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Specific Human Astrocyte Subtype Revealed by Affinity Purified GFAP(+1) Antibody; Unpurified Serum Cross-Reacts with Neurofilament-L in Alzheimer

The human GFAP splice variants GFAPΔ164 and GFAPΔexon6 both result in a GFAP protein isoform with a unique out-of-frame carboxy-terminus that can be detected by the GFAP(+1) antibody. We previously reported that GFAP(+1) was expressed in astrocytes and in degenerating neurons in Alzheimer's dis...

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Autores principales: Middeldorp, Jinte, van den Berge, Simone A., Aronica, Eleonora, Speijer, Dave, Hol, Elly M.
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2009
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2766629/
https://www.ncbi.nlm.nih.gov/pubmed/19888461
http://dx.doi.org/10.1371/journal.pone.0007663
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author Middeldorp, Jinte
van den Berge, Simone A.
Aronica, Eleonora
Speijer, Dave
Hol, Elly M.
author_facet Middeldorp, Jinte
van den Berge, Simone A.
Aronica, Eleonora
Speijer, Dave
Hol, Elly M.
author_sort Middeldorp, Jinte
collection PubMed
description The human GFAP splice variants GFAPΔ164 and GFAPΔexon6 both result in a GFAP protein isoform with a unique out-of-frame carboxy-terminus that can be detected by the GFAP(+1) antibody. We previously reported that GFAP(+1) was expressed in astrocytes and in degenerating neurons in Alzheimer's disease brains. In this study we aimed at further investigating the neuronal GFAP(+1) expression and we started by affinity purifying the GFAP(+1) antibody. The purified antibody resulted in a loss of neuronal GFAP(+1) signal, although other antibodies directed against the amino- and carboxy-terminus of GFAPα still revealed GFAP-immunopositive neurons, as described before. With an in-depth analysis of a western blot, followed by mass spectrometry we discovered that the previously detected neuronal GFAP(+1) expression was due to cross-reactivity of the antibody with neurofilament-L (NF-L). This was confirmed by double-label fluorescent immunohistochemistry and western blotting with the unpurified GFAP(+1) antibody and an antibody against NF-L. Our data imply that NF-L can accumulate in some tangle-like structures in Alzheimer brains. More importantly, the purified GFAP(+1) antibody clearly revealed a specific subtype of astrocytes in the adult human brain. These large astrocytes are present throughout the brain, e.g., along the subventricular zone, in the hippocampus, in the striatum and in the spinal cord of controls, Alzheimer, and Parkinson patients. The presence of a specific GFAP-isoform suggests a specialized function of these astrocytes.
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spelling pubmed-27666292009-11-04 Specific Human Astrocyte Subtype Revealed by Affinity Purified GFAP(+1) Antibody; Unpurified Serum Cross-Reacts with Neurofilament-L in Alzheimer Middeldorp, Jinte van den Berge, Simone A. Aronica, Eleonora Speijer, Dave Hol, Elly M. PLoS One Research Article The human GFAP splice variants GFAPΔ164 and GFAPΔexon6 both result in a GFAP protein isoform with a unique out-of-frame carboxy-terminus that can be detected by the GFAP(+1) antibody. We previously reported that GFAP(+1) was expressed in astrocytes and in degenerating neurons in Alzheimer's disease brains. In this study we aimed at further investigating the neuronal GFAP(+1) expression and we started by affinity purifying the GFAP(+1) antibody. The purified antibody resulted in a loss of neuronal GFAP(+1) signal, although other antibodies directed against the amino- and carboxy-terminus of GFAPα still revealed GFAP-immunopositive neurons, as described before. With an in-depth analysis of a western blot, followed by mass spectrometry we discovered that the previously detected neuronal GFAP(+1) expression was due to cross-reactivity of the antibody with neurofilament-L (NF-L). This was confirmed by double-label fluorescent immunohistochemistry and western blotting with the unpurified GFAP(+1) antibody and an antibody against NF-L. Our data imply that NF-L can accumulate in some tangle-like structures in Alzheimer brains. More importantly, the purified GFAP(+1) antibody clearly revealed a specific subtype of astrocytes in the adult human brain. These large astrocytes are present throughout the brain, e.g., along the subventricular zone, in the hippocampus, in the striatum and in the spinal cord of controls, Alzheimer, and Parkinson patients. The presence of a specific GFAP-isoform suggests a specialized function of these astrocytes. Public Library of Science 2009-11-04 /pmc/articles/PMC2766629/ /pubmed/19888461 http://dx.doi.org/10.1371/journal.pone.0007663 Text en Middeldorp 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, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Middeldorp, Jinte
van den Berge, Simone A.
Aronica, Eleonora
Speijer, Dave
Hol, Elly M.
Specific Human Astrocyte Subtype Revealed by Affinity Purified GFAP(+1) Antibody; Unpurified Serum Cross-Reacts with Neurofilament-L in Alzheimer
title Specific Human Astrocyte Subtype Revealed by Affinity Purified GFAP(+1) Antibody; Unpurified Serum Cross-Reacts with Neurofilament-L in Alzheimer
title_full Specific Human Astrocyte Subtype Revealed by Affinity Purified GFAP(+1) Antibody; Unpurified Serum Cross-Reacts with Neurofilament-L in Alzheimer
title_fullStr Specific Human Astrocyte Subtype Revealed by Affinity Purified GFAP(+1) Antibody; Unpurified Serum Cross-Reacts with Neurofilament-L in Alzheimer
title_full_unstemmed Specific Human Astrocyte Subtype Revealed by Affinity Purified GFAP(+1) Antibody; Unpurified Serum Cross-Reacts with Neurofilament-L in Alzheimer
title_short Specific Human Astrocyte Subtype Revealed by Affinity Purified GFAP(+1) Antibody; Unpurified Serum Cross-Reacts with Neurofilament-L in Alzheimer
title_sort specific human astrocyte subtype revealed by affinity purified gfap(+1) antibody; unpurified serum cross-reacts with neurofilament-l in alzheimer
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2766629/
https://www.ncbi.nlm.nih.gov/pubmed/19888461
http://dx.doi.org/10.1371/journal.pone.0007663
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