Siglec-H is a microglia-specific marker that discriminates microglia from CNS-associated macrophages and CNS-infiltrating monocytes

Konishi, Hiroyuki; Kobayashi, Masaaki; Kunisawa, Taikan; Imai, Kenta; Sayo, Akira; Malissen, Bernard; Crocker, Paul R.; Sato, Katsuaki; Kiyama, Hiroshi

doi:https://doi.org/10.1002/glia.23204

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Siglec-H is a microglia-specific marker that discriminates microglia from CNS-associated macrophages and CNS-infiltrating monocytes

http://hdl.handle.net/2237/27242

名前 / ファイル	ライセンス	アクション
Konishi_Glia_2017.pdf ファイル公開日:2018/12/01 (2.4 MB)

Item type

学術雑誌論文 / Journal Article(1)

公開日

2018-01-09

タイトル

Siglec-H is a microglia-specific marker that discriminates microglia from CNS-associated macrophages and CNS-infiltrating monocytes

言語

著者

Konishi, Hiroyuki
Kobayashi, Masaaki
Kunisawa, Taikan
Imai, Kenta
Sayo, Akira
Malissen, Bernard
Crocker, Paul R.
Sato, Katsuaki
Kiyama, Hiroshi

アクセス権

open access

アクセス権URI

http://purl.org/coar/access_right/c_abf2

権利

言語

権利情報

This is the peer reviewed version of the following article: [Konishi, H; Kobayashi, M; Kunisawa, T; Imai, K; Sayo, A; Malissen, B; Crocker, PR; Sato, K; Kiyama, H. (2017),Siglec-H is a microglia-specific marker that discriminates microglia from CNS-associated macrophages and CNS-infiltrating monocytes. GLIA, 65, 12: 1927-1943. doi:10.1111/jdv.13290], which has been published in final form at [http://doi.org/10.1002/glia.23204]. This article may be used for non-commercial purposes in accordance with Wiley Terms and Conditions for Self-Archiving.

キーワード

主題Scheme

Other

主題

perivascular spaces

キーワード

主題Scheme

Other

主題

allodynia

キーワード

主題Scheme

Other

主題

choroid plexus

キーワード

主題Scheme

Other

主題

inflammation

キーワード

主題Scheme

Other

主題

meninges

キーワード

主題Scheme

Other

主題

myeloid cells

キーワード

主題Scheme

Other

主題

pain

抄録

内容記述

Several types of myeloid cell are resident in the CNS. In the steady state, microglia are present in the CNS parenchyma, whereas macrophages reside in boundary regions of the CNS, such as perivascular spaces, the meninges and choroid plexus. In addition, monocytes infiltrate into the CNS parenchyma from circulation upon blood–brain barrier breakdown after CNS injury and inflammation. Although several markers, such as CD11b and ionized calcium-binding adapter molecule 1 (Iba1), are frequently used as microglial markers, they are also expressed by other types of myeloid cell and microglia-specific markers were not defined until recently. Previous transcriptome analyses of isolated microglia identified a transmembrane lectin, sialic acid-binding immunoglobulin-like lectin H (Siglec-H), as a molecular signature for microglia; however, this was not confirmed by histological studies in the nervous system and the reliability of Siglec-H as a microglial marker remained unclear. Here, we demonstrate that Siglec-H is an authentic marker for microglia in mice by immunohistochemistry using a Siglec-H-specific antibody. Siglec-H was expressed by parenchymal microglia from developmental stages to adulthood, and the expression was maintained in activated microglia under injury or inflammatory condition. However, Siglec-H expression was absent from CNS-associated macrophages and CNS-infiltrating monocytes, except for a minor subset of cells. We also show that the Siglech gene locus is a feasible site for specific targeting of microglia in the nervous system. In conclusion, Siglec-H is a reliable marker for microglia that will allow histological identification of microglia and microglia-specific gene manipulation in the nervous system.

言語

内容記述タイプ

Abstract

出版者

言語

出版者

Wiley

言語

eng

資源タイプ

資源タイプresource

http://purl.org/coar/resource_type/c_6501

タイプ

journal article

出版タイプ

出版タイプResource

http://purl.org/coar/version/c_ab4af688f83e57aa

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2021-03-01 13:47:53.388664

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Siglec-H is a microglia-specific marker that discriminates microglia from CNS-associated macrophages and CNS-infiltrating monocytes

× Konishi, Hiroyuki

× Kobayashi, Masaaki

× Kunisawa, Taikan

× Imai, Kenta

× Sayo, Akira

× Malissen, Bernard

× Crocker, Paul R.

× Sato, Katsuaki

× Kiyama, Hiroshi

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