DYSMYELINATION IN TRANSGENIC MICE RESULTING FROM EXPRESSION OF CLASS-I HISTOCOMPATIBILITY MOLECULES IN OLIGODENDROCYTES

Turnley, AM; Morahan, G; OKANO, H; Bernard, O; MIKOSHIBA, K; Allison, J; Bartlett, PF; Miller, JFAP

Author(s): Turnley, AM; Morahan, G; OKANO, H; Bernard, O; MIKOSHIBA, K; Allison, J; Bartlett, PF; Miller, JFAP;
Details: Publication Year 1991-10-10,Volume 353,Issue #6344,Page 566-569
Journal Title: NATURE
Publication Type: Journal Article
Abstract: MAJOR histocompatibility complex (MHC) molecules are not normally expressed in the central nervous system (CNS) 1-3. However, aberrant expression has been observed in multiple sclerosis lesions and could contribute to the destruction of myelin or the myelinating cells known as oligodendrocytes 4,5. The mechanism of cell damage associated with aberrant MHC molecule expression is unclear: for example, overexpression of class I (ref. 6) and class II (refs 7, 8) MHC molecules in pancreatic beta-cells in transgenic mice leads to nonimmune destruction of the cells and insulin-dependent diabetes mellitus. We have generated transgenic mice that express class I H-2K(b) MHC molecules, under the control of the myelin basic protein promoter, specifically in oligodendrocytes. Homozygous transgenic mice have a shivering phenotype, develop tonic seizures and die at 15-22 days. This phenotype, which we term 'wonky', is due to hypomyelination in the CNS, and not to involvement of the immune system. The primary defect appears to be a shortage of myelinating oligodendrocytes resulting from overexpression of the class I MHC molecules.
Publisher: MACMILLAN MAGAZINES LTD
Keywords: PANCREATIC BETA-CELLS; MYELIN BASIC-PROTEIN; MULTIPLE-SCLEROSIS; MHC MOLECULES; SCHWANN-CELLS; ANTIGENS; TOLERANCE; GENE; TRANSCRIPTION; INTERFERON
Publisher's Version: https://doi.org/10.1038/353566a0
Terms of Use/Rights Notice: Refer to copyright notice on published article.

Creation Date: 1991-10-10 12:00:00