Polaris, a protein disrupted in<i>orpk</i>mutant mice, is required for assembly of renal cilium

Yoder, Bradley K.; Tousson, Albert; Millican, Leigh; Wu, John H.; Bugg, Charles E.; Schafer, James A.; Balkovetz, Daniel F.; Watkins, Mary L.

doi:10.1152/ajprenal.00273.2001

Cited by 227 publications

(202 citation statements)

References 57 publications

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“…34,35 We recently reported that downregulation of Pkhd1 significantly decreases ciliary formation in cultured Pkhd1-silenced IMCD cells, suggesting that lack of FPC might disrupt ciliogenesis in renal epithelial cells. This result is consistent with studies in which transient small interference RNA-mediated inhibition of Pkhd1 in cholangiocytes resulted in shortening and decreased formation of cilia, 29 but spatial and environmental differences between in vivo tissues and in vitro cell culture may lead to different results.…”

Section: Discussionmentioning

confidence: 99%

“…FPC was demonstrated to localize to the primary cilium and/or basal bodies of renal tubular epithelia, [27][28][29][30][31] and malformation of the cilia was shown to induce cyst formation in the kidneys 34,35 ; therefore, we began to determine whether the lack of FPC also disrupts ciliogenesis in Pkhd1-deficient mice. We used IF with an anti-acetylated ␣-tubulin antibody to examine the number and morphology of renal primary cilia in 6-moold littermates.…”

Section: Lack Of Fpc Exhibits Aberrant Ciliogenesis In the Renal Epitmentioning

confidence: 99%

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Fibrocystin/Polyductin Modulates Renal Tubular Formation by Regulating Polycystin-2 Expression and Function

Kim

Fu²,

Hui

et al. 2008

Journal of the American Society of Nephrology

129

105

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Autosomal recessive polycystic kidney disease is caused by mutations in PKHD1, which encodes the membrane-associated receptor-like protein fibrocystin/polyductin (FPC). FPC associates with the primary cilia of epithelial cells and co-localizes with the Pkd2 gene product polycystin-2 (PC2), suggesting that these two proteins may function in a common molecular pathway. For investigation of this, a mouse model with a gene-targeted mutation in Pkhd1 that recapitulates phenotypic characteristics of human autosomal recessive polycystic kidney disease was produced. The absence of FPC is associated with aberrant ciliogenesis in the kidneys of Pkhd1-deficient mice. It was found that the COOH-terminus of FPC and the NH2-terminus of PC2 interact and that lack of FPC reduced PC2 expression but not vice versa, suggesting that PC2 may function immediately downstream of FPC in vivo. PC2-channel activities were dysregulated in cultured renal epithelial cells derived from Pkhd1 mutant mice, further supporting that both cystoproteins function in a common pathway. In addition, mice with mutations in both Pkhd1 and Pkd2 had a more severe renal cystic phenotype than mice with single mutations, suggesting that FPC acts as a genetic modifier for disease severity in autosomal dominant polycystic kidney disease that results from Pkd2 mutations. It is concluded that a functional and molecular interaction exists between FPC and PC2 in vivo.

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Section: Discussionmentioning

confidence: 99%

Section: Lack Of Fpc Exhibits Aberrant Ciliogenesis In the Renal Epitmentioning

confidence: 99%

Fibrocystin/Polyductin Modulates Renal Tubular Formation by Regulating Polycystin-2 Expression and Function

Kim

Fu²,

Hui

et al. 2008

Journal of the American Society of Nephrology

129

105

View full text Add to dashboard Cite

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“…In tetrahymena pyriformis, it has been shown that colchicine does not disrupt existing ciliary axonemes 30 and we found previously that vinblastine, a drug with a similar mechanism of action, left the ciliary axoneme of human embryonic kidney cells (HEK293T) intact 31 . At the same time, nocodazole in moderate to high concentrations has been shown to disrupt the ciliary axoneme along with the MT network 32,33 . In line with these observations, nocodazole dissolved the MT skeleton including the ciliary axoneme of the MIN6m9 b-cell line, whereas colchicine did not disassemble the ciliary axoneme ( We cannot exclude an effect of colchicine on ciliogenesis, although a parsimonious explanation might be the improved visibility of ciliary axonemes because of the absence of other acetylated MT structures that otherwise mask the axonemes.…”

