Chromosomal Mapping of the Human M6 Genes |
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| Authors: | S. Olinsky B. T. Loop A. DeKosky B. Ripepi W. Weng J. Cummins S. L. Wenger Y. Yan C. Lagenaur V. Narayanan |
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| Affiliation: | aThe Children's Hospital of Pittsburgh, University of Pittsburgh, Pittsburgh, Pennsylvania, 15213;bDepartment of Pediatrics, University of Pittsburgh, Pittsburgh, Pennsylvania, 15213;eDepartment of Neurology, University of Pittsburgh, Pittsburgh, Pennsylvania, 15213;dDepartment of Neurobiology, University of Pittsburgh, Pittsburgh, Pennsylvania, 15213;cDepartment of Human Genetics, University of Pittsburgh, Pittsburgh, Pennsylvania, 15213 |
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| Abstract: | M6 is a neuronal membrane glycoprotein that may have an important role in neural development. This molecule was initially defined by a monoclonal antibody that affected the survival of cultured cerebellar neurons and the outgrowth of neurites. The nature of the antigen was discovered by expression cDNA cloning using this monoclonal antibody. Two distinct murine M6 cDNAs (designated M6a and M6b) whose deduced amino acid sequences were remarkably similar to that of the myelin proteolipid protein were previously isolated. We have isolated partial human cDNA and genomic clones encoding M6a and M6b and have characterized them by restriction mapping, Southern hybridization with cDNA probes, and sequence analysis. We have localized these genes within the human genome by FISH (fluorescencein situhybridization). The human M6a gene is located at 4q34, and the M6b gene is located at Xp22.2. A number of human neurological disorders have been mapped to the Xp22 region, including Aicardi syndrome (MIM 304050), Rett syndrome (MIM 312750), X-linked Charcot–Marie–Tooth neuropathy (MIM 302801), and X-linked mental retardation syndromes (MRX1, MIM 309530). This raises the possibility that a defect in the M6b gene is responsible for one of these neurological disorders. |
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