Neurogenesis and neuronal differentiation in the postnatal frontal cortex in Down syndrome

Emma C. Utagawa; David G. Moreno; Kristian T. Schafernak; Nicoleta C. Arva; Michael H. Malek-Ahmadi; Elliott J. Mufson; Sylvia E. Perez

doi:10.1186/s40478-022-01385-w

Acta Neuropathologica Communications (Jun 2022)

Neurogenesis and neuronal differentiation in the postnatal frontal cortex in Down syndrome

Emma C. Utagawa,
David G. Moreno,
Kristian T. Schafernak,
Nicoleta C. Arva,
Michael H. Malek-Ahmadi,
Elliott J. Mufson,
Sylvia E. Perez

Affiliations

Emma C. Utagawa: Department of Translational Neuroscience, Barrow Neurological Institute
David G. Moreno: Department of Translational Neuroscience, Barrow Neurological Institute
Kristian T. Schafernak: Department of Pathology and Laboratory Medicine, Phoenix Children’s Hospital
Nicoleta C. Arva: Department of Pathology and Laboratory Medicine, Ann and Robert H. Lurie Children’s Hospital of Chicago
Michael H. Malek-Ahmadi: Banner Alzheimer’s Institute
Elliott J. Mufson: Department of Translational Neuroscience, Barrow Neurological Institute
Sylvia E. Perez: Department of Translational Neuroscience, Barrow Neurological Institute

DOI: https://doi.org/10.1186/s40478-022-01385-w
Journal volume & issue: Vol. 10, no. 1
pp. 1 – 27

Abstract

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Abstract Although Down syndrome (DS), the most common developmental genetic cause of intellectual disability, displays proliferation and migration deficits in the prenatal frontal cortex (FC), a knowledge gap exists on the effects of trisomy 21 upon postnatal cortical development. Here, we examined cortical neurogenesis and differentiation in the FC supragranular (SG, II/III) and infragranular (IG, V/VI) layers applying antibodies to doublecortin (DCX), non-phosphorylated heavy-molecular neurofilament protein (NHF, SMI-32), calbindin D-28K (Calb), calretinin (Calr), and parvalbumin (Parv), as well as β-amyloid (APP/Aβ and Aβ1–42) and phospho-tau (CP13 and PHF-1) in autopsy tissue from age-matched DS and neurotypical (NTD) subjects ranging from 28-weeks (wk)-gestation to 3 years of age. Thionin, which stains Nissl substance, revealed disorganized cortical cellular lamination including a delayed appearance of pyramidal cells until 44 wk of age in DS compared to 28 wk in NTD. SG and IG DCX-immunoreactive (-ir) cells were only visualized in the youngest cases until 83 wk in NTD and 57 wk DS. Strong SMI-32 immunoreactivity was observed in layers III and V pyramidal cells in the oldest NTD and DS cases with few appearing as early as 28 wk of age in layer V in NTD. Small Calb-ir interneurons were seen in younger NTD and DS cases compared to Calb-ir pyramidal cells in older subjects. Overall, a greater number of Calb-ir cells were detected in NTD, however, the number of Calr-ir cells were comparable between groups. Diffuse APP/Aβ immunoreactivity was found at all ages in both groups. Few young cases from both groups presented non-neuronal granular CP13 immunoreactivity in layer I. Stronger correlations between brain weight, age, thionin, DCX, and SMI-32 counts were found in NTD. These findings suggest that trisomy 21 affects postnatal FC lamination, neuronal migration/neurogenesis and differentiation of projection neurons and interneurons that likely contribute to cognitive impairment in DS.

Published in Acta Neuropathologica Communications

ISSN: 2051-5960 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Neurosciences. Biological psychiatry. Neuropsychiatry: Neurology. Diseases of the nervous system
Website: http://actaneurocomms.biomedcentral.com

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