Pathological dynamics of activated microglia following medial forebrain bundle transection

被引：80

作者：

Cho, BP

Song, DY

Sugama, S

Shin, DH

Shimizu, Y

Kim, SS

Kim, YS

Joh, TH

机构：

[1] Cornell Univ, Weill Med Coll, Dept Neurol & Neurosci, Burke Med Res Inst,Lab Mol Neurobiol, White Plains, NY 10605 USA

[2] Yonsei Univ, Wonju Coll Med, Dept Anat, Wonju, South Korea

[3] Yonsei Univ, Wonju Coll Med, Inst Basic Med Sci, Wonju, South Korea

[4] Nippon Med Coll, Dept Physiol 2, Tokyo 113, Japan

[5] Keimyung Univ, Sch Med, Dept Prevent Med, Taegu 700310, South Korea

[6] Keimyung Univ, Sch Med, Inst Brain, Taegu 700310, South Korea

[7] Kangwon Natl Univ, Coll Med, Dept Pharmacol, Chunchon, South Korea

来源：

GLIA | 2006年 / 53卷 / 01期

关键词：

axotomy; phagocytosis; ED1; MHC II; migration; dopaminergic neuron; Parkinson's disease;

D O I：

10.1002/glia.20265

中图分类号：

Q189 [神经科学];

学科分类号：

071006 ;

摘要：

To elucidate the role and pathological dynamics of activated microglia, this study assessed the phagocytic, immunophenotypic, morphological, and migratory properties of activated microglia in the medial forebrain bundle (MFB) axotomized rat brain. Activated microglia were identified using two different monoclonal antibodies: ED1 for phagocytic activity and OX6 for major histocompatibility complex (MHC) class H. Phagocytic microglia, characterized by ED1-immunoreactivity or ED1- and OX6-immunoreactivity, appeared in the MFB and substantia nigra (SN) as early as 1-3 days post-lesion (dpl), when there was no apparent loss of dopamine (DA) neurons. Thereafter, a great number of activated microglia selectively adhered to degenerating axons, dendrites and DA neuronal somas of the SN. This was followed by significant loss of these fibers and nigral DA neurons. Activation of microglia into phagocytic stage was most pronounced between 14-28 dpl and gradually subsided, but phagocytic microglia persisted until 70 dpl, the last time point examined. ED1 expression preceded MHC II expression in phagocytic microglia. All phagocytic microglia sticking to DA neurons showed activated but ramified form with enlarged somas and thickened processes. They were recruited to the SNc from cranial, dorsal and ventral aspects along various structures and finally stuck to DA neurons of the SNc. Characteristic rod-shaped microglia in the white matter were thought to migrate a long distance. The present study strongly suggests that neurons undergoing delayed neurodegeneration may be phagocytosed by numerous phagocytic, ramified microglia at various sites where specific surface signals are exposed or diffusible molecules are released. (c) 2005 Wiley-Liss, Inc.

引用

页码：92 / 102

页数：11

共 78 条

[1] EARLY RESPONSE OF BRAIN RESIDENT MICROGLIA TO KAINIC ACID-INDUCED HIPPOCAMPAL-LESIONS [J].

AKIYAMA, H ;

TOOYAMA, I ;

KONDO, H ;

IKEDA, K ;

KIMURA, H ;

MCGEER, EG ;

MCGEER, PL .

BRAIN RESEARCH, 1994, 635 (1-2) :257-268

[2]

Amat JA, 1996, GLIA, V16, P368, DOI 10.1002/(SICI)1098-1136(199604)16:4<368::AID-GLIA9>3.0.CO

[3]

2-W

[4] Glial pathology but absence of apoptotic nigral neurons in long-standing Parkinson's disease [J].

Banati, RB ;

Daniel, SE ;

Blunt, SB .

MOVEMENT DISORDERS, 1998, 13 (02) :221-227

[5] PHAGOCYTIC-ACTIVITY OF MACROPHAGES AND MICROGLIAL CELLS DURING THE COURSE OF ACUTE AND CHRONIC RELAPSING EXPERIMENTAL AUTOIMMUNE ENCEPHALOMYELITIS [J].

BAUER, J ;

SMINIA, T ;

WOUTERLOOD, FG ;

DIJKSTRA, CD .

JOURNAL OF NEUROSCIENCE RESEARCH, 1994, 38 (04) :365-375

[6] MESENCEPHALIC DOPAMINERGIC-NEURONS PROTECTED BY GDNF FROM AXOTOMY-INDUCED DEGENERATION IN THE ADULT BRAIN [J].

BECK, KD ;

VALVERDE, J ;

ALEXI, T ;

POULSEN, K ;

MOFFAT, B ;

VANDLEN, RA ;

ROSENTHAL, A ;

HEFTI, F .

NATURE, 1995, 373 (6512) :339-341

[7] DISPLACEMENT OF SYNAPTIC TERMINALS FROM REGENERATING MOTONEURONS BY MICROGLIAL CELLS [J].

BLINZING.K ;

KREUTZBE.G .

ZEITSCHRIFT FUR ZELLFORSCHUNG UND MIKROSKOPISCHE ANATOMIE, 1968, 85 (02) :145-&

[8] A QUANTITATIVE STUDY OF CELL-DEATH IN THE SUBSTANTIA-NIGRA FOLLOWING A MECHANICAL LESION OF THE MEDIAL FOREBRAIN-BUNDLE [J].

BRECKNELL, JE ;

DUNNETT, SB ;

FAWCETT, JW .

NEUROSCIENCE, 1995, 64 (01) :219-227

[9] REACTIVE NITROGEN INTERMEDIATES IN HUMAN NEUROPATHOLOGY - AN OVERVIEW [J].

BROSNAN, CF ;

BATTISTINI, L ;

RAINE, CS ;

DICKSON, DW ;

CASADEVALL, A ;

LEE, SC .

DEVELOPMENTAL NEUROSCIENCE, 1994, 16 (3-4) :152-161

[10] PATHOLOGICAL-CHANGES IN THE NUCLEUS OF MEYNERT IN ALZHEIMERS AND PARKINSONS DISEASES [J].

CANDY, JM ;

PERRY, RH ;

PERRY, EK ;

IRVING, D ;

BLESSED, G ;

FAIRBAIRN, AF ;

TOMLINSON, BE .

JOURNAL OF THE NEUROLOGICAL SCIENCES, 1983, 59 (02) :277-289

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