Your search keyword '"IFT144"' showing total 7 results

1. Identification of the primary ciliary proteins IFT38 and IFT144 to enhance serum-mediated YAP activation and cell proliferation.

Author

Yu, Jae-Hyun, Kim, Jeong Heon, Soung, Nak-Kyun, Moon, Eun-Yi, and Koo, Ja Hyun

Subjects

*CILIA & ciliary motion, *YAP signaling proteins, *MITOGENS, *CELL proliferation, *HIPPO signaling pathway, *G protein coupled receptors, *CELL growth

Abstract

Primary cilia are essential cellular antennae that transmit external signals into intracellular responses. These sensory organelles perform crucial tasks in triggering intracellular signaling pathways, including those initiated by G protein-coupled receptors (GPCRs). Given the involvement of GPCRs in serum-induced signaling, we investigated the contribution of ciliary proteins in mitogen perception and cell proliferation. We found that depletion of cilia via IFT88 silencing impaired cell growth and repressed YAP activation against serum and its mitogenic constituents, namely lysophosphatidic acid (LPA) and sphingosine 1-phosphate (S1P). To identify the key player of serum mitogen signaling, a mutant cell line library with 30 ablated individual ciliary proteins was established and screened based on YAP dephosphorylation and target gene induction. While 9 of them had altered signaling, ablation of IFT38 or IFT144 led to a particularly robust repression of YAP activation upon LPA and S1P. The deficiency of IFT38 and IFT144 attenuated cell proliferation, as corroborated in either 2-dimensional cultures or tumor spheroids. In subcutaneous skin melanoma patients, expression of IFT38 and IFT144 was associated with unfavorable outcomes in overall survival. In conclusion, our study demonstrates the involvement of ciliary proteins in mitogen signaling and identifies the regulatory roles of IFT38 and IFT144 in serum-mediated Hippo pathway signaling and cellular growth. • Cellular sensitivity to serum mitogens is controlled by primary cilia. • Functional comparison of ciliary proteins was done using CRISPRi cell line library. • IFT38 and IFT144 were identified as crucial components for serum mitogen perception. • Silencing IFT38 and IFT144 leads to reduced tumor spheroid growth. [ABSTRACT FROM AUTHOR]

Published

2023

2. Stargardt-like Clinical Characteristics and Disease Course Associated with Variants in the WDR19 Gene.

Author

Sajovic, Jana, Meglič, Andrej, Volk, Marija, Maver, Aleš, Jarc-Vidmar, Martina, Hawlina, Marko, and Fakin, Ana

Subjects

*DISEASE progression, *PERIMETRY, *STARGARDT disease, *OPTICAL coherence tomography, *GENETIC variation, *COLOR vision

Abstract

Variants in WDR19 (IFT144) have been implicated as another possible cause of Stargardt disease. The purpose of this study was to compare longitudinal multimodal imaging of a WDR19-Stargardt patient, harboring p.(Ser485Ile) and a novel c.(3183+1_3184-1)_(3261+1_3262-1)del variant, with 43 ABCA4-Stargardt patients. Age at onset, visual acuity, Ishihara color vision, color fundus, fundus autofluorescence (FAF), spectral-domain optical coherence tomography (OCT) images, microperimetry and electroretinography (ERG) were evaluated. First symptom of WDR19 patient was nyctalopia at the age of 5 years. After the age of 18 years, OCT showed hyper-reflectivity at the level of the external limiting membrane/outer nuclear layer. There was abnormal cone and rod photoreceptor function on ERG. Widespread fundus flecks appeared, followed by perifoveal photoreceptor atrophy. Fovea and peripapillary retina remained preserved until the latest exam at 25 years of age. ABCA4 patients had median age of onset at 16 (range 5–60) years and mostly displayed typical Stargardt triad. A total of 19% had foveal sparing. In comparison to ABCA4 patients, the WDR19 patient had a relatively large foveal preservation and severe rod photoreceptor impairment; however, it was still within the ABCA4 disease spectrum. Addition of WDR19 in the group of genes producing phenocopies of Stargardt disease underlines the importance of genetic testing and may help to understand its pathogenesis. [ABSTRACT FROM AUTHOR]

Published

2023

3. Stargardt-like Clinical Characteristics and Disease Course Associated with Variants in the WDR19 Gene

Author

Jana Sajovic, Andrej Meglič, Marija Volk, Aleš Maver, Martina Jarc-Vidmar, Marko Hawlina, and Ana Fakin