Section: Disruption Of Basal Body Integrity Impairs Insulin Secretionmentioning

confidence: 99%

Ciliary dysfunction impairs beta-cell insulin secretion and promotes development of type 2 diabetes in rodents

Christou-Savina²,

et al. 2014

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Type 2 diabetes mellitus is affecting more than 382 million people worldwide. Although much progress has been made, a comprehensive understanding of the underlying disease mechanism is still lacking. Here we report a role for the b-cell primary cilium in type 2 diabetes susceptibility. We find impaired glucose handling in young Bbs4 À / À mice before the onset of obesity. Basal body/ciliary perturbation in murine pancreatic islets leads to impaired first phase insulin release ex and in vivo. Insulin receptor is recruited to the cilium of stimulated b-cells and ciliary/basal body integrity is required for activation of downstream targets of insulin signalling. We also observe a reduction in the number of ciliated b-cells along with misregulated ciliary/basal body gene expression in pancreatic islets in a diabetic rat model. We suggest that ciliary function is implicated in insulin secretion and insulin signalling in the b-cell and that ciliary dysfunction could contribute to type 2 diabetes susceptibility.

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“…69,60,70 Although nephrocystin 3 and nephrocystin 4 have not been localized to cilia, nephrocystin 4 forms a complex with nephrocystin, suggesting that they may be colocalized in cilia. 63 Disruption of several additional genes in mouse also leads to PKD, and the protein products of at least two, cystin 65,71 and polaris/Tg737, 65,[72][73][74] are localized to cilia.…”

Section: Polycystic Kidney Diseasementioning

confidence: 99%

Cilium-generated signaling and cilia-related disorders

Pan

Wang

Snell

2005

Laboratory Investigation

210

183

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Biologists have long known that humans experience their environment through cilia. Light, odorant, and sound perception depend on these microtubule-filled, complex organelles present on cells in primary sensory tissues. Recently, discoveries on the mechanism of assembly of cilia (flagella) in the lowly, biflagellated, eucaryotic green alga Chlamydomonas have triggered a renaissance of interest in the organelles along with a recognition of their key sensory roles in nonsensory tissues. Chlamydomonas researchers uncovered an entirely new set of cellular machinery essential for transporting the protein components of cilia and flagella in all ciliated/ flagellated eukaryotic cells between their site of synthesis in the cell body and their site of assembly at the tip of the flagellum (intraflagellar transport: IFT). Prompted by the surprising observations that disruption of IFT genes in mice led to polycystic kidney disease (PKD) and that PKD proteins are present on the sensory cilia of Caenorhabditis elegans, researchers have made a direct connection between PKD and cilia. At least five (and possibly all) of the seven identified human genes disrupted in PKD and a related disorder nephronophthisis encode proteins expressed in the primary cilia that project into the lumen from the epithelial cells that line renal tubules. Moreover, the renal cilia are flow sensors and at least two of the PKD genes encode ciliary transmembrane proteins essential for mechanosensation. Although their roles have not yet been as clearly identified, cilia also are at the center of a rare human disorder, Bardet-Biedl syndrome (BBS), in which patients exhibit phenotypes of common human diseases, including obesity and increased incidence of hypertension and diabetes. Five of the eight known BBS genes encode basal body or cilia proteins in mice or humans, and homologues of two of the remaining genes are present in basal bodies/cilia of model organisms. Here we briefly describe the biology of cilia and flagella, we outline how studies on model organisms have led to our current understanding of the roles of these organelles and their proteins in health and disease, and we highlight the notion that the primary cilia present on cells throughout the body, even those on brain neurons, may be essential for as yet undiscovered cilium-generated signaling functions.

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Polaris, a protein disrupted inorpkmutant mice, is required for assembly of renal cilium

Cited by 227 publications

References 57 publications

Fibrocystin/Polyductin Modulates Renal Tubular Formation by Regulating Polycystin-2 Expression and Function

Fibrocystin/Polyductin Modulates Renal Tubular Formation by Regulating Polycystin-2 Expression and Function

Ciliary dysfunction impairs beta-cell insulin secretion and promotes development of type 2 diabetes in rodents

Cilium-generated signaling and cilia-related disorders

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