Aurora A and AKT Kinase Signaling Associated with Primary Cilia

Dysregulation of kinase signaling is associated with various pathological conditions, including cancer, inflammation, and autoimmunity; consequently, the kinases involved have become major therapeutic targets. While kinase signaling pathways play crucial roles in multiple cellular processes, the precise manner in which their dysregulation contributes to disease is dependent on the context; for example, the cell/tissue type or subcellular localization of the kinase or substrate. Thus, context-selective targeting of dysregulated kinases may serve to increase the therapeutic specificity while reducing off-target adverse effects. Primary cilia are antenna-like structures that extend from the plasma membrane and function by detecting extracellular cues and transducing signals into the cell. Cilia formation and signaling are dynamically regulated through context-dependent mechanisms; as such, dysregulation of primary cilia contributes to disease in a variety of ways. Here, we review the involvement of primary cilia-associated signaling through aurora A and AKT kinases with respect to cancer, obesity, and other ciliopathies.

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Primary Cilia in Glial Cells: An Oasis in the Journey to Overcoming Neurodegenerative Diseases

Frontiers in Neuroscience ◽

10.3389/fnins.2021.736888 ◽

2021 ◽

Vol 15 ◽

Author(s):

Soo Mi Ki ◽

Hui Su Jeong ◽

Ji Eun Lee

Keyword(s):

Neurodegenerative Diseases ◽

Glial Cells ◽

Primary Cilia ◽

Regulatory Mechanisms ◽

Close Attention ◽

Cellular Processes ◽

Cilia Formation ◽

And Function ◽

Cellular Organelles

Many neurodegenerative diseases have been associated with defects in primary cilia, which are cellular organelles involved in diverse cellular processes and homeostasis. Several types of glial cells in both the central and peripheral nervous systems not only support the development and function of neurons but also play significant roles in the mechanisms of neurological disease. Nevertheless, most studies have focused on investigating the role of primary cilia in neurons. Accordingly, the interest of recent studies has expanded to elucidate the role of primary cilia in glial cells. Correspondingly, several reports have added to the growing evidence that most glial cells have primary cilia and that impairment of cilia leads to neurodegenerative diseases. In this review, we aimed to understand the regulatory mechanisms of cilia formation and the disease-related functions of cilia, which are common or specific to each glial cell. Moreover, we have paid close attention to the signal transduction and pathological mechanisms mediated by glia cilia in representative neurodegenerative diseases. Finally, we expect that this field of research will clarify the mechanisms involved in the formation and function of glial cilia to provide novel insights and ideas for the treatment of neurodegenerative diseases in the future.

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KIF14 controls ciliogenesis via regulation of Aurora A and is important for Hedgehog signaling

The Journal of Cell Biology ◽

10.1083/jcb.201904107 ◽

2020 ◽

Vol 219 (6) ◽

Cited By ~ 6

Author(s):

Petra Pejskova ◽

Madeline Louise Reilly ◽

Lucia Bino ◽

Ondrej Bernatik ◽

Linda Dolanska ◽

...

Keyword(s):

Cell Cycle ◽

Primary Cilium ◽

Hedgehog Signaling ◽

Cell Cycle Progression ◽

Primary Cilia ◽

Aurora A ◽

Pathway Activation ◽

Cilia Formation ◽

Tightly Coupled ◽

Hh Signaling

Primary cilia play critical roles in development and disease. Their assembly and disassembly are tightly coupled to cell cycle progression. Here, we present data identifying KIF14 as a regulator of cilia formation and Hedgehog (HH) signaling. We show that RNAi depletion of KIF14 specifically leads to defects in ciliogenesis and basal body (BB) biogenesis, as its absence hampers the efficiency of primary cilium formation and the dynamics of primary cilium elongation, and disrupts the localization of the distal appendage proteins SCLT1 and FBF1 and components of the IFT-B complex. We identify deregulated Aurora A activity as a mechanism contributing to the primary cilium and BB formation defects seen after KIF14 depletion. In addition, we show that primary cilia in KIF14-depleted cells are defective in response to HH pathway activation, independently of the effects of Aurora A. In sum, our data point to KIF14 as a critical node connecting cell cycle machinery, effective ciliogenesis, and HH signaling.

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Prdx1 Promotes the Loss of Primary Cilia in Esophageal Squamous Cell Carcinoma

10.21203/rs.2.17849/v1 ◽

2019 ◽

Author(s):

Fanghua Gong ◽

Qiongzhen Chen ◽

Jinmeng Li ◽

Xiaoning Yang ◽

Junfeng Ma ◽

...

