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SSEA‐4 and YKL‐40 positive progenitor subtypes in the subventricular zone of developing human neocortex

The glycosphingolipid SSEA‐4 and the glycoprotein YKL‐40 have both been associated with human embryonic and neural stem cell differentiation. We investigated the distribution of SSEA‐4 and YKL‐40 positive cells in proliferative zones of human fetal forebrain using immunohistochemistry and double‐lab...

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Autores principales: Brøchner, Christian B., Møllgård, Kjeld
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5049638/
https://www.ncbi.nlm.nih.gov/pubmed/26295543
http://dx.doi.org/10.1002/glia.22905
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author Brøchner, Christian B.
Møllgård, Kjeld
author_facet Brøchner, Christian B.
Møllgård, Kjeld
author_sort Brøchner, Christian B.
collection PubMed
description The glycosphingolipid SSEA‐4 and the glycoprotein YKL‐40 have both been associated with human embryonic and neural stem cell differentiation. We investigated the distribution of SSEA‐4 and YKL‐40 positive cells in proliferative zones of human fetal forebrain using immunohistochemistry and double‐labeling immunofluorescence. A few small rounded SSEA‐4 and YKL‐40 labeled cells were present in the radial glial BLBP positive proliferative zones adjacent to the lateral ganglionic eminence from 12th week post conception. With increasing age, a similarly stained cell population appeared more widespread in the subventricular zone. At midgestation, the entire subventricular zone showed patches of SSEA‐4, YKL‐40, and BLBP positive cells. Co‐labeling with markers for radial glial cells (RGCs) and neuronal, glial, and microglial markers tested the lineage identity of this subpopulation of radial glial descendants. Adjacent to the ventricular zone, a minor fraction showed overlap with GFAP but not with nestin, Olig2, NG2, or S100. No co‐localization was found with neuronal markers NeuN, calbindin, DCX or with markers for microglial cells (Iba‐1, CD68). Moreover, the SSEA‐4 and YKL‐40 positive cell population in subventricular zone was largely devoid of Tbr2, a marker for intermediate neuronal progenitor cells descending from RGCs. YKL‐40 has recently been found in astrocytes in the neuron‐free fimbria, and both SSEA‐4 and YKL‐40 are present in malignant astroglial brain tumors. We suggest that the population of cells characterized by immunohistochemical combination of antibodies against SSEA‐4 and YKL‐40 and devoid of neuronal and microglial markers represent a yet unexplored astrogenic lineage illustrating the complexity of astroglial development. GLIA 2016;64:90–104
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spelling pubmed-50496382016-10-06 SSEA‐4 and YKL‐40 positive progenitor subtypes in the subventricular zone of developing human neocortex Brøchner, Christian B. Møllgård, Kjeld Glia Research Articles The glycosphingolipid SSEA‐4 and the glycoprotein YKL‐40 have both been associated with human embryonic and neural stem cell differentiation. We investigated the distribution of SSEA‐4 and YKL‐40 positive cells in proliferative zones of human fetal forebrain using immunohistochemistry and double‐labeling immunofluorescence. A few small rounded SSEA‐4 and YKL‐40 labeled cells were present in the radial glial BLBP positive proliferative zones adjacent to the lateral ganglionic eminence from 12th week post conception. With increasing age, a similarly stained cell population appeared more widespread in the subventricular zone. At midgestation, the entire subventricular zone showed patches of SSEA‐4, YKL‐40, and BLBP positive cells. Co‐labeling with markers for radial glial cells (RGCs) and neuronal, glial, and microglial markers tested the lineage identity of this subpopulation of radial glial descendants. Adjacent to the ventricular zone, a minor fraction showed overlap with GFAP but not with nestin, Olig2, NG2, or S100. No co‐localization was found with neuronal markers NeuN, calbindin, DCX or with markers for microglial cells (Iba‐1, CD68). Moreover, the SSEA‐4 and YKL‐40 positive cell population in subventricular zone was largely devoid of Tbr2, a marker for intermediate neuronal progenitor cells descending from RGCs. YKL‐40 has recently been found in astrocytes in the neuron‐free fimbria, and both SSEA‐4 and YKL‐40 are present in malignant astroglial brain tumors. We suggest that the population of cells characterized by immunohistochemical combination of antibodies against SSEA‐4 and YKL‐40 and devoid of neuronal and microglial markers represent a yet unexplored astrogenic lineage illustrating the complexity of astroglial development. GLIA 2016;64:90–104 John Wiley and Sons Inc. 2015-08-21 2016-01 /pmc/articles/PMC5049638/ /pubmed/26295543 http://dx.doi.org/10.1002/glia.22905 Text en © 2015 The Authors. Glia Published by Wiley Periodicals, Inc. This is an open access article under the terms of the Creative Commons Attribution‐NonCommercial‐NoDerivs (http://creativecommons.org/licenses/by-nc-nd/4.0/) License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non‐commercial and no modifications or adaptations are made.
spellingShingle Research Articles
Brøchner, Christian B.
Møllgård, Kjeld
SSEA‐4 and YKL‐40 positive progenitor subtypes in the subventricular zone of developing human neocortex
title SSEA‐4 and YKL‐40 positive progenitor subtypes in the subventricular zone of developing human neocortex
title_full SSEA‐4 and YKL‐40 positive progenitor subtypes in the subventricular zone of developing human neocortex
title_fullStr SSEA‐4 and YKL‐40 positive progenitor subtypes in the subventricular zone of developing human neocortex
title_full_unstemmed SSEA‐4 and YKL‐40 positive progenitor subtypes in the subventricular zone of developing human neocortex
title_short SSEA‐4 and YKL‐40 positive progenitor subtypes in the subventricular zone of developing human neocortex
title_sort ssea‐4 and ykl‐40 positive progenitor subtypes in the subventricular zone of developing human neocortex
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5049638/
https://www.ncbi.nlm.nih.gov/pubmed/26295543
http://dx.doi.org/10.1002/glia.22905
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