COMPLEMENT AND CYTOKINE GENE-EXPRESSION IN CULTURED MICROGLIA DERIVED FROM POSTMORTEM HUMAN BRAINS

被引：213

作者：

WALKER, DG ^{[1
]}

KIM, SU ^{[1
]}

MCGEER, PL ^{[1
]}

机构：

[1] UNIV BRITISH COLUMBIA,DEPT MED,DIV NEUROL,VANCOUVER,BC V6T 1W5,CANADA

来源：

JOURNAL OF NEUROSCIENCE RESEARCH | 1995年 / 40卷 / 04期

关键词：

MICROGLIA; ALZHEIMER DISEASE; CYTOKINE; COMPLEMENT; POLYMERASE CHAIN REACTION;

D O I：

10.1002/jnr.490400407

中图分类号：

Q189 [神经科学];

学科分类号：

071006 ;

摘要：

Microglia were successfully cultured from human brain tissue from normal and neurologically diseased cases obtained 3.5-10 hours postmortem. Final cell preparations were more than 99% pure as judged by latex bead phagocytosis, expression of microglial phenotypic markers, and absence of astrocytic markers. The expression of complement genes C1qB, C3, and C4 as well as genes for interleukin-(IL-)1 alpha, IL-1 beta, IL-6, tumor necrosis factor (TNF)alpha, IL-1 receptor antagonist, and transforming growth factor beta, but not inducible nitric oxide synthase, by these cells was detected by polymerase chain reaction (PCR) analysis. The pattern of gene expression was evaluated following stimulation of the cells with lipopolysaccharide, phorbol myristate acetate, gamma interferon, and beta amyloid peptide. There was considerable variation in gene response to these activating agents. However, it was of interest that beta-amyloid peptide (1-40) increased the expression of IL-1 beta mRNA in these cells. The number of cases in this study was too small to permit evaluation of microglial response according to the disease state, but the results demonstrate the potential for such studies in the future. (C) 1995 Wiley-Liss, Inc.

引用

页码：478 / 493

页数：16

共 77 条

[1] THE PROTEASE INHIBITOR, ALPHA-1-ANTICHYMOTRYPSIN, IS A COMPONENT OF THE BRAIN AMYLOID DEPOSITS IN NORMAL AGING AND ALZHEIMERS-DISEASE [J].

ABRAHAM, CR ;

POTTER, H .

ANNALS OF MEDICINE, 1989, 21 (02) :77-81

[2] MAJOR HISTOCOMPATIBILITY COMPLEX ANTIGEN EXPRESSION ON RAT MICROGLIA FOLLOWING EPIDURAL KAINIC ACID LESIONS [J].

AKIYAMA, H ;

ITAGAKI, S ;

MCGEER, PL .

JOURNAL OF NEUROSCIENCE RESEARCH, 1988, 20 (02) :147-157

[3] BETA-AMYLOID STIMULATES GLIAL-CELLS INVITRO TO PRODUCE GROWTH-FACTORS THAT ACCUMULATE IN SENILE PLAQUES IN ALZHEIMERS-DISEASE [J].

ARAUJO, DM ;

COTMAN, CW .

BRAIN RESEARCH, 1992, 569 (01) :141-145

[4] CYTOTOXICITY OF MICROGLIA [J].

BANATI, RB ;

GEHRMANN, J ;

SCHUBERT, P ;

KREUTZBERG, GW .

GLIA, 1993, 7 (01) :111-118

[5] EARLY AND RAPID DE-NOVO SYNTHESIS OF ALZHEIMER BETA-A4-AMYLOID PRECURSOR PROTEIN (APP) IN ACTIVATED MICROGLIA [J].

BANATI, RB ;

GEHRMANN, J ;

CZECH, C ;

MONNING, U ;

JONES, LL ;

KONIG, G ;

BEYREUTHER, K ;

KREUTZBERG, GW .

GLIA, 1993, 9 (03) :199-210

[6] INTERLEUKIN-1 AND TUMOR NECROSIS FACTOR-MEDIATED REGULATION OF C3 GENE-EXPRESSION IN HUMAN ASTROGLIOMA CELLS [J].

BARNUM, SR ;

JONES, JL ;

BENVENISTE, EN .

GLIA, 1993, 7 (03) :225-236

[7]

BELT KT, 1984, CELL, V36, P907

[8] MICROGLIAL-PRODUCED NITRIC-OXIDE AND REACTIVE NITROGEN-OXIDES MEDIATE NEURONAL CELL-DEATH [J].

BOJE, KM ;

ARORA, PK .

BRAIN RESEARCH, 1992, 587 (02) :250-256

[9]

BOYLE EA, 1990, AM J PATHOL, V137, P575

[10] INTERLEUKIN-6 IS THE MAJOR REGULATOR OF ACUTE PHASE PROTEIN-SYNTHESIS IN ADULT HUMAN HEPATOCYTES [J].

CASTELL, JV ;

GOMEZLECHON, MJ ;

DAVID, M ;

ANDUS, T ;

GEIGER, T ;

TRULLENQUE, R ;

FABRA, R ;

HEINRICH, PC .

FEBS LETTERS, 1989, 242 (02) :237-239

← 1 2 3 4 5 6 7 8 →