Basal forebrain cholinergic neurons are vulnerable in a mouse model of Down syndrome and their molecular fingerprint is rescued by maternal choline supplementation-Reference-Cited by-同舟云学术

Basal forebrain cholinergic neurons are vulnerable in a mouse model of Down syndrome and their molecular fingerprint is rescued by maternal choline supplementation

Published:2023-05-16 Issue:6 Volume:37 Page:
ISSN:0892-6638
Container-title:The FASEB Journal
language:en
Short-container-title:The FASEB Journal

Author:

Alldred Melissa J.¹²,Pidikiti Harshitha¹,Heguy Adriana³,Roussos Panos¹⁴⁵⁶,Ginsberg Stephen D.¹²⁷⁸^ORCID

Affiliation:

1. Center for Dementia Research, Nathan Kline Institute Orangeburg New York USA

2. Department of Psychiatry New York University Grossman School of Medicine New York New York USA

3. Genome Technology Center, New York University Grossman School of Medicine New York New York USA

4. Department of Genetics and Genomic Sciences Icahn School of Medicine at Mount Sinai New York New York USA

5. Department of Psychiatry Icahn School of Medicine at Mount Sinai New York New York USA

6. The Institute for Data Science and Genomic Technology, Icahn School of Medicine at Mount Sinai New York New York USA

7. Department of Neuroscience & Physiology New York University Grossman School of Medicine New York New York USA

8. NYU Neuroscience Institute, New York University Grossman School of Medicine New York New York USA

Abstract

AbstractBasal forebrain cholinergic neuron (BFCN) degeneration is a hallmark of Down syndrome (DS) and Alzheimer's disease (AD). Current therapeutics in these disorders have been unsuccessful in slowing disease progression, likely due to poorly understood complex pathological interactions and dysregulated pathways. The Ts65Dn trisomic mouse model recapitulates both cognitive and morphological deficits of DS and AD, including BFCN degeneration and has shown lifelong behavioral changes due to maternal choline supplementation (MCS). To test the impact of MCS on trisomic BFCNs, we performed laser capture microdissection to individually isolate choline acetyltransferase‐immunopositive neurons in Ts65Dn and disomic littermates, in conjunction with MCS at the onset of BFCN degeneration. We utilized single population RNA sequencing (RNA‐seq) to interrogate transcriptomic changes within medial septal nucleus (MSN) BFCNs. Leveraging multiple bioinformatic analysis programs on differentially expressed genes (DEGs) by genotype and diet, we identified key canonical pathways and altered physiological functions within Ts65Dn MSN BFCNs, which were attenuated by MCS in trisomic offspring, including the cholinergic, glutamatergic and GABAergic pathways. We linked differential gene expression bioinformatically to multiple neurological functions, including motor dysfunction/movement disorder, early onset neurological disease, ataxia and cognitive impairment via Ingenuity Pathway Analysis. DEGs within these identified pathways may underlie aberrant behavior in the DS mice, with MCS attenuating the underlying gene expression changes. We propose MCS ameliorates aberrant BFCN gene expression within the septohippocampal circuit of trisomic mice through normalization of principally the cholinergic, glutamatergic, and GABAergic signaling pathways, resulting in attenuation of underlying neurological disease functions.

Funder

National Institutes of Health

Publisher

Wiley

Subject

Genetics,Molecular Biology,Biochemistry,Biotechnology

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