Xiong, Yue

doi:10.1016/s1097-2765(00)80482-7

Cited by 427 publications

(481 citation statements)

References 19 publications

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“…In budding yeast, it is known that there is only one member of the ySAG/yROC/yRbx/Hrt family. Targeted disruption of this gene results in cell death that can be fully rescued by ROC1/Rbx1 Ohta et al, 1999) or ySAG (this report) or ROC2, an N-terminal truncated SAG, as reported (Ohta et al, 1999). Since both ROC1/Rbx1/Hrt1 and SAG has ubiquitin ligase activity when complexed with SCF component, it is likely that SAG/ROC/Rbx/Hrt regulates cell cycle through ubiquitin/proteolysis pathway.…”

Section: Discussionmentioning

confidence: 54%

“…We showed a morphological cell enlargement and a broad distribution of¯uorescence intensities with an increased DNA content in SAG knockout cells (Figure 4). Several recent ®ndings also support this notion: (1) Xenopus Cdc34, an E2 that binds to SAG/ROC/Rbx/Hrt Ohta et al, 1999;Seol et al, 1999;Skowyra et al, 1999;Tan et al, 1999;Tyers and Willems, 1999) promoted degradation of Wee1 (Michael and Newport, 1998), a key G2/M negative regulator (McGowan and Russell, 1993;Parker and Piwnica Worms, 1992); (2) SCF components, Skp1 and Cul1 were localized to the centrosome and regulated the centrosome duplication cycle in mammalian cells (Freed et al, 1999); and (3) Cdc4, an F-box protein in SCF complex was required for the onset of S phase as well as anaphase in Saccharomyces cerevisiae (Goh and Surana, 1999).…”

Section: Discussionmentioning

confidence: 80%

“…Among genes that are involved in G1?S progression, Cul1 is a SAG/ROC binding protein and a component of E3 SCF complex required for SIC-1 degradation Ohta et al, 1999;Willems et al, 1996). CLG1 is a cyclin-like protein that interacts with Pho85p (Matsumoto and Wickner, 1993), a Ser/Thr kinase involved in induction of G1?S progression (Espinoza et al, 1994;Levine et al, 1995).…”

Section: Discussionmentioning

confidence: 99%

“…SAG is also shown to be a component of E3 ubiquitin ligase involved in the degradation of many biological important molecules including IkB Ohta et al, 1999;Skowyra et al, 1999;Tan et al, 1999). It is possible that anti-apopotosis activity of SAG/ROC/Rbx can also be achieved through ubiquitination and degradation of IkB, an inhibitor of NF-kB (Ohta et al, 1999;Tan et al, 1999), leading to activation of apoptosis inhibitor, NF-kB (Beg and Baltimore, 1996;Mayo et al, 1997;Van Antwerp et al, 1996, 1998Wang et al, 1996). This hypothesis is being tested currently in our laboratory.…”

Section: Discussionmentioning

confidence: 99%

“…While this manuscript was in its late stage of preparation, several groups have reported the cloning and characterization of ROC1 (regulator of cullins), Rbx1 (RING box) or Hrt1 that either binds to cullins or VHL tumor suppressor gene product or SCF complex to form important E3 ubiquitin ligase complex Ohta et al, 1999;Seol et al, 1999;Skowyra et al, 1999;Tan et al, 1999;Tyers and Willems, 1999). By direct sequencing comparison, SAG turns out to be the second member of this ROC/Rbx/Hrt family (ROC2/Rbx2/Hrt2).…”

Section: Like Roc1 Sag Binds To Cul1mentioning

confidence: 99%

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Yeast homolog of human SAG/ROC2/Rbx2/Hrt2 is essential for cell growth, but not for germination: chip profiling implicates its role in cell cycle regulation

Swaroop¹,

Wang²,

Miller³

et al. 2000

Oncogene

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In an attempt to understand the signaling pathway mediating redox-induced apoptosis, we cloned SAG, an evolutionarily conserved zinc RING ®nger gene that, when overexpressed, protects cells from apoptosis induced by redox agents. Here we report functional characterization of SAG by the use of yeast genetics approach. Targeted disruption of ySAG, yeast homolog of human SAG, and subsequent tetrad analysis revealed that ySAG is required for yeast viability. Complementation experiment showed that the lethal phenotype induced by the ySAG deletion is fully rescued by wildtype SAG, but not by several hSAG mutants. Complementation experiment has also con®rmed that ySAG is essential for normal vegetative growth, rather than being required for sporulation. Furthermore, cell death induced by SAG deletion was accompanied by cell enlargement and abnormal cell cycle pro®ling with an increased DNA content. Importantly, SAG was found to be the second family member of Rbx (RING box protein) or ROC (Regulator of cullins) or Hrt that is a component of SCF E3 ubiquitin ligase. Indeed, like ROC1/Rbx1/Hrt1, SAG binds to Cul1 and SAG-Cul1 complex has ubiquitin ligase activity to promote poly-ubiquitination of E2/ Cdc34. This ligase activity is required for complementation of death phenotype induced by ySAG disruption. Finally, chip pro®ling of the entire yeast genome revealed induction of several G1/S as well as G2/M checkpoint control genes upon SAG withdrawal. Thus, SAG appears to control cell cycle progression in yeast by promoting ubiquitination and degradation of cell cycle regulatory proteins.

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Section: Discussionmentioning

confidence: 54%

Section: Discussionmentioning

confidence: 80%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Like Roc1 Sag Binds To Cul1mentioning

confidence: 99%

See 3 more Smart Citations

Yeast homolog of human SAG/ROC2/Rbx2/Hrt2 is essential for cell growth, but not for germination: chip profiling implicates its role in cell cycle regulation

Swaroop¹,

Wang²,

Miller³

et al. 2000

Oncogene

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Modes of regulation of ubiquitin-mediated protein degradation

2000

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The ubiquitin-proteasome pathway is responsible for the major portion of specific cellular protein degradation. Ubiquitin-mediated degradation is involved in physiological regulation of many cellular processes, including cell cycle progression, differentiation, and signal transduction. Here, we review the basic mechanisms of the ubiquitin system and the various ways in which ubiquitin-mediated degradation can be modulated by physiological signals.

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Promotion of S-phase entry and cell growth under serum starvation by SAG/ROC2/Rbx2/Hrt2, an E3 ubiquitin ligase component: Association with inhibition of p27 accumulation

et al. 2001

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ROC1, a Homolog of APC11, Represents a Family of Cullin Partners with an Associated Ubiquitin Ligase Activity

Cited by 427 publications

References 19 publications

Yeast homolog of human SAG/ROC2/Rbx2/Hrt2 is essential for cell growth, but not for germination: chip profiling implicates its role in cell cycle regulation

Yeast homolog of human SAG/ROC2/Rbx2/Hrt2 is essential for cell growth, but not for germination: chip profiling implicates its role in cell cycle regulation

Modes of regulation of ubiquitin-mediated protein degradation

Promotion of S-phase entry and cell growth under serum starvation by SAG/ROC2/Rbx2/Hrt2, an E3 ubiquitin ligase component: Association with inhibition of p27 accumulation

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