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New functions of B9D2 in tight junctions and epithelial polarity

Ciliopathies are a diverse group of disorders resulting from abnormalities in the development or function of multiple organs. While significant research has clarified the role of the primary cilium in transducing numerous signalling pathways, elucidating causes of neuronal and skeletal development d...

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Published in:	Scientific reports 2024-10, Vol.14 (1), p.25293-15, Article 25293
Main Authors:	Caenen-Braz, Chloe, Bouzhir, Latifa, Dupuis-Williams, Pascale
Format:	Article
Language:	English
Subjects:	631/136 631/80 Abnormalities, Multiple - genetics Abnormalities, Multiple - metabolism Abnormalities, Multiple - pathology Animals B9 domain proteins Bile ducts morphogenesis Cell Polarity Cerebellum - abnormalities Cerebellum - metabolism Cerebellum - pathology Cilia - metabolism Ciliary Motility Disorders Ciliopathy Congenital defects Encephalocele Epithelial Cells - metabolism Epithelial Cells - pathology Eye Abnormalities - genetics Eye Abnormalities - metabolism Eye Abnormalities - pathology Hedgehog protein Humanities and Social Sciences Humans Investigations Kidney Diseases, Cystic - genetics Kidney Diseases, Cystic - metabolism Kidney Diseases, Cystic - pathology Kidneys Liver Liver diseases Localization MARVEL Domain Containing 2 Protein - genetics MARVEL Domain Containing 2 Protein - metabolism Mice Microscopy multidisciplinary Mutation Nervous system Neurodevelopmental disorders Phenotypes Polycystic Kidney Diseases Proteins Retina - abnormalities Retina - metabolism Retinitis Pigmentosa - genetics Retinitis Pigmentosa - metabolism Retinitis Pigmentosa - pathology Science Science (multidisciplinary) Signal Transduction Tight junctions Tight Junctions - metabolism
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description	Ciliopathies are a diverse group of disorders resulting from abnormalities in the development or function of multiple organs. While significant research has clarified the role of the primary cilium in transducing numerous signalling pathways, elucidating causes of neuronal and skeletal development disorders, the origins of other ciliopathy-related conditions, such as hepatic fibrocystic diseases, remain elusive. Additionally, attempts to correlate specific ciliary proteins with distinct phenotypes have been largely unsuccessful due to the variable and overlapping symptoms of ciliopathies. This study aims to elucidate the extraciliary roles of the protein B9D2 in the development of biliary dysgenesis, a condition present in Meckel-Gruber and Joubert syndromes caused by mutations in this protein. Traditionally, B9D2 is known for its role at the transition zone of the primary cilium in the transduction of signalling pathways notably Wingless and Hedgehog. Our work demonstrates that before ciliogenesis occurs, B9D2 is crucial for the maturation and maintenance of tight junctions ensuring epithelial barrier tightness and appropriate biliary lumen formation. This study provides new insights into the mechanisms underlying biliary dysgenesis in hepatic ciliopathies, suggesting that further exploration of the non-ciliary functions of proteins involved in ciliopathies could lead to a better understanding and treatment of these complex disorders.
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While significant research has clarified the role of the primary cilium in transducing numerous signalling pathways, elucidating causes of neuronal and skeletal development disorders, the origins of other ciliopathy-related conditions, such as hepatic fibrocystic diseases, remain elusive. Additionally, attempts to correlate specific ciliary proteins with distinct phenotypes have been largely unsuccessful due to the variable and overlapping symptoms of ciliopathies. This study aims to elucidate the extraciliary roles of the protein B9D2 in the development of biliary dysgenesis, a condition present in Meckel-Gruber and Joubert syndromes caused by mutations in this protein. Traditionally, B9D2 is known for its role at the transition zone of the primary cilium in the transduction of signalling pathways notably Wingless and Hedgehog. 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subjects	631/136 631/80 Abnormalities, Multiple - genetics Abnormalities, Multiple - metabolism Abnormalities, Multiple - pathology Animals B9 domain proteins Bile ducts morphogenesis Cell Polarity Cerebellum - abnormalities Cerebellum - metabolism Cerebellum - pathology Cilia - metabolism Ciliary Motility Disorders Ciliopathy Congenital defects Encephalocele Epithelial Cells - metabolism Epithelial Cells - pathology Eye Abnormalities - genetics Eye Abnormalities - metabolism Eye Abnormalities - pathology Hedgehog protein Humanities and Social Sciences Humans Investigations Kidney Diseases, Cystic - genetics Kidney Diseases, Cystic - metabolism Kidney Diseases, Cystic - pathology Kidneys Liver Liver diseases Localization MARVEL Domain Containing 2 Protein - genetics MARVEL Domain Containing 2 Protein - metabolism Mice Microscopy multidisciplinary Mutation Nervous system Neurodevelopmental disorders Phenotypes Polycystic Kidney Diseases Proteins Retina - abnormalities Retina - metabolism Retinitis Pigmentosa - genetics Retinitis Pigmentosa - metabolism Retinitis Pigmentosa - pathology Science Science (multidisciplinary) Signal Transduction Tight junctions Tight Junctions - metabolism
title	New functions of B9D2 in tight junctions and epithelial polarity
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