Morphological impairments in microglia precede age-related neuronal degeneration in senescence-accelerated mice

The ageing brain is characterized by degenerative changes in both neurons and glia. Although neurons are known to lose dendritic complexity with ageing, age‐related changes in the morphology of microglia have not been well documented. We investigated potential age‐related changes in microglial morph...

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Veröffentlicht in:	Neuropathology 2011-02, Vol.31 (1), p.20-28
Hauptverfasser:	Hasegawa-Ishii, Sanae, Takei, Shiro, Chiba, Yoichi, Furukawa, Ayako, Umegaki, Hiroyuki, Iguchi, Akihisa, Kawamura, Noriko, Yoshikawa, Keisuke, Hosokawa, Masanori, Shimada, Atsuyoshi
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Schlagworte:	Age ageing Aging Aging - pathology animal model Animal models Animals Antibodies Brain Cameras Cell body Hippocampus Hippocampus - pathology Image Processing, Computer-Assisted Immunohistochemistry Mice Mice, Mutant Strains Microglia Microglia - pathology Nerve Degeneration - pathology Neurodegeneration Neurons Neurons - pathology
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creator	Hasegawa-Ishii, Sanae Takei, Shiro Chiba, Yoichi Furukawa, Ayako Umegaki, Hiroyuki Iguchi, Akihisa Kawamura, Noriko Yoshikawa, Keisuke Hosokawa, Masanori Shimada, Atsuyoshi
description	The ageing brain is characterized by degenerative changes in both neurons and glia. Although neurons are known to lose dendritic complexity with ageing, age‐related changes in the morphology of microglia have not been well documented. We investigated potential age‐related changes in microglial morphology using mouse models. Senescence‐accelerated mouse prone 10 (SAMP10) in which neuronal degeneration begins to appear around 8 months of age and becomes progressively remarkable with advancing age was used as a model of brain ageing. Senescence‐accelerated mouse resistant 1 (SAMR1) in which age‐related neuronal changes are inconspicuous was used as usual‐ageing controls. Hippocampal sections prepared from 3‐, 8‐ and 14‐month‐old SAMP10 and 3‐, 8‐, 14‐ and 24‐month‐old SAMR1 mice were stained immunohistochemically with anti‐Iba‐1 antibody to highlight microglia. Stick figures of individual microglia reflecting the length and complexity of cytoplasmic processes were made by camera lucida drawing. Parameters representing morphological features of microglia were quantified using an image analyzer: area of convex closure, cell body area, number of primary processes, maximal branch order, combined projection length, number of segments and number of tips. Pathological changes of processes such as beading and clusters of fragmented twigs were counted. In microglia of 3‐ and 8‐month‐old SAMP10 mice, combined projection length was shorter and numbers of segments and tips were smaller than those in age‐matched SAMR1 mice. Similar changes were detected in SAMR1 mice at age 14 months and older. Microglia of SAMP10 mice at all ages were characterized by having frequent pathological changes in processes, which were not remarkable in SAMR1 mice at any age. These morphological abnormalities in microglia of SAMP10 mice preceded the onset of neuronal degeneration and may lead to making brain tissue less protective to neurons. We propose that preceding abnormalities in microglia may contribute to the vulnerability to age‐related neuronal degeneration in SAMP10 mice.
