Loss of Kindlin-1 causes skin atrophy and lethal neonatal intestinal epithelial dysfunction

Loss of Kindlin-1 causes skin atrophy and lethal neonatal intestinal epithelial dysfunction

Kindler Syndrome (KS), characterized by transient skin blistering followed by abnormal pigmentation, skin atrophy, and skin cancer, is caused by mutations in the FERMT1 gene. Although a few KS patients have been reported to also develop ulcerative colitis (UC), a causal link to the FERMT1 gene mutat...

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Veröffentlicht in:PLoS genetics 2008-12, Vol.4 (12), p.e1000289-e1000289
Hauptverfasser: Ussar, Siegfried, Moser, Markus, Widmaier, Moritz, Rognoni, Emanuel, Harrer, Christian, Genzel-Boroviczeny, Orsolya, Fässler, Reinhard
Format: Artikel
Sprache:eng
Schlagworte:
Animals
Animals, Newborn
Atrophy - metabolism
Atrophy - mortality
Atrophy - physiopathology
Biochemistry
Carrier Proteins - genetics
Carrier Proteins - metabolism
Cell Adhesion
Cell adhesion & migration
Cell Biology/Cell Adhesion
Cell Line
Cellular biology
Colitis, Ulcerative - metabolism
Colitis, Ulcerative - mortality
Colitis, Ulcerative - pathology
Colitis, Ulcerative - physiopathology
Colon
Dermatology/Pediatric Skin Diseases, including Genetic Diseases
Dermatology/Photodermatology and Skin Aging
Epithelium - metabolism
Epithelium - pathology
Epithelium - physiopathology
Gastroenterology and Hepatology/Inflammatory Bowel Disease
Gene Knockout Techniques
Genetics and Genomics/Disease Models
Genetics and Genomics/Genetics of Disease
Humans
Immunology/Immune Response
Intestines - metabolism
Intestines - pathology
Intestines - physiopathology
Mice
Mice, Knockout
Mutation
Proteins
Skin - metabolism
Skin - pathology
Skin - physiopathology
Skin Diseases, Genetic - metabolism
Skin Diseases, Genetic - mortality
Skin Diseases, Genetic - pathology
Skin Diseases, Genetic - physiopathology
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Zusammenfassung:Kindler Syndrome (KS), characterized by transient skin blistering followed by abnormal pigmentation, skin atrophy, and skin cancer, is caused by mutations in the FERMT1 gene. Although a few KS patients have been reported to also develop ulcerative colitis (UC), a causal link to the FERMT1 gene mutation is unknown. The FERMT1 gene product belongs to a family of focal adhesion proteins (Kindlin-1, -2, -3) that bind several beta integrin cytoplasmic domains. Here, we show that deleting Kindlin-1 in mice gives rise to skin atrophy and an intestinal epithelial dysfunction with similarities to human UC. This intestinal dysfunction results in perinatal lethality and is triggered by defective intestinal epithelial cell integrin activation, leading to detachment of this barrier followed by a destructive inflammatory response.
ISSN:1553-7404
1553-7390
1553-7404
DOI:10.1371/journal.pgen.1000289