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A novel DAG-dependent mechanism links PKCa and Cyclin B1 regulating cell cycle progression

dc.contributor.authorPoli, Alessandro
dc.contributor.authorRamazzotti, Giulia
dc.contributor.authorMatteucci, Alessandro
dc.contributor.authorManzoli, Lucia
dc.contributor.authorLonetti, Annalisa
dc.contributor.authorSuh, Pann-Ghill
dc.contributor.authorMcCubrey, James A.
dc.contributor.authorCocco, Lucio
dc.date.accessioned2016-06-16T19:17:34Z
dc.date.available2016-06-16T19:17:34Z
dc.date.issued2014-11
dc.description.abstractThrough the years, different studies showed the involvement of Protein Kinase C (PKC) in cell cycle control, in particular during G1/S transition. Little is known about their role at G2/M checkpoint. In this study, using K562 human erythroleukemia cell line, we found a novel and specific mechanism through which the conventional isoform PKC⍺ positively affects Cyclin B1 modulating G2/M progression of cell cycle. Since the kinase activity of this PKC isoform was not necessary in this process, we demonstrated that PKC⍺, physically interacting with Cyclin B1, avoided its degradation and stimulated its nuclear import at mitosis. Moreover, the process resulted to be strictly connected with the increase in nuclear diacylglycerol levels (DAG) at G2/M checkpoint, due to the activity of nuclear Phospholipase C β1 (PLCβ1), the only PLC isoform mainly localized in the nucleus of K562 cells. Taken together, our findings indicated a novel DAG dependent mechanism able to regulate the G2/M progression of the cell cycle.en_US
dc.identifier.citationOncotarget; 5:22 p. 11526-11540en_US
dc.identifier.issn1949-2553
dc.identifier.pmidpmc4294327en_US
dc.identifier.urihttp://hdl.handle.net/10342/5667
dc.relation.urihttp://www.ncbi.nlm.nih.gov/pmc/articles/PMC4294327/en_US
dc.subjectPKCen_US
dc.subjectCyclinen_US
dc.subjectCell Cycleen_US
dc.subjectPLCen_US
dc.subjectDAGen_US
dc.subjectnucleien_US
dc.titleA novel DAG-dependent mechanism links PKCa and Cyclin B1 regulating cell cycle progressionen_US
dc.typeArticleen_US
ecu.journal.issue22en_US
ecu.journal.nameOncotargeten_US
ecu.journal.pages11526-11540en_US
ecu.journal.volume5en_US

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