Deficient activation of microglia during optic nerve degeneration

Fanny Reichert; Shlomo Rotshenker

doi:10.1016/S0165-5728(96)00112-9

Deficient activation of microglia during optic nerve degeneration

Fanny Reichert, Shlomo Rotshenker

Institute for Medical Research Israel-Canada (IMRIC)

Research output: Contribution to journal › Article › peer-review

82 Scopus citations

Abstract

Transection of an optic nerve (ON) is follwed by slow removal of myelin. We studied microglia for the expression of molecules that characterize activated myelin phagocytosing macrophages: MAC-1, FcγII/III receptor (FcR), MAC-2, and F4/80. In-vitro, microglia expressed all molecules and phagocytosed myelin. In-vivo, intact ON displayed high levels of MAC-1, little FcR and F4/80, and no MAC-2. The expression of these molecules was upregulated differentially in in-vivo degenerating ON: MAC-1 uniformly, FcR and F4/80 variably, and MAC-2 sporadically. The distribution of MAC-2 expression correlated best with a pattern of sporadic structural degeneration. Thus in-vivo, ON injury is followed by deficient microglia activation, which we suggest contributes significantly to the slow clearance of myelin.

Original language	English
Pages (from-to)	153-161
Number of pages	9
Journal	Journal of Neuroimmunology
Volume	70
Issue number	2
DOIs	https://doi.org/10.1016/S0165-5728(96)00112-9
State	Published - Nov 1996

Keywords

MAC-2
Macrophage
Microglia
Myelin
Nerve regeneration
Optic nerve
Wallerian degeneration

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10.1016/S0165-5728(96)00112-9

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title = "Deficient activation of microglia during optic nerve degeneration",

abstract = "Transection of an optic nerve (ON) is follwed by slow removal of myelin. We studied microglia for the expression of molecules that characterize activated myelin phagocytosing macrophages: MAC-1, FcγII/III receptor (FcR), MAC-2, and F4/80. In-vitro, microglia expressed all molecules and phagocytosed myelin. In-vivo, intact ON displayed high levels of MAC-1, little FcR and F4/80, and no MAC-2. The expression of these molecules was upregulated differentially in in-vivo degenerating ON: MAC-1 uniformly, FcR and F4/80 variably, and MAC-2 sporadically. The distribution of MAC-2 expression correlated best with a pattern of sporadic structural degeneration. Thus in-vivo, ON injury is followed by deficient microglia activation, which we suggest contributes significantly to the slow clearance of myelin.",

keywords = "MAC-2, Macrophage, Microglia, Myelin, Nerve regeneration, Optic nerve, Wallerian degeneration",

author = "Fanny Reichert and Shlomo Rotshenker",

year = "1996",

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AU - Reichert, Fanny

AU - Rotshenker, Shlomo

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N2 - Transection of an optic nerve (ON) is follwed by slow removal of myelin. We studied microglia for the expression of molecules that characterize activated myelin phagocytosing macrophages: MAC-1, FcγII/III receptor (FcR), MAC-2, and F4/80. In-vitro, microglia expressed all molecules and phagocytosed myelin. In-vivo, intact ON displayed high levels of MAC-1, little FcR and F4/80, and no MAC-2. The expression of these molecules was upregulated differentially in in-vivo degenerating ON: MAC-1 uniformly, FcR and F4/80 variably, and MAC-2 sporadically. The distribution of MAC-2 expression correlated best with a pattern of sporadic structural degeneration. Thus in-vivo, ON injury is followed by deficient microglia activation, which we suggest contributes significantly to the slow clearance of myelin.

AB - Transection of an optic nerve (ON) is follwed by slow removal of myelin. We studied microglia for the expression of molecules that characterize activated myelin phagocytosing macrophages: MAC-1, FcγII/III receptor (FcR), MAC-2, and F4/80. In-vitro, microglia expressed all molecules and phagocytosed myelin. In-vivo, intact ON displayed high levels of MAC-1, little FcR and F4/80, and no MAC-2. The expression of these molecules was upregulated differentially in in-vivo degenerating ON: MAC-1 uniformly, FcR and F4/80 variably, and MAC-2 sporadically. The distribution of MAC-2 expression correlated best with a pattern of sporadic structural degeneration. Thus in-vivo, ON injury is followed by deficient microglia activation, which we suggest contributes significantly to the slow clearance of myelin.

KW - MAC-2

KW - Macrophage

KW - Microglia

KW - Myelin

KW - Nerve regeneration

KW - Optic nerve

KW - Wallerian degeneration

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Deficient activation of microglia during optic nerve degeneration

Abstract

Keywords

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