Iba-1(-)/CD68(+) microglia are a prominent feature of age-associated deep subcortical white matter lesions

Deep subcortical lesions (DSCL) of the brain, are present in ~60% of the ageing population, and are linked to cognitive decline and depression. DSCL are associated with demyelination, blood brain barrier (BBB) dysfunction, and microgliosis. Microglia are the main immune cell of the brain. Under phys...

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Autores principales: Waller, Rachel, Baxter, Lynne, Fillingham, Daniel J., Coelho, Santiago, Pozo, Jose M., Mozumder, Meghdoot, Frangi, Alejandro F., Ince, Paul G., Simpson, Julie E., Highley, J. Robin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2019
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6347230/
https://www.ncbi.nlm.nih.gov/pubmed/30682074
http://dx.doi.org/10.1371/journal.pone.0210888
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author Waller, Rachel
Baxter, Lynne
Fillingham, Daniel J.
Coelho, Santiago
Pozo, Jose M.
Mozumder, Meghdoot
Frangi, Alejandro F.
Ince, Paul G.
Simpson, Julie E.
Highley, J. Robin
author_facet Waller, Rachel
Baxter, Lynne
Fillingham, Daniel J.
Coelho, Santiago
Pozo, Jose M.
Mozumder, Meghdoot
Frangi, Alejandro F.
Ince, Paul G.
Simpson, Julie E.
Highley, J. Robin
author_sort Waller, Rachel
collection PubMed
description Deep subcortical lesions (DSCL) of the brain, are present in ~60% of the ageing population, and are linked to cognitive decline and depression. DSCL are associated with demyelination, blood brain barrier (BBB) dysfunction, and microgliosis. Microglia are the main immune cell of the brain. Under physiological conditions microglia have a ramified morphology, and react to pathology with a change to a more rounded morphology as well as showing protein expression alterations. This study builds on previous characterisations of DSCL and radiologically ‘normal-appearing’ white matter (NAWM) by performing a detailed characterisation of a range of microglial markers in addition to markers of vascular integrity. The Cognitive Function and Ageing Study (CFAS) provided control white matter (WM), NAWM and DSCL human post mortem tissue for immunohistochemistry using microglial markers (Iba-1, CD68 and MHCII), a vascular basement membrane marker (collagen IV) and markers of BBB integrity (fibrinogen and aquaporin 4). The immunoreactive profile of CD68 increased in a stepwise manner from control WM to NAWM to DSCL. This correlated with a shift from small, ramified cells, to larger, more rounded microglia. While there was greater Iba-1 immunoreactivity in NAWM compared to controls, in DSCL, Iba-1 levels were reduced to control levels. A prominent feature of these DSCL was a population of Iba-1(-)/CD68(+) microglia. There were increases in collagen IV, but no change in BBB integrity. Overall the study shows significant differences in the immunoreactive profile of microglial markers. Whether this is a cause or effect of lesion development remains to be elucidated. Identifying microglia subpopulations based on their morphology and molecular markers may ultimately help decipher their function and role in neurodegeneration. Furthermore, this study demonstrates that Iba-1 is not a pan-microglial marker, and that a combination of several microglial markers is required to fully characterise the microglial phenotype.
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spelling pubmed-63472302019-02-02 Iba-1(-)/CD68(+) microglia are a prominent feature of age-associated deep subcortical white matter lesions Waller, Rachel Baxter, Lynne Fillingham, Daniel J. Coelho, Santiago Pozo, Jose M. Mozumder, Meghdoot Frangi, Alejandro F. Ince, Paul G. Simpson, Julie E. Highley, J. Robin PLoS One Research Article Deep subcortical lesions (DSCL) of the brain, are present in ~60% of the ageing population, and are linked to cognitive decline and depression. DSCL are associated with demyelination, blood brain barrier (BBB) dysfunction, and microgliosis. Microglia are the main immune cell of the brain. Under physiological conditions microglia have a ramified morphology, and react to pathology with a change to a more rounded morphology as well as showing protein expression alterations. This study builds on previous characterisations of DSCL and radiologically ‘normal-appearing’ white matter (NAWM) by performing a detailed characterisation of a range of microglial markers in addition to markers of vascular integrity. The Cognitive Function and Ageing Study (CFAS) provided control white matter (WM), NAWM and DSCL human post mortem tissue for immunohistochemistry using microglial markers (Iba-1, CD68 and MHCII), a vascular basement membrane marker (collagen IV) and markers of BBB integrity (fibrinogen and aquaporin 4). The immunoreactive profile of CD68 increased in a stepwise manner from control WM to NAWM to DSCL. This correlated with a shift from small, ramified cells, to larger, more rounded microglia. While there was greater Iba-1 immunoreactivity in NAWM compared to controls, in DSCL, Iba-1 levels were reduced to control levels. A prominent feature of these DSCL was a population of Iba-1(-)/CD68(+) microglia. There were increases in collagen IV, but no change in BBB integrity. Overall the study shows significant differences in the immunoreactive profile of microglial markers. Whether this is a cause or effect of lesion development remains to be elucidated. Identifying microglia subpopulations based on their morphology and molecular markers may ultimately help decipher their function and role in neurodegeneration. Furthermore, this study demonstrates that Iba-1 is not a pan-microglial marker, and that a combination of several microglial markers is required to fully characterise the microglial phenotype. Public Library of Science 2019-01-25 /pmc/articles/PMC6347230/ /pubmed/30682074 http://dx.doi.org/10.1371/journal.pone.0210888 Text en © 2019 Waller et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Waller, Rachel
Baxter, Lynne
Fillingham, Daniel J.
Coelho, Santiago
Pozo, Jose M.
Mozumder, Meghdoot
Frangi, Alejandro F.
Ince, Paul G.
Simpson, Julie E.
Highley, J. Robin
Iba-1(-)/CD68(+) microglia are a prominent feature of age-associated deep subcortical white matter lesions
title Iba-1(-)/CD68(+) microglia are a prominent feature of age-associated deep subcortical white matter lesions
title_full Iba-1(-)/CD68(+) microglia are a prominent feature of age-associated deep subcortical white matter lesions
title_fullStr Iba-1(-)/CD68(+) microglia are a prominent feature of age-associated deep subcortical white matter lesions
title_full_unstemmed Iba-1(-)/CD68(+) microglia are a prominent feature of age-associated deep subcortical white matter lesions
title_short Iba-1(-)/CD68(+) microglia are a prominent feature of age-associated deep subcortical white matter lesions
title_sort iba-1(-)/cd68(+) microglia are a prominent feature of age-associated deep subcortical white matter lesions
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6347230/
https://www.ncbi.nlm.nih.gov/pubmed/30682074
http://dx.doi.org/10.1371/journal.pone.0210888
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