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Neuropathologic variation in frontotemporal dementia due to the intronic tau 10(+16) mutation.

作者信息

Lantos P L, Cairns N J, Khan M N, King A, Revesz T, Janssen J C, Morris H, Rossor M N

机构信息

Department of Neuropathology, Institute of Psychiatry, King's College London, UK.

出版信息

Neurology. 2002 Apr 23;58(8):1169-75. doi: 10.1212/wnl.58.8.1169.

Abstract

BACKGROUND

An increasing number of recently described tau mutations show considerable clinical heterogeneity. The assessment of this phenotypic variation is of vital importance in the differential diagnosis of neurodegenerative diseases.

OBJECTIVE

To assess the neuropathologic heterogeneity in a comprehensive study of 12 brains with a tau mutation at exon 10(+16) (C-to-T) splice site from 9 families.

METHODS

A comprehensive neuropathologic examination has been carried out, using a wide range of tau antibodies.

RESULTS

All brains showed frontotemporal atrophy of varying severity and pallor of the pigmented nuclei of the brainstem. The histologic changes were more extensive to include other cortical areas, the deep gray matter, and the white matter. The hallmark histologic lesions were the tau-positive neuronal and glial inclusions. In neurons, these ranged from typical neurofibrillary tangles through well-circumscribed inclusions to diffuse cytoplasmic staining. This tau pathology was complemented by the presence of large, abnormal achromatic neurons, neuronal loss, astrocytosis, and superficial status spongiosus.

CONCLUSION

The distribution, type, and severity of these histologic abnormalities varied not only from case to case but also within the same brain. These brains with a common tau mutation raise important differential diagnostic problems: cases in the past might have been misdiagnosed as corticobasal degeneration or even atypical Pick disease, disorders with similar, if not identical, phenotypic manifestations.

摘要

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