Subjects

Stargardt disease, WDR19, Genetics, phenocopy, Stargardt-like disease, ABCA4, Genetics (clinical), IFT144, fundus flavimaculaus

Abstract

Variants in WDR19 (IFT144) have been implicated as another possible cause of Stargardt disease. The purpose of this study was to compare longitudinal multimodal imaging of a WDR19-Stargardt patient, harboring p.(Ser485Ile) and a novel c.(3183+1_3184-1)_(3261+1_3262-1)del variant, with 43 ABCA4-Stargardt patients. Age at onset, visual acuity, Ishihara color vision, color fundus, fundus autofluorescence (FAF), spectral-domain optical coherence tomography (OCT) images, microperimetry and electroretinography (ERG) were evaluated. First symptom of WDR19 patient was nyctalopia at the age of 5 years. After the age of 18 years, OCT showed hyper-reflectivity at the level of the external limiting membrane/outer nuclear layer. There was abnormal cone and rod photoreceptor function on ERG. Widespread fundus flecks appeared, followed by perifoveal photoreceptor atrophy. Fovea and peripapillary retina remained preserved until the latest exam at 25 years of age. ABCA4 patients had median age of onset at 16 (range 5–60) years and mostly displayed typical Stargardt triad. A total of 19% had foveal sparing. In comparison to ABCA4 patients, the WDR19 patient had a relatively large foveal preservation and severe rod photoreceptor impairment; however, it was still within the ABCA4 disease spectrum. Addition of WDR19 in the group of genes producing phenocopies of Stargardt disease underlines the importance of genetic testing and may help to understand its pathogenesis.

Published

2023

4. Mutations in WDR19 encoding the intraflagellar transport component IFT144 cause a broad spectrum of ciliopathies.

Author

Fehrenbach, Henry, Decker, Christian, Eisenberger, Tobias, Frank, Valeska, Hampel, Tobias, Walden, Ulrike, Amann, Kerstin, Krüger-Stollfuß, Ingrid, Bolz, Hanno, Häffner, Karsten, Pohl, Martin, and Bergmann, Carsten

Subjects

*CILIOPATHY, *CELLS, *GENETIC mutation, *PHENOTYPES, *SHORT-rib polydactyly syndrome

Abstract

Background: An emerging number of clinically and genetically heterogeneous diseases now collectively termed ciliopathies have been connected to the dysfunction of primary cilia. We describe an 8-year-old girl with a complex phenotype that did not clearly match any familiar syndrome. Case-Diagnosis/Treatment: Hypotonia, facial dysmorphism and retardation were noted shortly after birth. Other features included short stature, mild skeletal anomalies, strabism, deafness, subdural hygroma, hepatosplenomegaly and end-stage renal failure. Renal biopsy revealed tubular atrophy, interstitial fibrosis and segmental glomerulosclerosis. After exclusion of a chromosomal abnormality by array-comparative genomic hybridization (CGH), we performed next-generation sequencing (NGS) using a customized panel that targeted 131 genes known or hypothesized to cause ciliopathies. We identified the novel homozygous WDR19 mutation c.1483G > C (p.Gly495Arg) that affects an evolutionarily highly conserved residue in the intraflagellar transport protein IFT144, is absent from databases and is predicted to be pathogenic by all bioinformatic sources used. Conclusion: Mutations in WDR19 encoding the intraflagellar transport component IFT144 have recently been described in single families with the clinically overlapping skeletal ciliopathies Jeune and Sensenbrenner syndromes, combined or isolated nephronophthisis (NPHP) and retinitis pigmentosa (RP) (Senior-Loken syndrome). Our patient emphasizes the usefulness and efficiency of a comprehensive NGS panel approach in patients with unclassified ciliopathies. It further suggests that WDR19 mutations can cause a broad spectrum of ciliopathies that extends to Jeune and Sensenbrenner syndromes, RP and renal NPHP-like phenotypes. [ABSTRACT FROM AUTHOR]

Published

2014

5. IFT144 and mild retinitis pigmentosa in Mainzer-Saldino syndrome: A new association

Author

Montolío-Marzo S, Català-Mora J, Madrid-Aris Á, Armstrong J, Diaz-Carcajosa J, and Carreras E

Subjects

Retinitis pigmentosa, genetic structures, Intraflagellar transport, Ciliopathy, IFT144, sense organs, eye diseases, Mainzer-saldino syndrome

