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HISTOPATHOLOGICAL STUDIES ON ASTROCYTE IN VARIOUS LIVER DISEASES : A STUDY OF ALZHEIMER GLIA TYPE II Hideki Kida 1 , Aturo Jimi 1 , Kazuo Anegawa 2 , Michio Oumaru 3 , Masaru Tomimatu 3 , Youichirou Inoue 3 , Muneyasu Shirouzu 3 , Shigemi Anraku 4 1The First Department of Pathology Kurume University School of Medicine 2The First Department of Internal Medicine, Kurume University School of Medicine 3Department of Psychiatry Kurume University School of Medicine 4Institute of Brain Diseases, Kurume University School of Medicine pp.1275-1281
Published Date 1980/12/1
DOI https://doi.org/10.11477/mf.1406204690
  • Abstract
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In order to study the histopathological changes of astrocyte in liver diseases, 72 autopsy cases of various liver diseases such as liver cirrhosis, hepato-cellular carcinoma, acute hepatic necrosis, and etc., except for Wilson's disease were studied and 15 cases without liver lesion were studied as a control. Alzheimer glia type II (A-II glia) was found in 62 cases out of 72 cases with liver disease and 5 cases among 15 control cases. Statistically, a significant difference of the incidence of A-II glia was seen between the cases with liver disease and control group (p<0.01). Histological changes of A-II glia were classified into three stages according to Stadler's staging.

In the cases with liver disease, A-II glias of stage II and III were predominant, whereas in control group stage I was predominant with a statistic significance (p<0.01). In most cases with liver disease, A-II glia was remarkably seen in corpus striatum and dentate nuclei with a significant dif-ference of that in cerebral cortex (p<0.01).

In liver cirrhosis of Miyake's type A, A-II gliasof stage III were predominant, whereas in liver cirrhosis Miyake's type B A-II glias of stage II were predominant, and in the cases of acute hepatic necrosis A-II glias of stage I were predominant. In general, stronger degeneration of astrocyte was recognized in the cases of cirrhosis without hepa-tocellular carcinoma than in the cases with hepa-tocellular carcinoma.

There was no relationship between the size of primary and or metastatic hepatic tumors and the incidence and the stage of A-II glias. In concern to the incidence and the stage of A-II glias, no significant difference was seen between metastatic hepatic tumors and hepatocellular carcinoma.

There was no relationship between spleen weight and A-II glia.

Furthermore, no relationship was seen between esophageal varices and A-II glia. There was a close relationship between A-II glia and conscious-ness disturbance, especially, in the cases presenting prolonged or repeated consciousness disturbance.

There was a positive correlation between serum ammonia levels, and the incidence and the stage of A-II glia. Also, there was relationship between ICG (or BSP) test and A-II glia.

No relationship was seen between serum trans-aminase and A-II glia, and between blood sugar levels and A-II glia, and between BUN and A-II glia.


Copyright © 1980, Igaku-Shoin Ltd. All rights reserved.

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電子版ISSN 2185-405X 印刷版ISSN 0006-8969 医学書院

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