Fetuin-A protein distribution in mature inflamed and ischemic brain tissue

BACKGROUND: The liver-derived plasma protein fetuin-A is strongly expressed during fetal life, hence its name. Fetuin-A protein is normally present in most fetal organs and tissues, including brain tissue. Fetuin-A was neuroprotective in animal models of cerebral ischemia and lethal chronic inflamma...

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Autores principales: Heinen, Miriam Christina, Babler, Anne, Weis, Joachim, Elsas, Johannes, Nolte, Kay, Kipp, Markus, Jahnen-Dechent, Willi, Häusler, Martin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2018
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6226147/
https://www.ncbi.nlm.nih.gov/pubmed/30412582
http://dx.doi.org/10.1371/journal.pone.0206597
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author Heinen, Miriam Christina
Babler, Anne
Weis, Joachim
Elsas, Johannes
Nolte, Kay
Kipp, Markus
Jahnen-Dechent, Willi
Häusler, Martin
author_facet Heinen, Miriam Christina
Babler, Anne
Weis, Joachim
Elsas, Johannes
Nolte, Kay
Kipp, Markus
Jahnen-Dechent, Willi
Häusler, Martin
author_sort Heinen, Miriam Christina
collection PubMed
description BACKGROUND: The liver-derived plasma protein fetuin-A is strongly expressed during fetal life, hence its name. Fetuin-A protein is normally present in most fetal organs and tissues, including brain tissue. Fetuin-A was neuroprotective in animal models of cerebral ischemia and lethal chronic inflammation, suggesting a role beyond the neonatal period. Little is known, however, on the presence of fetuin-A in mature human brain tissue under different physiological and pathological conditions. METHODS: We studied by immunohistochemistry (IHC) the distribution of fetuin-A protein in mature human brain autopsy tissues from patients without neurological disease, patients with inflammatory brain disorders, and patients with ischemic brain lesions. To identify fetuin-A-positive cells in these tissues we co-localized fetuin-A with GFAP (astrocytes) and CD68 (macrophages, activated microglia). RESULTS AND DISCUSSION: Unlike previous reports, we detected fetuin-A protein also in mature human brain as would be expected from an abundant plasma protein also present in cerebrospinal fluid. Fetuin-A immunoreactivity was increased in ischemic white matter and decreased in inflamed cerebellar tissue. Fetuin-A immunostaining was predominantly associated with neurons and astrocytes. Unlike the developing brain, the adult brain lacked fetuin-A immunostaining in CD68-positive microglia. Our findings suggest a role for fetuin-A in tissue remodeling of neonatal brain, which becomes obsolete in the adult brain, but is re-activated in damaged brain tissue. To further assess the role of fetuin-A in the mature brain, animal models involving ischemia and inflammation need to be studied.
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spelling pubmed-62261472018-11-19 Fetuin-A protein distribution in mature inflamed and ischemic brain tissue Heinen, Miriam Christina Babler, Anne Weis, Joachim Elsas, Johannes Nolte, Kay Kipp, Markus Jahnen-Dechent, Willi Häusler, Martin PLoS One Research Article BACKGROUND: The liver-derived plasma protein fetuin-A is strongly expressed during fetal life, hence its name. Fetuin-A protein is normally present in most fetal organs and tissues, including brain tissue. Fetuin-A was neuroprotective in animal models of cerebral ischemia and lethal chronic inflammation, suggesting a role beyond the neonatal period. Little is known, however, on the presence of fetuin-A in mature human brain tissue under different physiological and pathological conditions. METHODS: We studied by immunohistochemistry (IHC) the distribution of fetuin-A protein in mature human brain autopsy tissues from patients without neurological disease, patients with inflammatory brain disorders, and patients with ischemic brain lesions. To identify fetuin-A-positive cells in these tissues we co-localized fetuin-A with GFAP (astrocytes) and CD68 (macrophages, activated microglia). RESULTS AND DISCUSSION: Unlike previous reports, we detected fetuin-A protein also in mature human brain as would be expected from an abundant plasma protein also present in cerebrospinal fluid. Fetuin-A immunoreactivity was increased in ischemic white matter and decreased in inflamed cerebellar tissue. Fetuin-A immunostaining was predominantly associated with neurons and astrocytes. Unlike the developing brain, the adult brain lacked fetuin-A immunostaining in CD68-positive microglia. Our findings suggest a role for fetuin-A in tissue remodeling of neonatal brain, which becomes obsolete in the adult brain, but is re-activated in damaged brain tissue. To further assess the role of fetuin-A in the mature brain, animal models involving ischemia and inflammation need to be studied. Public Library of Science 2018-11-09 /pmc/articles/PMC6226147/ /pubmed/30412582 http://dx.doi.org/10.1371/journal.pone.0206597 Text en © 2018 Heinen 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
Heinen, Miriam Christina
Babler, Anne
Weis, Joachim
Elsas, Johannes
Nolte, Kay
Kipp, Markus
Jahnen-Dechent, Willi
Häusler, Martin
Fetuin-A protein distribution in mature inflamed and ischemic brain tissue
title Fetuin-A protein distribution in mature inflamed and ischemic brain tissue
title_full Fetuin-A protein distribution in mature inflamed and ischemic brain tissue
title_fullStr Fetuin-A protein distribution in mature inflamed and ischemic brain tissue
title_full_unstemmed Fetuin-A protein distribution in mature inflamed and ischemic brain tissue
title_short Fetuin-A protein distribution in mature inflamed and ischemic brain tissue
title_sort fetuin-a protein distribution in mature inflamed and ischemic brain tissue
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6226147/
https://www.ncbi.nlm.nih.gov/pubmed/30412582
http://dx.doi.org/10.1371/journal.pone.0206597
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