REACTIVE MICROGLIA MACROPHAGES PHAGOCYTOSE AMYLOID PRECURSOR PROTEIN PRODUCED BY NEURONS FOLLOWING NEURAL DAMAGE

被引：88

作者：

SHIGEMATSU, K

MCGEER, PL

WALKER, DG

ISHII, T

MCGEER, EG

机构：

[1] UNIV BRITISH COLUMBIA,DEPT PSYCHIAT,KINSMEN LAB NEUROL RES,2255 WESBROOK MALL,VANCOUVER V6T 1W5,BC,CANADA

[2] PSYCHIAT RES INST TOKYO,DEPT ULTRASTRUCT,TOKYO 156,JAPAN

来源：

JOURNAL OF NEUROSCIENCE RESEARCH | 1992年 / 31卷 / 03期

关键词：

APP; AXON; KAINIC ACID; RAT; NEURAL DEGENERATION;

D O I：

10.1002/jnr.490310306

中图分类号：

Q189 [神经科学];

学科分类号：

071006 ;

摘要：

Kainic acid lesions of rat striatum caused an elevation of amyloid precursor protein (APP) immunoreactivity in neurons and neurites, some of which were then phagocytosed by reactive microglia/macrophages. Immunoexpression of APP was observed in neurites and neurons 1 day after the kainic injection. Four days after lesioning, immunoreactivity was still concentrated in thick and distorted neurites, but it began to appear in microglia/macrophages and in the tissue matrix. The cells were identified as microglia/macrophages by the phenotypic markers Ia (OX6), leukocyte common antigen (OX1), C3bi receptor (OX42), and macrophage marker (ED1). They were negative for the astrocytic marker glial fibrillary acidic protein (GFAP). APP immunoreactivity in these phagocytic cells was most prominent between 1 week and 1 month postlesioning. No extracellular amyloid fibrils were detectable. These results suggest that APP production is rapidly upregulated in damaged neurons and accumulates in degenerating axons. However, phagocytosis of APP by reactive microglia/macrophages in this rat model does not result in production of Alzheimer type amyloid deposits.

引用

页码：443 / 453

页数：11

共 44 条

[1] LOCALIZATION OF AMYLOID BETA-PROTEIN MESSENGER-RNA IN BRAINS FROM PATIENTS WITH ALZHEIMERS-DISEASE
BAHMANYAR, S
HIGGINS, GA
GOLDGABER, D
LEWIS, DA
MORRISON, JH
WILSON, MC
SHANKAR, SK
GAJDUSEK, DC
[J]. SCIENCE, 1987, 237 (4810) : 77 - 80
[2] THE AMYLOID PRECURSOR PROTEIN IS CONCENTRATED IN NEURONAL LYSOSOMES IN NORMAL AND ALZHEIMER-DISEASE SUBJECTS
BENOWITZ, LI
RODRIGUEZ, W
PASKEVICH, P
MUFSON, EJ
SCHENK, D
NEVE, RL
[J]. EXPERIMENTAL NEUROLOGY, 1989, 106 (03) : 237 - 250
[3] INSITU HYBRIDIZATION OF NUCLEUS BASALIS NEURONS SHOWS INCREASED BETA-AMYLOID MESSENGER-RNA IN ALZHEIMER-DISEASE
COHEN, ML
GOLDE, TE
USIAK, MF
YOUNKIN, LH
YOUNKIN, SG
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1988, 85 (04) : 1227 - 1231
[4] COLE GM, 1991, NEUROBIOL AGING, V12, P81
[5] CRAS P, 1990, AM J PATHOL, V137, P241
[6] ANTISERUM RAISED AGAINST A SUBSEQUENCE OF ALZHEIMER AMYLOID PRECURSOR PROTEIN SELECTIVELY LABELS A SUBSET OF MICROGLIAL CELLS
CURRIE, J
BARCIKOWSKA, M
WEGIEL, J
MORYS, J
WISNIEWSKI, HM
[J]. JOURNAL OF NEUROPATHOLOGY AND EXPERIMENTAL NEUROLOGY, 1989, 48 (03) : 328 - 328
[7] DIJKSTRA CD, 1985, IMMUNOLOGY, V54, P589
[8] ALZHEIMERS-DISEASE AND DOWNS-SYNDROME - SHARING OF A UNIQUE CEREBROVASCULAR AMYLOID FIBRIL PROTEIN
GLENNER, GG
WONG, CW
[J]. BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1984, 122 (03) : 1131 - 1135
[9] CHARACTERIZATION AND CHROMOSOMAL LOCALIZATION OF A CDNA-ENCODING BRAIN AMYLOID OF ALZHEIMERS-DISEASE
GOLDGABER, D
LERMAN, MI
MCBRIDE, OW
SAFFIOTTI, U
GAJDUSEK, DC
[J]. SCIENCE, 1987, 235 (4791) : 877 - 880
[10] DEMONSTRATION OF MICROGLIAL CELLS IN AND AROUND SENILE (NEURITIC) PLAQUES IN THE ALZHEIMER BRAIN - AN IMMUNOHISTOCHEMICAL STUDY USING A NOVEL MONOCLONAL-ANTIBODY
HAGA, S
AKAI, K
ISHII, T
[J]. ACTA NEUROPATHOLOGICA, 1989, 77 (06) : 569 - 575

← 1 2 3 4 5 →