Calmodulin activation of Aurora-A kinase (AURKA) is required during ciliary disassembly and in mitosis

Plotnikova, Olga; Nikonova, Anna S.; Loskutov, Yuriy V.; Kozyulina, Polina Y.; Pugacheva, Elena N.; Golemis, Erica A.

doi:10.1091/mbc.e11-12-1056

Cited by 132 publications

(153 citation statements)

References 49 publications

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“…Nedd9 binding and activation of Aurora-A is required for ciliary resorption (12,31), and we have observed that Aurora-A expression is elevated in the cystic tissue of patients with ADPKD (20). These results suggested the hypothesis that defects in Aurora-A activation at cilia might underlie the observed trafficking and morphological defects.…”

Section: Nedd9mentioning

confidence: 59%

Nedd9 restrains renal cystogenesis in Pkd1 ^−/− mice

Nikonova

Plotnikova

Serzhanova

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

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Significance This study uses mouse models for the first time to our knowledge to identify that NEDD9, a nonenzymatic scaffolding protein that is commonly amplified in cancer, has an important restraining function for the development of renal cysts in autosomal dominant polycystic kidney disease (ADPKD). In the absence of NEDD9, failure to activate Aurora-A kinase causes multiple abnormalities in cilia, intensifying the effect of genetic deficiency of mutations in the polycystic kidney disease (PKD) 1 gene, the most common cause of PKD. As important implications, clinical inhibitors of Aurora-A also intensified ADPKD induced by mutation of PKD1 , suggesting caution in use of these agents, whereas recently reported polymorphisms in Nedd9 may contribute to the genetic heterogeneity of ADPKD presentation in affected families.

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Section: Nedd9mentioning

confidence: 59%

Nedd9 restrains renal cystogenesis in Pkd1 ^−/− mice

Nikonova

Plotnikova

Serzhanova

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

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“…Increases in cellular levels of phospho-AURKA are associated with an increase in cilia disassembly (Pugacheva et al, 2007;Plotnikova et al, 2012) and similar defects are observed in Inpp5e 2/2 cells (Bielas et al, 2009). To determine whether there was a shared functional basis to these phenotypes, we serum starved fibroblasts from wild-type and Inpp5e 2/2 mice and profiled cilia disassembly upon the addition of serum in the presence or absence of an AURKA inhibitor (C1368) or vehicle control (DMSO).…”

Section: Functional Dissection Of the Role Of The Aurka-inpp5e Interamentioning

confidence: 79%

“…Plasmids, cell culture and inhibitors AURKA and catalytically inactive AURKA (K162R) were expressed from pcDNA3.1-mRFP vector (Plotnikova et al, 2012), murine wild-type INPP5E, INPP5E D480N and INPP4B were expressed from pcDNA3.1-HA, and FLAG-INPP5E was expressed from pcDNA3.1-Flag. V5-tagged human wild-type INPP5E and INPP5E containing Joubert syndrome (JBTS) missense mutations were cloned into pLenti6.2/V5-DEST (Life Technologies).…”

Section: Methodsmentioning

confidence: 99%

“…AURKA localises to the ciliary basal body in mammalian cells, where it regulates ciliary disassembly through interactions with NEDD9 and other proteins (Pugacheva et al, 2007). Increases in phosphorylation of AURKA are linked to increased cilia disassembly (Pugacheva et al, 2007;Plotnikova et al, 2012), whereas Inpp5e 2/2 MEFs have ciliary disassembly defects (Jacoby et al, 2009). In serum-starved primary fibroblasts from Inpp5e 2/2 mice, we observed an increase in the level of phosphorylated AURKA compared with that of wild-type cells.…”

Section: Aurka Levels Are Regulated By Inpp5ementioning

confidence: 99%

“…In addition to other ciliopathy features, Inpp5e 2/2 mice also develop renal cysts, a phenotype that is frequently associated with primary cilium defects (Jacoby et al, 2009). Taking into account the previously described role for AURKA in PKD (Plotnikova et al, 2011) and in the regulation of primary cilia stability (Pugacheva et al, 2007;Plotnikova et al, 2012), we evaluated the impact of altered AURKA function in a cellular model of INPP5E-dependent cyst formation. To examine whether the AURKA-INPP5E complex impacted upon these features, we depleted INPP5E from IMCD3 cells and grew them in a threedimensional (3D) Matrigel matrix.…”

Section: Functional Dissection Of the Role Of The Aurka-inpp5e Interamentioning

confidence: 99%

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INPP5E interacts with AURKA, linking phosphoinositide signalling to primary cilium stability

Plotnikova

Seo

Cottle

et al. 2014

Journal of Cell Science

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Mutations in inositol polyphosphate 5-phosphatase E (INPP5E) cause the ciliopathies known as Joubert and MORM syndromes; however, the role of INPP5E in ciliary biology is not well understood. Here, we describe an interaction between INPP5E and AURKA, a centrosomal kinase that regulates mitosis and ciliary disassembly, and we show that this interaction is important for the stability of primary cilia. Furthermore, AURKA phosphorylates INPP5E and thereby increases its 5-phosphatase activity, which in turn promotes transcriptional downregulation of AURKA, partly through an AKTdependent mechanism. These findings establish the first direct link between AURKA and phosphoinositide signaling and suggest that the function of INPP5E in cilia is at least partly mediated by its interactions with AURKA.

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Primary Cilia as Signaling Hubs in Health and Disease

et al. 2018

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Primary cilia detect extracellular cues and transduce these signals into cells to regulate proliferation, migration, and differentiation. Here, the function of primary cilia as signaling hubs of growth factors and morphogens is in focus. First, the molecular mechanisms regulating the assembly and disassembly of primary cilia are described. Then, the role of primary cilia in mediating growth factor and morphogen signaling to maintain human health and the potential mechanisms by which defects in these pathways contribute to human diseases, such as ciliopathy, obesity, and cancer are described. Furthermore, a novel signaling pathway by which certain growth factors stimulate cell proliferation through suppression of ciliogenesis is also described, suggesting novel therapeutic targets in cancer.

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Calmodulin activation of Aurora-A kinase (AURKA) is required during ciliary disassembly and in mitosis

Abstract: This study demonstrates for the first time that binding of calcium-activated calmodulin to a minimal interaction site within the disordered N-terminal domain is required for the essential Aurora-A activity in mitosis and in regulation of ciliary disassembly.

Cited by 132 publications

References 49 publications

Nedd9 restrains renal cystogenesis in Pkd1 ^−/− mice

Nedd9 restrains renal cystogenesis in Pkd1 ^−/− mice

INPP5E interacts with AURKA, linking phosphoinositide signalling to primary cilium stability

Primary Cilia as Signaling Hubs in Health and Disease

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Calmodulin activation of Aurora-A kinase (AURKA) is required during ciliary disassembly and in mitosis

Abstract: This study demonstrates for the first time that binding of calcium-activated calmodulin to a minimal interaction site within the disordered N-terminal domain is required for the essential Aurora-A activity in mitosis and in regulation of ciliary disassembly.

Cited by 132 publications

References 49 publications

Nedd9 restrains renal cystogenesis in Pkd1 −/− mice

Nedd9 restrains renal cystogenesis in Pkd1 −/− mice

INPP5E interacts with AURKA, linking phosphoinositide signalling to primary cilium stability

Primary Cilia as Signaling Hubs in Health and Disease

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Product

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Nedd9 restrains renal cystogenesis in Pkd1 ^−/− mice

Nedd9 restrains renal cystogenesis in Pkd1 ^−/− mice