2015
DOI: 10.1242/jcs.173559
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PDGFRβ and oncogenic, mutant PDGFRα D842V promote disassembly of primary cilia by a PLCγ and AURKA dependent mechanism

Abstract: Primary cilia are microtubule-based sensory organelles projecting from most quiescent mammalian cells, which disassemble in cells cultured in serum-deprived conditions upon re-addition of serum or growth factors. Platelet-derived growth factors (PDGF) are implicated in deciliation, but the specific receptor isoforms and mechanisms involved are unclear. We report that PDGFRβ promotes deciliation in cultured cells and provide evidence implicating PLCγ and intracellular Ca 2+ release in this process. Activation o… Show more

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Cited by 25 publications
(24 citation statements)
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References 44 publications
(74 reference statements)
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“…For example, certain ciliary signalling proteins, such as Smo (a key regulator of Hh signalling) or platelet-derived growth factor receptor (PDGFR), are proto-oncogenes that are aberrantly activated at cilia in cancer 82,83 . Remarkably, whereas some types of cancer (basal cell carcinoma and medulloblastoma) are dependent on cilia 84,85 , other cancers, including melanoma and breast, pancreatic, renal, and prostate cancer, exhibit loss of cilia, most likely during the early stages of oncogenesis 8690 .…”
Section: A Role For the Cilium In Cell Cycle Control And Human Cancermentioning
confidence: 99%
“…For example, certain ciliary signalling proteins, such as Smo (a key regulator of Hh signalling) or platelet-derived growth factor receptor (PDGFR), are proto-oncogenes that are aberrantly activated at cilia in cancer 82,83 . Remarkably, whereas some types of cancer (basal cell carcinoma and medulloblastoma) are dependent on cilia 84,85 , other cancers, including melanoma and breast, pancreatic, renal, and prostate cancer, exhibit loss of cilia, most likely during the early stages of oncogenesis 8690 .…”
Section: A Role For the Cilium In Cell Cycle Control And Human Cancermentioning
confidence: 99%
“…Nevertheless, when GFP-tagged PDGFRa was expressed in RPE cells, the fusion protein was found to localize to the primary cilium ( Fig. 2B) (Nielsen et al 2015), suggesting that these cells indeed contain the machinery for targeting the receptor to this organelle. Moreover, careful examination of newly divided, cultured NIH3T3 cells revealed that PDGFRa localizes asynchronously to cilia of two sister cells, with the receptor preferentially accumulating in the cilium emanating from the cell with the oldest mother centriole (Anderson and Stearns 2009).…”
Section: Primary Cilia and Regulation Of Pdgfraa Signalingmentioning
confidence: 98%
“…Subsequent studies have confirmed cilia-specific localization of PDGFRa in a range of additional cell types, including rat astrocytes and neuroblasts (Danilov et al 2009), mouse heart ventricular cells (Gerhardt et al 2013), human embryonic stem cells (Awan et al 2010), ovarian surface epithelial cells (Egeberg et al 2012), and mouse osteoblasts (Noda et al 2016). Of note, in some ciliated cell types, such as rat oligodendrocytes (Falcon-Urrutia et al 2015) and mouse heart atrial cells (Gerhardt et al 2013), PDGFRa seems to be conspicuously absent from the organelle, whereas in retinal pigment epithelial (RPE) cells, which are commonly used in ciliary studies, PDGFRa seems hardly to be expressed at all (Lei et al 2011;Nielsen et al 2015). Nevertheless, when GFP-tagged PDGFRa was expressed in RPE cells, the fusion protein was found to localize to the primary cilium ( Fig.…”
Section: Primary Cilia and Regulation Of Pdgfraa Signalingmentioning
confidence: 99%
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