doi_str_mv	10.1111/j.1440-1789.2010.01126.x
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Although neurons are known to lose dendritic complexity with ageing, age‐related changes in the morphology of microglia have not been well documented. We investigated potential age‐related changes in microglial morphology using mouse models. Senescence‐accelerated mouse prone 10 (SAMP10) in which neuronal degeneration begins to appear around 8 months of age and becomes progressively remarkable with advancing age was used as a model of brain ageing. Senescence‐accelerated mouse resistant 1 (SAMR1) in which age‐related neuronal changes are inconspicuous was used as usual‐ageing controls. Hippocampal sections prepared from 3‐, 8‐ and 14‐month‐old SAMP10 and 3‐, 8‐, 14‐ and 24‐month‐old SAMR1 mice were stained immunohistochemically with anti‐Iba‐1 antibody to highlight microglia. Stick figures of individual microglia reflecting the length and complexity of cytoplasmic processes were made by camera lucida drawing. Parameters representing morphological features of microglia were quantified using an image analyzer: area of convex closure, cell body area, number of primary processes, maximal branch order, combined projection length, number of segments and number of tips. Pathological changes of processes such as beading and clusters of fragmented twigs were counted. In microglia of 3‐ and 8‐month‐old SAMP10 mice, combined projection length was shorter and numbers of segments and tips were smaller than those in age‐matched SAMR1 mice. Similar changes were detected in SAMR1 mice at age 14 months and older. Microglia of SAMP10 mice at all ages were characterized by having frequent pathological changes in processes, which were not remarkable in SAMR1 mice at any age. These morphological abnormalities in microglia of SAMP10 mice preceded the onset of neuronal degeneration and may lead to making brain tissue less protective to neurons. 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Although neurons are known to lose dendritic complexity with ageing, age‐related changes in the morphology of microglia have not been well documented. We investigated potential age‐related changes in microglial morphology using mouse models. Senescence‐accelerated mouse prone 10 (SAMP10) in which neuronal degeneration begins to appear around 8 months of age and becomes progressively remarkable with advancing age was used as a model of brain ageing. Senescence‐accelerated mouse resistant 1 (SAMR1) in which age‐related neuronal changes are inconspicuous was used as usual‐ageing controls. Hippocampal sections prepared from 3‐, 8‐ and 14‐month‐old SAMP10 and 3‐, 8‐, 14‐ and 24‐month‐old SAMR1 mice were stained immunohistochemically with anti‐Iba‐1 antibody to highlight microglia. Stick figures of individual microglia reflecting the length and complexity of cytoplasmic processes were made by camera lucida drawing. Parameters representing morphological features of microglia were quantified using an image analyzer: area of convex closure, cell body area, number of primary processes, maximal branch order, combined projection length, number of segments and number of tips. Pathological changes of processes such as beading and clusters of fragmented twigs were counted. In microglia of 3‐ and 8‐month‐old SAMP10 mice, combined projection length was shorter and numbers of segments and tips were smaller than those in age‐matched SAMR1 mice. Similar changes were detected in SAMR1 mice at age 14 months and older. Microglia of SAMP10 mice at all ages were characterized by having frequent pathological changes in processes, which were not remarkable in SAMR1 mice at any age. These morphological abnormalities in microglia of SAMP10 mice preceded the onset of neuronal degeneration and may lead to making brain tissue less protective to neurons. We propose that preceding abnormalities in microglia may contribute to the vulnerability to age‐related neuronal degeneration in SAMP10 mice.