Basement membrane fragility underlies embryonic lethality in fukutin-null mice
pmid: 15837576
Basement membrane fragility underlies embryonic lethality in fukutin-null mice
Fukuyama-type congenital muscular dystrophy (FCMD), associated with brain malformation due to defects in neuronal migration, is caused by mutations in fukutin. Several lines of evidence suggest that the fukutin protein plays a pivotal role in synthesis of O-mannosyl sugar moieties of alpha-dystroglycan, a cell surface laminin receptor. Here, through targeted disruption of the orthologous mouse fukutin gene, we show that the fukutin protein is essential, as homozygous-null embryos die by E9.5 of gestation. Fukutin-null embryos show phenotypic diversity, features of which include growth retardation, folding of the egg cylinder, leakage of maternal red blood cells into the yolk sac cavity, and an increased number of apoptotic cells in the ectoderm. Loss of immunoreactivity against sugar moieties in alpha-dystroglycan suggests a reduced laminin-binding capacity. Ultrastructural analysis shows thin and breached basement membranes (BMs). BM fragility may underlie all of these abnormal phenotypes, and maintenance of BM function may require fukutin-mediated glycosylation of alpha-dystroglycan early in embryonic development.
- Fujita Health University Japan
- Osaka University Japan
- Osaka Gakuin University Japan
- Shimane University Japan
- Otsuka Pharmaceutical Indonesia
Mice, Knockout, Basement membrane, Glycosylation, Proteins, Neurosciences. Biological psychiatry. Neuropsychiatry, α-Dystroglycan, Basement Membrane, Mice, Inbred C57BL, Mice, Phenotype, Pregnancy, Transferases, Embryo Loss, fukutin, Animals, Female, Dystroglycans, Gene Deletion, RC321-571
Mice, Knockout, Basement membrane, Glycosylation, Proteins, Neurosciences. Biological psychiatry. Neuropsychiatry, α-Dystroglycan, Basement Membrane, Mice, Inbred C57BL, Mice, Phenotype, Pregnancy, Transferases, Embryo Loss, fukutin, Animals, Female, Dystroglycans, Gene Deletion, RC321-571
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