Keyword(s):

Squamous Cell Carcinoma ◽

Esophageal Squamous Cell Carcinoma ◽

Cell Carcinoma ◽

Squamous Cell ◽

Primary Cilia ◽

Molecular Mechanisms ◽

Tumor Formation ◽

Aurora A ◽

Cilia Formation ◽

Signaling Axis

Abstract Background: Loss of primary cilia is frequently observed in tumor cells, suggesting that the absence of this organelle may promote tumorigenesis through aberrant signal transduction, the inability to exit the cell cycle, and promotion of tumor cell invasion. Primary cilia loss also occurs in esophageal squamous cell carcinoma (ESCC) cells, but the molecular mechanisms that explain how ESCC cells lose primary cilia remain poorly understood. Methods: Inhibiting the expression of Prdx1 in the ESCC cells to detect the up-regulated genes related to cilium regeneration and down-regulated genes related to cilium disassembly by Gene chip. And, mice and cell experiments were carried to confirm the role of the HEF1-Aurora A-HDAC6 signaling axis in ESCC. Results: In this study, we found that silencing Peroxiredoxin 1 (Prdx1) restores primary cilia formation, and over-expressing Prdx1 induces primary cilia loss in ESCC cells. We also showed that the expression of Prdx1 regulates the action of the HEF1-Aurora A-HDAC6 signaling axis to promote the disassembly of primary cilia, and suppression of Prdx1 results in decreased tumor formation and tumor mass volume in vivo. Conclusions: These results suggest that Prdx1 is a novel regulator of primary cilia formation in ESCC cells.

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NRF2-dependent gene expression promotes ciliogenesis and Hedgehog signaling

Scientific Reports ◽

10.1038/s41598-019-50356-0 ◽

2019 ◽

Vol 9 (1) ◽

Cited By ~ 6

Author(s):

Ana Martin-Hurtado ◽

Raquel Martin-Morales ◽

Natalia Robledinos-Antón ◽

Ruth Blanco ◽

Ines Palacios-Blanco ◽

...

Keyword(s):

Hedgehog Signaling ◽

Primary Cilia ◽

Embryonic Stem ◽

Mtor Inhibitors ◽

Gene Promoters ◽

Protein Levels ◽

Functional Connections ◽

Differentiated Cells ◽

Cilia Formation ◽

And Function

Abstract The transcription factor NRF2 is a master regulator of cellular antioxidant and detoxification responses, but it also regulates other processes such as autophagy and pluripotency. In human embryonic stem cells (hESCs), NRF2 antagonizes neuroectoderm differentiation, which only occurs after NRF2 is repressed via a Primary Cilia-Autophagy-NRF2 (PAN) axis. However, the functional connections between NRF2 and primary cilia, microtubule-based plasma membrane protrusions that function as cellular antennae, remain poorly understood. For instance, nothing is known about whether NRF2 affects cilia, or whether cilia regulation of NRF2 extends beyond hESCs. Here, we show that NRF2 and primary cilia reciprocally regulate each other. First, we demonstrate that fibroblasts lacking primary cilia have higher NRF2 activity, which is rescued by autophagy-activating mTOR inhibitors, indicating that the PAN axis also operates in differentiated cells. Furthermore, NRF2 controls cilia formation and function. NRF2-null cells grow fewer and shorter cilia and display impaired Hedgehog signaling, a cilia-dependent pathway. These defects are not due to increased oxidative stress or ciliophagy, but rather to NRF2 promoting expression of multiple ciliogenic and Hedgehog pathway genes. Among these, we focused on GLI2 and GLI3, the transcription factors controlling Hh pathway output. Both their mRNA and protein levels are reduced in NRF2-null cells, consistent with their gene promoters containing consensus ARE sequences predicted to bind NRF2. Moreover, GLI2 and GLI3 fail to accumulate at the ciliary tip of NRF2-null cells upon Hh pathway activation. Given the importance of NRF2 and ciliary signaling in human disease, our data may have important biomedical implications.

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Ndel1 suppresses ciliogenesis in proliferating cells by regulating the trichoplein–Aurora A pathway

The Journal of Cell Biology ◽

10.1083/jcb.201507046 ◽

2016 ◽

Vol 212 (4) ◽

pp. 409-423 ◽

Cited By ~ 39

Author(s):

Hironori Inaba ◽

Hidemasa Goto ◽

Kousuke Kasahara ◽

Kanako Kumamoto ◽

Shigenobu Yonemura ◽

...

