TY - JOUR
T1 - Glial cell degeneration and hypomyelination caused by overexpression of myelin proteolipid protein gene
AU - Kagawa, Tetsushi
AU - Ikenaka, Kazuhiro
AU - Inoue, Yoshiro
AU - Kuriyama, Shigeki
AU - Tsujii, Tadasu
AU - Nakao, Junji
AU - Nakajima, Kazunori
AU - Aruga, Jun
AU - Okano, Hideyuki
AU - Mikoshiba, Katsuhiko
N1 - Funding Information:
We wish to thank Drs. J. Cregor Sutcliffe and Klaus-Armin Nave for providing us with the P/p and DM-20 cDNA clones (~27 and pCll), and Dr. Steve E. Pfeiffer for providing us with the 01 monoclonal antibody and for helpful suggestions on immunohistochemical studies. We thank Dr. Anthony T. Campagnoni for his critical reading of this manuscript. This work was supported by a Grant-in-Aid for Scientific Research from the Ministry of Education and by a grant from the National Center for Nervous, Mental and Muscular Disorders of the Ministry of Health and Welfare.
PY - 1994/8
Y1 - 1994/8
N2 - Myelin proteolipid protein (PLP), the major myelin protein in the CNS, has been thought to function in myelin assembly. Thus, mutations within the gene coding for PLP (Plp) cause hypomyelination, such as the jimpy phenotype in mice and Pelizaeus-Merzbacher disease in humans. However, these mutants often exhibit premature death of oligodendrocytes, which form CNS myelin. To elucidate the functional roles of Pip gene products in the maturation and/or survival of oligodendrocytes, we produced transgenic mice overexpressing the Plp gene by introducing extra wild-type mouse Pip genes. Surprisingly, transgenic mice bearing 4 more Plp genes exhibited dysmyelination in the CNS, whereas those with 2 more Plp genes showed normal myelination at an early age (3 weeks after birth), but later developed demyelination. Overexpression of the Plp gene resulted in arrested maturation of oligodendrocytes, and the severity of arrest was dependent on the extent of overexpression. Overexpression also led to oligodendrocyte cell death, apparently caused by abnormal swelling of the Golgi apparatus. Thus, tight regulation of Plpgene expression is necessary for normal oligodendrocyte differentiation and survival, and its overexpression can be the cause of both dys- and demyelination.
AB - Myelin proteolipid protein (PLP), the major myelin protein in the CNS, has been thought to function in myelin assembly. Thus, mutations within the gene coding for PLP (Plp) cause hypomyelination, such as the jimpy phenotype in mice and Pelizaeus-Merzbacher disease in humans. However, these mutants often exhibit premature death of oligodendrocytes, which form CNS myelin. To elucidate the functional roles of Pip gene products in the maturation and/or survival of oligodendrocytes, we produced transgenic mice overexpressing the Plp gene by introducing extra wild-type mouse Pip genes. Surprisingly, transgenic mice bearing 4 more Plp genes exhibited dysmyelination in the CNS, whereas those with 2 more Plp genes showed normal myelination at an early age (3 weeks after birth), but later developed demyelination. Overexpression of the Plp gene resulted in arrested maturation of oligodendrocytes, and the severity of arrest was dependent on the extent of overexpression. Overexpression also led to oligodendrocyte cell death, apparently caused by abnormal swelling of the Golgi apparatus. Thus, tight regulation of Plpgene expression is necessary for normal oligodendrocyte differentiation and survival, and its overexpression can be the cause of both dys- and demyelination.
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U2 - 10.1016/0896-6273(94)90358-1
DO - 10.1016/0896-6273(94)90358-1
M3 - Article
C2 - 7520255
AN - SCOPUS:0028133486
SN - 0896-6273
VL - 13
SP - 427
EP - 442
JO - Neuron
JF - Neuron
IS - 2
ER -