Widespread expression of the peripheral myelin protein‐22 gene (pmp22) in neural and non‐neural tissues during murine development
- 15 December 1995
- journal article
- Published by Wiley in Journal of Neuroscience Research
- Vol. 42 (6), 733-741
- https://doi.org/10.1002/jnr.490420602
Abstract
The gene encoding the peripheral myelin protein PMP22 is affected by various mutations in the hereditary peripheral neuropathies Charcot‐Marie‐Tooth disease type 1A (CMT1A), Déjérine‐Sottas syndrome (DSS) and hereditary neuropathy with liability to pressure palsies (HNPP). In contrast to the recent remarkable progress in the genetics of the PMP22 gene, the biological function of PMP22 remains largely unknown. In this report, we have confirmed by using in situ hybridization techniques that high levels of PMP22 niRNA are present in maturing peripheral nerves of the 2‐week‐old mouse, a finding consistent with the PNS‐specific defect observed in hereditary peripheral neuropathies. However, high levels of PMP22 transcripts were also found in the villi of the adult gut, and PMP22 expression was detected in various non‐neural tissues during embryonic mouse development. In early embryogenesis (9.5 days postconception, dpc), PMP22 RNA expression appears restricted to the epithelial ectodermal layer. During early organogenesis (11.5 dpc), particularly high levels of expression are present in the capsule surrounding the liver and in the forming gut, while low levels of PMP22 mRNA can be fund in precartilagous condensations forming the vertebrae and the ventricular layer of the myelencephalon. During midgestation development (14.5 dpc to 16.5 dpc), the number of PMP22‐positive tissues increases, and high expression is detected in several mesoderm‐derived tissues, in particular connective tissues of the face region, bones including the vertebrae, the lung mesenchym, and in muscles. In addition, high expression is also found in ectoderm‐derived tissues, especially the epithelia of the lens and the skin. These findings strongly suggest that PMP22 serves not only a PNSspecific function but is also of broader biological significance in cell proliferation and/or differentiation. ©1995 Wiley‐Liss, Inc.Keywords
This publication has 31 references indexed in Scilit:
- Biology and Genetics of Hereditary Motor and Sensory NeuropathiesAnnual Review of Neuroscience, 1995
- Peripheral myelin protein 22: Facts and hypothesesJournal of Neuroscience Research, 1995
- Charcot-Marie-tooth disease: a new paradigm for the mechanism of inherited diseaseTrends in Genetics, 1994
- Differential expression of two mRNA species indicates a dual function of peripheral myelin protein PMP22 in cell growth and myelinationJournal of Neuroscience Research, 1994
- Two autosomal dominant neuropathies result from reciprocal DNA duplication/deletion of a region on chromosome 17Human Molecular Genetics, 1994
- Dejerine–Sottas syndrome associated with point mutation in the peripheral myelin protein 22 (PMP22) geneNature Genetics, 1993
- Progress in the molecular understanding of hereditary peripheral neuropathies reveals new insights into the biology of the peripheral nervous systemTrends in Neurosciences, 1993
- Coexpression of PMP22 gene with MBP and P0 during de novo myelination and nerve repairGlia, 1993
- Long Lives for Homozygous Trembler Mutant Mice Despite Virtual Absence of Peripheral Nerve MyelinScience, 1988
- Detection of mRNAs in sea urchin embryos by in situ hybridization using asymmetric RNA probesDevelopmental Biology, 1984