Keyword(s):

Primary Cilia ◽

Serum Starvation ◽

Aurora A ◽

Proliferating Cells ◽

Quiescent Cells ◽

Cell Cycle Reentry ◽

Upstream Regulator ◽

Cilia Formation ◽

Mother Centriole ◽

Component Protein

Primary cilia protrude from the surface of quiescent cells and disassemble at cell cycle reentry. We previously showed that ciliary reassembly is suppressed by trichoplein-mediated Aurora A activation pathway in growing cells. Here, we report that Ndel1, a well-known modulator of dynein activity, localizes at the subdistal appendage of the mother centriole, which nucleates a primary cilium. In the presence of serum, Ndel1 depletion reduces trichoplein at the mother centriole and induces unscheduled primary cilia formation, which is reverted by forced trichoplein expression or coknockdown of KCTD17 (an E3 ligase component protein for trichoplein). Serum starvation induced transient Ndel1 degradation, subsequent to the disappearance of trichoplein at the mother centriole. Forced expression of Ndel1 suppressed trichoplein degradation and axonemal microtubule extension during ciliogenesis, similar to trichoplein induction or KCTD17 knockdown. Most importantly, the proportion of ciliated and quiescent cells was increased in the kidney tubular epithelia of newborn Ndel1-hypomorphic mice. Thus, Ndel1 acts as a novel upstream regulator of the trichoplein–Aurora A pathway to inhibit primary cilia assembly.

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Phosphoinositide lipids in primary cilia biology

Biochemical Journal ◽

10.1042/bcj20200277 ◽

2020 ◽

Vol 477 (18) ◽

pp. 3541-3565

Author(s):

Sarah E. Conduit ◽

Bart Vanhaesebroeck

Keyword(s):

Primary Cilia ◽

Critical Role ◽

Phospholipid Composition ◽

Cell Types ◽

Phosphoinositide Metabolism ◽

Lipid Phosphatases ◽

Regulatory Enzymes ◽

Lipid Species ◽

Cilia Formation ◽

And Function

Primary cilia are solitary signalling organelles projecting from the surface of most cell types. Although the ciliary membrane is continuous with the plasma membrane it exhibits a unique phospholipid composition, a feature essential for normal cilia formation and function. Recent studies have illustrated that distinct phosphoinositide lipid species localise to specific cilia subdomains, and have begun to build a ‘phosphoinositide map’ of the cilium. The abundance and localisation of phosphoinositides are tightly regulated by the opposing actions of lipid kinases and lipid phosphatases that have also been recently discovered at cilia. The critical role of phosphoinositides in cilia biology is highlighted by the devastating consequences of genetic defects in cilia-associated phosphoinositide regulatory enzymes leading to ciliopathy phenotypes in humans and experimental mouse and zebrafish models. Here we provide a general introduction to primary cilia and the roles phosphoinositides play in cilia biology. In addition to increasing our understanding of fundamental cilia biology, this rapidly expanding field may inform novel approaches to treat ciliopathy syndromes caused by deregulated phosphoinositide metabolism.

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Dynein-2 intermediate chains play crucial but distinct roles in primary cilia formation and function

10.1101/251694 ◽

2018 ◽

Cited By ~ 1

Author(s):

Laura Vuolo ◽

Nicola L. Stevenson ◽

Kate J. Heesom ◽

David J. Stephens

Keyword(s):

Transition Zone ◽

Cell Lines ◽

Primary Cilia ◽

Point Mutations ◽

Intraflagellar Transport ◽

Jeune Syndrome ◽

Cilia Formation ◽

Microtubule Motor ◽

And Function ◽

Intermediate Chains

AbstractThe dynein-2 microtubule motor is the retrograde motor for intraflagellar transport. Mutations in dynein-2 components cause skeletal ciliopathies, notably Jeune syndrome. Dynein-2 comprises a heterodimer of two non-identical intermediate chains, WDR34 and WDR60. Here, we use knockout cell lines to demonstrate that each intermediate chain has a distinct role in cilia function. Both proteins are required to maintain a functional transition zone and for efficient bidirectional intraflagellar transport, only WDR34 is essential for axoneme extension. In contrast, only WDR60 is essential for co-assembly of the other subunits. Furthermore, WDR60 cannot compensate for loss of WDR34 or vice versa. This work defines a functional asymmetry to match the subunit asymmetry within the dynein-2 motor. Analysis of causative point mutations in WDR34 and WDR60 can partially restore function to knockout cells. Our data show that Jeune syndrome is caused by defects in transition zone architecture as well as intraflagellar transport.SUMMARYHere, Vuolo and colleagues use engineered knockout human cell lines to define roles for dynein-2 intermediate chains. WDR34 is required for axoneme extension, while WDR60 is not. Both subunits are required for cilia transition zone organization and bidirectional intraflagellar transport.

