Literature DB >> 25468773

Microglial numbers attain adult levels after undergoing a rapid decrease in cell number in the third postnatal week.

Maria Nikodemova1, Rebecca S Kimyon1, Ishani De2, Alissa L Small1, Lara S Collier2, Jyoti J Watters3.   

Abstract

During postnatal development, microglia, CNS resident innate immune cells, are essential for synaptic pruning, neuronal apoptosis and remodeling. During this period microglia undergo morphological and phenotypic transformations; however, little is known about how microglial number and density is regulated during postnatal CNS development. We found that after an initial increase during the first 14 postnatal days, microglial numbers in mouse brain began declining in the third postnatal week and were reduced by 50% by 6weeks of age; these "adult" levels were maintained until at least 9months of age. Microglial CD11b levels increased, whereas CD45 and ER-MP58 declined between P10 and adulthood, consistent with a maturing microglial phenotype. Our data indicate that both increased microglial apoptosis and a decreased proliferative capacity contribute to the developmental reduction in microglial numbers. We found no correlation between developmental reductions in microglial numbers and brain mRNA levels of Cd200, Cx3Cl1, M-Csf or Il-34. We tested the ability of M-Csf-overexpression, a key growth factor promoting microglial proliferation and survival, to prevent microglial loss in the third postnatal week. Mice overexpressing M-Csf in astrocytes had higher numbers of microglia at all ages tested. However, the developmental decline in microglial numbers still occurred, suggesting that chronically elevated M-CSF is unable to overcome the developmental decrease in microglial numbers. Whereas the identity of the factor(s) regulating microglial number and density during development remains to be determined, it is likely that microglia respond to a "maturation" signal since the reduction in microglial numbers coincides with CNS maturation.
Copyright © 2014 Elsevier B.V. All rights reserved.

Entities:  

Keywords:  Apoptosis; Development; Flow cytometry; Gene expression; M-CSF; Proliferation

Mesh:

Substances:

Year:  2014        PMID: 25468773      PMCID: PMC4297717          DOI: 10.1016/j.jneuroim.2014.11.018

Source DB:  PubMed          Journal:  J Neuroimmunol        ISSN: 0165-5728            Impact factor:   3.478


  54 in total

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  55 in total

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2.  A Developmental Analysis of Juxtavascular Microglia Dynamics and Interactions with the Vasculature.

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Review 5.  Emerging Roles for CSF-1 Receptor and its Ligands in the Nervous System.

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7.  Similar Microglial Cell Densities across Brain Structures and Mammalian Species: Implications for Brain Tissue Function.

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Review 8.  The immune system as a novel regulator of sex differences in brain and behavioral development.

Authors:  Lars H Nelson; Kathryn M Lenz
Journal:  J Neurosci Res       Date:  2017-01-02       Impact factor: 4.164

9.  Developmental Heterogeneity of Microglia and Brain Myeloid Cells Revealed by Deep Single-Cell RNA Sequencing.

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10.  Developmental changes in microglial mobilization are independent of apoptosis in the neonatal mouse hippocampus.

Authors:  Ukpong B Eyo; Samuel A Miner; Joshua A Weiner; Michael E Dailey
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