</description><subject>Age</subject><subject>ageing</subject><subject>Aging</subject><subject>Aging - pathology</subject><subject>animal model</subject><subject>Animal models</subject><subject>Animals</subject><subject>Antibodies</subject><subject>Brain</subject><subject>Cameras</subject><subject>Cell body</subject><subject>Hippocampus</subject><subject>Hippocampus - pathology</subject><subject>Image Processing, Computer-Assisted</subject><subject>Immunohistochemistry</subject><subject>Mice</subject><subject>Mice, Mutant Strains</subject><subject>Microglia</subject><subject>Microglia - pathology</subject><subject>Nerve Degeneration - pathology</subject><subject>Neurodegeneration</subject><subject>Neurons</subject><subject>Neurons - pathology</subject><issn>0919-6544</issn><issn>1440-1789</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2011</creationdate><recordtype>article</recordtype><sourceid>EIF</sourceid><recordid>eNqFkctuFDEQRS1ERCaBX0C9Y9UT2-1H9wYJopBESsJDBCQ2Vo1dPXhwP7B7lMnf42bCbKmNq3xPXVm-hBSMLlmus82SCUFLputmyWm-pYxxtdw9I4uD8JwsaMOaUkkhjslJShtKmW54_YIccyoaXQm2IMPtEMefQxjW3kIofDeCjx32Uyp8X3TexmEdPBRjRIsOC1hjGTHAhK7ocRuHPm85XGOPESY_9PNaylOy2FsswVoMs5T57IYvyVELIeGrp_OU3H-4-Hp-Vd58vLw-f3dTWlFTVTJoqeNQWeaoBaxAiaYSkkOLVNJWCocr4WjrEKyWNdcrsEqtGCqoapRNdUre7H3HOPzeYppM5_OTQoAeh20ytW6E5lLV_yeF1EpyLjP5-oncrjp0Zoy-g_ho_v1mBt7ugQcf8PGgM2rm1MzGzOGYORwzp2b-pmZ25u7i_tPcZoNyb-DThLuDAcRfRulKS_P97tL8-PJe8-r2s_lW_QGtmZzA</recordid><startdate>201102</startdate><enddate>201102</enddate><creator>Hasegawa-Ishii, Sanae</creator><creator>Takei, Shiro</creator><creator>Chiba, Yoichi</creator><creator>Furukawa, Ayako</creator><creator>Umegaki, Hiroyuki</creator><creator>Iguchi, Akihisa</creator><creator>Kawamura, Noriko</creator><creator>Yoshikawa, Keisuke</creator><creator>Hosokawa, Masanori</creator><creator>Shimada, Atsuyoshi</creator><general>Blackwell Publishing Asia</general><scope>BSCLL</scope><scope>CGR</scope><scope>CUY</scope><scope>CVF</scope><scope>ECM</scope><scope>EIF</scope><scope>NPM</scope><scope>7X8</scope><scope>7TK</scope></search><sort><creationdate>201102</creationdate><title>Morphological impairments in microglia precede age-related neuronal degeneration in senescence-accelerated mice</title><author>Hasegawa-Ishii, Sanae ; Takei, Shiro ; Chiba, Yoichi ; Furukawa, Ayako ; Umegaki, Hiroyuki ; Iguchi, Akihisa ; Kawamura, Noriko ; Yoshikawa, Keisuke ; Hosokawa, Masanori ; Shimada, Atsuyoshi</author></sort><facets><frbrtype>5</frbrtype><frbrgroupid>cdi_FETCH-LOGICAL-c4806-1af0d2a3c1d0cae3a6493452afe050f54deb4d0fdeac75827bac66b1e6a38e593</frbrgroupid><rsrctype>articles</rsrctype><prefilter>articles</prefilter><language>eng</language><creationdate>2011</creationdate><topic>Age</topic><topic>ageing</topic><topic>Aging</topic><topic>Aging - pathology</topic><topic>animal model</topic><topic>Animal models</topic><topic>Animals</topic><topic>Antibodies</topic><topic>Brain</topic><topic>Cameras</topic><topic>Cell body</topic><topic>Hippocampus</topic><topic>Hippocampus - pathology</topic><topic>Image Processing, Computer-Assisted</topic><topic>Immunohistochemistry</topic><topic>Mice</topic><topic>Mice, Mutant Strains</topic><topic>Microglia</topic><topic>Microglia - pathology</topic><topic>Nerve Degeneration - pathology</topic><topic>Neurodegeneration</topic><topic>Neurons</topic><topic>Neurons - pathology</topic><toplevel>peer_reviewed</toplevel><toplevel>online_resources</toplevel><creatorcontrib>Hasegawa-Ishii, Sanae</creatorcontrib><creatorcontrib>Takei, Shiro</creatorcontrib><creatorcontrib>Chiba, Yoichi</creatorcontrib><creatorcontrib>Furukawa, Ayako</creatorcontrib><creatorcontrib>Umegaki, Hiroyuki</creatorcontrib><creatorcontrib>Iguchi, Akihisa</creatorcontrib><creatorcontrib>Kawamura, Noriko</creatorcontrib><creatorcontrib>Yoshikawa, Keisuke</creatorcontrib><creatorcontrib>Hosokawa, Masanori</creatorcontrib><creatorcontrib>Shimada, Atsuyoshi</creatorcontrib><collection>Istex</collection><collection>Medline</collection><collection>MEDLINE</collection><collection>MEDLINE (Ovid)</collection><collection>MEDLINE</collection><collection>MEDLINE</collection><collection>PubMed</collection><collection>MEDLINE - Academic</collection><collection>Neurosciences Abstracts</collection><jtitle>Neuropathology</jtitle></facets><delivery><delcategory>Remote Search Resource</delcategory><fulltext>fulltext</fulltext></delivery><addata><au>Hasegawa-Ishii, Sanae</au><au>Takei, Shiro</au><au>Chiba, Yoichi</au><au>Furukawa, Ayako</au><au>Umegaki, Hiroyuki</au><au>Iguchi, Akihisa</au><au>Kawamura, Noriko</au><au>Yoshikawa, Keisuke</au><au>Hosokawa, Masanori</au><au>Shimada, Atsuyoshi</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>Morphological impairments in microglia precede age-related neuronal degeneration in senescence-accelerated mice</atitle><jtitle>Neuropathology</jtitle><addtitle>Neuropathology</addtitle><date>2011-02</date><risdate>2011</risdate><volume>31</volume><issue>1</issue><spage>20</spage><epage>28</epage><pages>20-28</pages><issn>0919-6544</issn><eissn>1440-1789</eissn><abstract>The ageing brain is characterized by degenerative changes in both neurons and glia. Although neurons are known to lose dendritic complexity with ageing, age‐related changes in the morphology of microglia have not been well documented. We investigated potential age‐related changes in microglial morphology using mouse models. Senescence‐accelerated mouse prone 10 (SAMP10) in which neuronal degeneration begins to appear around 8 months of age and becomes progressively remarkable with advancing age was used as a model of brain ageing. Senescence‐accelerated mouse resistant 1 (SAMR1) in which age‐related neuronal changes are inconspicuous was used as usual‐ageing controls. Hippocampal sections prepared from 3‐, 8‐ and 14‐month‐old SAMP10 and 3‐, 8‐, 14‐ and 24‐month‐old SAMR1 mice were stained immunohistochemically with anti‐Iba‐1 antibody to highlight microglia. Stick figures of individual microglia reflecting the length and complexity of cytoplasmic processes were made by camera lucida drawing. Parameters representing morphological features of microglia were quantified using an image analyzer: area of convex closure, cell body area, number of primary processes, maximal branch order, combined projection length, number of segments and number of tips. Pathological changes of processes such as beading and clusters of fragmented twigs were counted. In microglia of 3‐ and 8‐month‐old SAMP10 mice, combined projection length was shorter and numbers of segments and tips were smaller than those in age‐matched SAMR1 mice. Similar changes were detected in SAMR1 mice at age 14 months and older. Microglia of SAMP10 mice at all ages were characterized by having frequent pathological changes in processes, which were not remarkable in SAMR1 mice at any age. These morphological abnormalities in microglia of SAMP10 mice preceded the onset of neuronal degeneration and may lead to making brain tissue less protective to neurons. We propose that preceding abnormalities in microglia may contribute to the vulnerability to age‐related neuronal degeneration in SAMP10 mice.</abstract><cop>Melbourne, Australia</cop><pub>Blackwell Publishing Asia</pub><pmid>20497341</pmid><doi>10.1111/j.1440-1789.2010.01126.x</doi><tpages>9</tpages></addata></record>
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subjects	Age ageing Aging Aging - pathology animal model Animal models Animals Antibodies Brain Cameras Cell body Hippocampus Hippocampus - pathology Image Processing, Computer-Assisted Immunohistochemistry Mice Mice, Mutant Strains Microglia Microglia - pathology Nerve Degeneration - pathology Neurodegeneration Neurons Neurons - pathology
title	Morphological impairments in microglia precede age-related neuronal degeneration in senescence-accelerated mice
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