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Dynein-2 intermediate chains play crucial but distinct roles in primary cilia formation and function

eLife ◽

10.7554/elife.39655 ◽

2018 ◽

Vol 7 ◽

Cited By ~ 9

Author(s):

Laura Vuolo ◽

Nicola L Stevenson ◽

Kate J Heesom ◽

David J Stephens

Keyword(s):

Transition Zone ◽

Primary Cilia ◽

Complex Function ◽

Intraflagellar Transport ◽

Loss Of Function ◽

Jeune Syndrome ◽

Cilia Formation ◽

Microtubule Motor ◽

And Function ◽

Intermediate Chains

The dynein-2 microtubule motor is the retrograde motor for intraflagellar transport. Mutations in dynein-2 components cause skeletal ciliopathies, notably Jeune syndrome. Dynein-2 contains a heterodimer of two non-identical intermediate chains, WDR34 and WDR60. Here, we use knockout cell lines to demonstrate that each intermediate chain has a distinct role in cilium function. Using quantitative proteomics, we show that WDR34 KO cells can assemble a dynein-2 motor complex that binds IFT proteins yet fails to extend an axoneme, indicating complex function is stalled. In contrast, WDR60 KO cells do extend axonemes but show reduced assembly of dynein-2 and binding to IFT proteins. Both proteins are required to maintain a functional transition zone and for efficient bidirectional intraflagellar transport. Our results indicate that the subunit asymmetry within the dynein-2 complex is matched with a functional asymmetry between the dynein-2 intermediate chains. Furthermore, this work reveals that loss of function of dynein-2 leads to defects in transition zone architecture, as well as intraflagellar transport.

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Author response: Dynein-2 intermediate chains play crucial but distinct roles in primary cilia formation and function

10.7554/elife.39655.024 ◽

2018 ◽

Author(s):

Laura Vuolo ◽

Nicola L Stevenson ◽

Kate J Heesom ◽

David J Stephens

Keyword(s):

Primary Cilia ◽

Author Response ◽

Cilia Formation ◽

And Function ◽

Intermediate Chains

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Primary Cilia Formation Does Not Rely on WNT/β-Catenin Signaling

Frontiers in Cell and Developmental Biology ◽

10.3389/fcell.2021.623753 ◽

2021 ◽

Vol 9 ◽

Author(s):

Ondrej Bernatik ◽

Petra Paclikova ◽

Anna Kotrbova ◽

Vitezslav Bryja ◽

Lukas Cajanek

Keyword(s):

Primary Cilia ◽

Wnt Pathway ◽

Inhibitory Effect ◽

Positive Role ◽

Knock Out ◽

Wnt Ligands ◽

Cilia Formation ◽

And Function ◽

Cilium Length

Primary cilia act as crucial regulators of embryo development and tissue homeostasis. They are instrumental for modulation of several signaling pathways, including Hedgehog, WNT, and TGF-β. However, gaps exist in our understanding of how cilia formation and function is regulated. Recent work has implicated WNT/β-catenin signaling pathway in the regulation of ciliogenesis, yet the results are conflicting. One model suggests that WNT/β-catenin signaling negatively regulates cilia formation, possibly via effects on cell cycle. In contrast, second model proposes a positive role of WNT/β-catenin signaling on cilia formation, mediated by the re-arrangement of centriolar satellites in response to phosphorylation of the key component of WNT/β-catenin pathway, β-catenin. To clarify these discrepancies, we investigated possible regulation of primary cilia by the WNT/β-catenin pathway in cell lines (RPE-1, NIH3T3, and HEK293) commonly used to study ciliogenesis. We used WNT3a to activate or LGK974 to block the pathway, and examined initiation of ciliogenesis, cilium length, and percentage of ciliated cells. We show that the treatment by WNT3a has no- or lesser inhibitory effect on cilia formation. Importantly, the inhibition of secretion of endogenous WNT ligands using LGK974 blocks WNT signaling but does not affect ciliogenesis. Finally, using knock-out cells for key WNT pathway components, namely DVL1/2/3, LRP5/6, or AXIN1/2 we show that neither activation nor deactivation of the WNT/β-catenin pathway affects the process of ciliogenesis. These results suggest that WNT/β-catenin-mediated signaling is not generally required for efficient cilia formation. In fact, activation of the WNT/β-catenin pathway in some systems seems to moderately suppress ciliogenesis.

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