PUBLICATION

Integrative systems and functional analyses reveal a role of dopaminergic signaling in myelin pathogenesis

Authors

Ding, S., Gu, Y., Cai, Y., Cai, M., Yang, T., Bao, S., Shen, W., Ni, X., Chen, G., Xing, L.

ID

ZDB-PUB-200304-28

Date

2020

Source

Journal of translational medicine 18: 109 (Journal)

Registered Authors

Keywords

Dopaminergic signaling, genetics, in vivo analysis, myelin pathogenesis, transcriptome, zebrafish

MeSH Terms

Clustered Regularly Interspaced Short Palindromic Repeats
Animals
CRISPR-Associated Protein 9
Myelin Sheath*
Signal Transduction
Zebrafish*/genetics
Humans

(all 7)

PubMed

32122379 Full text @ J Transl Med

Abstract

Background Myelin sheaths surrounding axons are critical for electrical signal transmission in the central nervous system (CNS). Diseases with myelin defects such as multiple sclerosis (MS) are devastating neurological conditions for which few effective treatments are available. Dysfunction of the dopaminergic system has been observed in multiple neurological disorders. Its role in myelin pathogenesis, however, is unclear.

Methods This work used a combination of literature curation, bioinformatics, pharmacological and genetic manipulation, as well as confocal imaging techniques. Literature search was used to establish a complete set of genes which is associated with MS in humans. Bioinformatics analyses include pathway enrichment and crosstalk analyses with human genetic association studies as well as gene set enrichment and causal relationship analyses with transcriptome data. Pharmacological and CRISPR/Cas9 (clustered regularly interspaced short palindromic repeats/CRISPR-associated protein 9) genetic manipulation were applied to inhibit the dopaminergic signaling in zebrafish. Imaging techniques were used to visualize myelin formation in vivo.

Results Systematic analysis of human genetic association studies revealed that the dopaminergic synapse signaling pathway is enriched in candidate gene sets. Transcriptome analysis confirmed that expression of multiple dopaminergic gene sets was significantly altered in patients with MS. Pathway crosstalk analysis and gene set causal relationship analysis reveal that the dopaminergic synapse signaling pathway interacts with or is associated with other critical pathways involved in MS. We also found that disruption of the dopaminergic system leads to myelin deficiency in zebrafish.

Conclusions Dopaminergic signaling may be involved in myelin pathogenesis. This study may offer a novel molecular mechanism of demyelination in the nervous system.

Genes / Markers

Figures

Show all Figures

Expression

Phenotype

Fish	Conditions	Stage	Phenotype	Figure
ck1Tg	chemical treatment: oxidopamine	Protruding-mouth	dopaminergic neuron decreased amount, abnormal	Fig. 4
ck1Tg	chemical treatment: oxidopamine	Protruding-mouth	myelination disrupted, abnormal	Fig. 4
ck1Tg + CRISPR2-otpa + CRISPR2-otpb	standard conditions	Protruding-mouth	myelination disrupted, abnormal	Fig. 5
ck1Tg + CRISPR2-otpa + CRISPR2-otpb	standard conditions	Protruding-mouth	whole organism dopamine decreased amount, abnormal	Fig. 5

1 - 4 of 4

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Mutations / Transgenics

Allele	Construct	Type	Affected Genomic Region
ck1Tg	Tg(mbp:EGFP)	Transgenic Insertion

Human Disease / Model

Human Disease	Fish	Conditions	Evidence
multiple sclerosis			TAS

Sequence Targeting Reagents

Target	Reagent	Reagent Type
otpa	CRISPR2-otpa	CRISPR
otpb	CRISPR2-otpb	CRISPR

Fish

Fish
ck1Tg
ck1Tg + CRISPR2-otpa + CRISPR2-otpb

Antibodies

Orthology

Engineered Foreign Genes

Marker	Marker Type	Name
EGFP	EFG	EGFP

Mapping

Ding et al., 2020 ZDB-PUB-200304-28 PMID:32122379

Integrative systems and functional analyses reveal a role of dopaminergic signaling in myelin pathogenesis

Ding et al., 2020

ZDB-PUB-200304-28
PMID:32122379