Intracytoplasmic inclusion bodies of the thalamus and the substantia nigra, and Marinesco bodies in myotonic dystrophy: a quantitative morphological study

Intracytoplasmic inclusion bodies of the thalamus and the substantia nigra, and Marinesco bodies have been studied in four patients with myotonic dystrophy (MyD), eight patients with other neurological diseases (control A), and eight patients without neurological diseases (control B). The percentage...

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Bibliographic Details
Published in:Acta neuropathologica 1989-01, Vol.77 (4), p.350-356
Main Authors: Ono, S, Inoue, K, Mannen, T, Mitake, S, Shirai, T, Kanda, F, Jinnai, K, Takahashi, K
Format: Article
Language:English
Subjects:
Adult
Aged
Female
Humans
Inclusion Bodies - pathology
Inclusion Bodies - ultrastructure
Male
Microscopy, Electron
Middle Aged
Myotonic Dystrophy - pathology
Substantia Nigra - pathology
Substantia Nigra - ultrastructure
Thalamus - pathology
Thalamus - ultrastructure
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Summary:Intracytoplasmic inclusion bodies of the thalamus and the substantia nigra, and Marinesco bodies have been studied in four patients with myotonic dystrophy (MyD), eight patients with other neurological diseases (control A), and eight patients without neurological diseases (control B). The percentages of the affected cells were calculated by dividing the number of neurons including intracytoplasmic inclusion bodies of the thalamus and the substantia nigra, and Marinesco bodies, by the total cell count in these respective regions. Statistical analyses were performed with regard to the frequency of these bodies by using Student's t test. There was a significantly higher incidence of intracytoplasmic inclusion bodies of the thalamus (13.2% versus 0.7%, P less than 0.001) and the substantia nigra (20.4% versus 2.7%, P less than 0.001), and Marinesco bodies (37.4% versus 4.1%, P less than 0.001) in patients with MyD than in controls A and B. From our observations, it is suggested that the presence with a high frequency, in combination, of these bodies is not an incidental finding but may have an intimate and important relationship with the pathogenesis of MyD, and may be a conspicuous and diagnostically important feature of MyD.
ISSN:0001-6322
1432-0533
DOI:10.1007/bf00687369