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Astrogliogenesis in human fetal brain: complex spatiotemporal immunoreactivity patterns of GFAP , S100, AQP 4 and YKL ‐40
Author(s) -
Holst Camilla Bjørnbak,
Brøchner Christian Beltoft,
VittingSeerup Kristoffer,
Møllgård Kjeld
Publication year - 2019
Publication title -
journal of anatomy
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.932
H-Index - 118
eISSN - 1469-7580
pISSN - 0021-8782
DOI - 10.1111/joa.12948
Subject(s) - biology , astrocyte , glial fibrillary acidic protein , neuroscience , hippocampal formation , cerebral cortex , lineage markers , hippocampus , microbiology and biotechnology , progenitor cell , central nervous system , immunohistochemistry , immunology , stem cell
The astroglial lineage consists of heterogeneous cells instrumental for normal brain development, function and repair. Unfortunately, this heterogeneity complicates research in the field, which suffers from lack of truly specific and sensitive astroglial markers. Nevertheless, single astroglial markers are often used to describe astrocytes in different settings. We therefore investigated and compared spatiotemporal patterns of immunoreactivity in developing human brain from 12 to 21 weeks post conception and publicly available RNA expression data for four established and potential astroglial markers – GFAP , S100, AQP 4 and YKL ‐40. In the hippocampal region, we also screened for C3, a complement component highly expressed in A1‐reactive astrocytes. We found diverging partly overlapping patterns of the established astroglial markers GFAP , S100 and AQP 4, confirming that none of these markers can fully describe and discriminate different developmental forms and subpopulations of astrocytes in human developing brain, although AQP 4 seems to be the most sensitive and specific marker for the astroglial lineage at midgestation. AQP 4 characterizes a brain‐wide water transport system in cerebral cortex with regional differences in immunoreactivity at midgestation. AQP 4 distinguishes a vast proportion of astrocytes and subpopulations of radial glial cells destined for the astroglial lineage, including astrocytes determined for the future glia limitans and apical truncated radial glial cells in ganglionic eminences, devoid of GFAP and S100. YKL ‐40 and C3d, previously found in reactive astrocytes, stain different subpopulations of astrocytes/astroglial progenitors in developing hippocampus at midgestation and may characterize specific subpopulations of ‘developmental astrocytes’. Our results clearly reflect that lack of pan‐astrocytic markers necessitates the consideration of time, region, context and aim when choosing appropriate astroglial markers.