2009
DOI: 10.4161/cc.8.5.7787
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Mitotic kinase dynamics of the active form of AMPK (Phospho-AMPKαThr172) in human cancer cells

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Cited by 48 publications
(56 citation statements)
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“…7 Intriguingly, we recently reported that the Threonine 172-phosphorylated active form of the α-catalytic subunit of AMPK (PP-AMPKα Thr172 ) is specifically upregulated within mitotic areas in human cancer tissues. 8 Careful immunohistochemical analyses confirmed that PP-AMPKα Thr172 exhibits a series of choreographed movements at precise nucleocytoplasmic locations and at specific times from prophase to telophase. Biochemical analyses revealed further that kinetic changes of AMPKα activation occur in a cell cycle phase-dependent manner and strictly in parallel to that of well-characterized M-phase activated kinases.…”
Section: Ampkmentioning
confidence: 99%
“…7 Intriguingly, we recently reported that the Threonine 172-phosphorylated active form of the α-catalytic subunit of AMPK (PP-AMPKα Thr172 ) is specifically upregulated within mitotic areas in human cancer tissues. 8 Careful immunohistochemical analyses confirmed that PP-AMPKα Thr172 exhibits a series of choreographed movements at precise nucleocytoplasmic locations and at specific times from prophase to telophase. Biochemical analyses revealed further that kinetic changes of AMPKα activation occur in a cell cycle phase-dependent manner and strictly in parallel to that of well-characterized M-phase activated kinases.…”
Section: Ampkmentioning
confidence: 99%
“…13 In this regard, we have previously reported that the active form of AMPK directly binds the mitotic apparatus and travels from centrosomes to the spindle midzone during mitosis. [32][33][34] Recently, we have established that polo-like kinase 1 (PLK1) is a novel regulator of AMPK activation at the mitotic apparatus. 35 These findings, altogether, may suggest the existence of a functional link connecting PLK1, AMPK and P-Raptor Ser722 during mitosis.…”
Section: ©2 0 1 1 L a N D E S B I O S C I E N C E D O N O T D I S Tmentioning
confidence: 99%
“…30 When analyzing mitotic areas of human cancer tissues, we have recently shown that, upon activating phosphorylation of Thr172 at its α catalytic subunit, AMPK distinctively organized in the form of a distinct punctuate staining during mitosis and cytokinesis. 31 Importantly, eye-catching P-AMPK Thr172 spots were not distributed randomly in the cytoplasm of mitotic cells but rather appeared to display choreographed series of movements at precise nucleo-cytoplasmic locations and specific times from prophase to telophase in vivo. Moreover, the kinetic of changes in in vitro AMPK activation was found to occur in a cell cycle phase-dependent manner and strictly in parallel to that of well-characterized mitotic kinases such as Aurora B.…”
Section: Introductionmentioning
confidence: 99%