Abstract

Ciliopathies are a wide and heterogeneous group of diseases affecting intraflagellar transport. Among them, Mainzer-Saldino syndrome (MSS) shows phalangeal cone-shaped epiphysis, renal disease and retinal involvement. Short stature, cerebellar ataxia and hepatic fibrosis might also be found. IFT140 is the most commonly reported mutation in MSS. We will report on the case of a patient with a clinical diagnosis of Mainzer-Saldino syndrome due to IFT144 dysfunction. This mutation has not been previously related to MSS but it has been found in other ciliopathies and both syndromic and non-syndromic retinitis pigmentosa. At birth our patient showed trigonocephaly, early progressive renal failure requiring transplant, intrahepatic biliary duct dilation, cone-shaped epiphyses, growth retardation and retinitis pigmentosa with mild ophthalmic impairment. The best corrected visual acuity reached 0.15/0.22 LogMAR. The posterior pole showed abnormal macular reflex, mild vascular attenuation in the periphery and diffuse pigmentary changes. Autofluorescence showed bull's eye signal increase. Computerized optic tomography assessed the absence of external retinal layers in the extrafoveal macula. In conclusion, IFT144 genetic study may be involved in MSS and thus must be considered for diagnosis. Mild ophthalmic symptomatology despite early onset retinitis pigmentosa in the context of MSS has been found in this case caused by IFT144 mutation.

Published

2020

6. WDR19: An ancient, retrograde, intraflagellar ciliary protein is mutated in autosomal recessive retinitis pigmentosa and in Senior-Loken syndrome.

Author

Coussa, R G, Otto, E A, Gee, H‐Y, Arthurs, P, Ren, H, Lopez, I, Keser, V, Fu, Q, Faingold, R, Khan, A, Schwartzentruber, J, Majewski, J, Hildebrandt, F, and Koenekoop, R K

Subjects

*RETINITIS pigmentosa, *BLINDNESS, *GENOTYPE-environment interaction, *VISION disorders, *RETINAL degeneration, *SINGLE nucleotide polymorphisms, *THERAPEUTICS

Abstract

Autosomal recessive retinitis pigmentosa ( arRP) is a clinically and genetically heterogeneous retinal disease that causes blindness. Our purpose was to identify the causal gene, describe the phenotype and delineate the mutation spectrum in a consanguineous Quebec arRP family. We performed Arrayed Primer Extension ( APEX) technology to exclude ∼500 arRP mutations in ∼20 genes. Homozygosity mapping [single nucleotide polymorphism ( SNP) genotyping] identified 10 novel significant homozygous regions. We performed next generation sequencing and whole exome capture. Sanger sequencing provided cosegregation. We screened another 150 retinitis pigmentosa ( RP) and 200 patients with Senior-Løken Syndrome ( SLS). We identified a novel missense mutation in WDR19, c.2129T>C which lead to a p. Leu710Ser. We found the same mutation in a second Quebec arRP family. Interestingly, two of seven affected members of the original family developed 'sub-clinical' renal cysts. We hypothesized that more severe WDR19 mutations may lead to severe ciliopathies and found seven WDR19 mutations in five SLS families. We identified a new gene for both arRP and SLS. WDR19 is a ciliary protein associated with the intraflagellar transport machinery. We are currently investigating the full extent of the mutation spectrum. Our findings are crucial in expanding the understanding of childhood blindness and identifying new genes. [ABSTRACT FROM AUTHOR]

Published

2013

7. Functional analysis of candidate genes affecting Hoxa10 activity

Author

Mesquita, André Daniel Faustino, Perez, Moises Mallo, and Thorsteinsdóttir, Sólveig, 1962

Subjects

Hox genes, Teses de mestrado - 2017, Grg3, Departamento de Biologia Animal, IFT144, Motivo C1, Smad4

Abstract

Tese de mestrado, Biologia Evolutiva e do Desenvolvimento, Universidade de Lisboa, Faculdade de Ciências, 2017 Submitted by Teresa Boa (tdboa@fc.ul.pt) on 2018-01-08T16:44:26Z No. of bitstreams: 1 ulfc121567_tm_André_Mesquita.pdf: 2903439 bytes, checksum: cd298aa2eb6e790dd5dd2fbd97046eaa (MD5) Made available in DSpace on 2018-01-08T16:44:37Z (GMT). No. of bitstreams: 1 ulfc121567_tm_André_Mesquita.pdf: 2903439 bytes, checksum: cd298aa2eb6e790dd5dd2fbd97046eaa (MD5) Previous issue date: 2017

Published

2017