FUKUYAMA CONGENITAL MUSCULAR DYSTROPHY: NEUROPATHOLOGY AND IMMUNOHISTOCHEMISTRY Qin J1, Mizuguchi M2, Itoh M2, Takashima S2 1 Peking University First Hospital, Beijing, China 2 National Institute of Neuroscience, NCNP, Tokyo, Japan   Objective: To elucidate the neuropathological features of Fukuyama type congenital muscular dystrophy (FCMD) and the related immuno-expression in its cerebral cortices. Methods: Cerebral cortices of 8 FCMD cases were from the Brain Bank in the National Institute of Neuroscience, NCNP. Nine age-matched normal brains were obtained as a control group. H&E and Kluver-Barrera staining was used for the neuropathological study. For immunohoistochemical research, the antisera anti-DCX2 (specific to doublecortin protein) and anti-LIS1 (specific to LIS1 protein, responsible for Miller-Dieker syndrome ) were involved. Results: All FCMD brains showed malformations. Polymicrogyria was found in cerebral cortex in all, and in cerebellar cortices in 5 cases. Pachygyria was demonstrated in the fronto-parietal or cerebellar regions in 3 cases. In the control group, DCX immunoreactivity was detected predominantly in the fetal cerebral cortex, and only left weak immunoreactivity in pyramidal cells after birth. A similar expression of LIS1 to DCX2 was demonstrated The abnormal distribution of DCX immunolabeling was associated with neuronal disarrangement in FCMD. Conclusion: FCMD is a congenital disorder with brain malformation, particularly polymicrogyria and pachygyria, with an abnormal distribution of DCX expression, associated with neuronal disarrangement.

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