EphrinB2 knockdown in cervical spinal cord preserves diaphragm innervation in a mutant SOD1 mouse model of ALS

Urban, Mark W.; Charsar, Brittany A.; Heinsinger, Nicolette M.; Markandaiah, Shashirekha S.; Sprimont, Lindsay; Zhou, Wei; Henderson, Nathan T; Ghosh, Biswarup; Cain, Rachel E.; Trotti, Davide; Pasinelli, Piera; Wright, Megan C.; Dalva, Matthew B.; Lepore, Angelo C.

doi:10.7554/elife.89298

Cited by 3 publications

(1 citation statement)

References 70 publications

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“…Recent studies have shown that SERPINA1 [563], LRRK2 [522], CHRNA4 [564], CD22 [565], TF (transferrin) ssociated tyrosine kinase) [579], FGF14 [580], INSC (INSC spindle orientation adaptor protein) [581], BARHL1 [582], PRKCH (protein kinase C eta) [583], SLC24A4 [584], TMEM176B [585], MBP (myelin basic protein) [586], ACAN (aggrecan) [587], SHH (sonic hedgehog signaling molecule) [588], SIRT2 [589], RBP4 [590], ISM1 [591], HOXB6 [592], CDH13 [593], NTF3 [594], TRPC6 [595], MMP3 [596], HLA-DRB5 [597], HLA-DRB1 [546], CD74 [598], VWF (von Willebrand factor) [599], MDGA1 [600], ANGPT2 [601], NEDD4L [602], CASP1 [603], CHRNA5 [604], CCND2 [605], BRCA2 [606], TET1 [607], ZBTB20 [608], OAS1 [609], EGFR (epidermal growth factor receptor) [610], ABCA1 [611], PLXNA4 [612], FOXG1 [613], WEE1 [433], MAP1B [614], ANK1 [615], GRM3 [436], COMT (catechol-O-methyltransferase) [616], SLC10A4 [617], GPR39 [618] and LIFR (LIF receptor subunit alpha) [562] could promote Alzheimer’s disease progression. SERPINA1 [619], LRRK2 [620], CHRNA4 [621], TLR2 [622], MOBP (myelin associated oligodendrocyte basic protein) [623], AATK (apoptosis associated tyrosine kinase) [624], MBP (myelin basic protein) [625], SHH (sonic hedgehog signaling molecule) [626], XDH (xanthine dehydrogenase) [627], RBP4 [628], GRIA2 [629], NR3C2 [630], HLA-DRB5 [631], HLA-DRA [631], NEDD4L [632], CASP1 [633], EFNB2 [634], CYP7B1 [635], EGFR (epidermal growth factor receptor) [636], MAP1B [637], GRM3 [638<...…”

Section: Discussionmentioning

confidence: 99%

Identification of key genes and signaling pathway in the pathogenesis of Huntington's disease via bioinformatics and next generation sequencing data analysis

Vastrad,

Vastrad

2024

Preprint

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Huntington's disease (HD) is the primary cause of progressive motor deficits, psychiatric symptoms, and cognitive impairment. The exact molecular mechanisms of HD pathogenesis are largely unknown. This investigation aims to identify the hub genes, miRNA and TFs in HD and explore their potential molecular regulatory network. Next generation sequencing (NGS) dataset (GSE105041) was extracted from the Gene Expression Omnibus (GEO) database. An integrated bioinformatics pipeline including identification of differentially expressed genes (DEGs), Gene ontology and REACTOME pathway enrichment analysis, protein-protein interaction (PPI) network and module analysis, miRNA-hub gene regulatory network analysis and TF-hub gene regulatory network analysis, and receiver operating characteristic curve (ROC) analysis were applied to identify hub genes, miRNA and TFs, and key drivers of HD pathogenesis. We identified 958 DEGs in the discovery phase, consisting of 479 up regulated genes and 479 down regulated genes. GO and REACTOME enrichment analyses of the 479 up regulated genes and 479 down regulated genes showed that they were mainly involved in multicellular organismal process, developmental process, signaling by GPCR and MHC class II antigen presentation. Further analysis of the PPI network using Cytoscape and PEWCC plugins identified 10 hub genes, including LRRK2, MTUS2, HOXA1, IL7R, ERBB3, EGFR, TEX101, WDR76, NEDD4L and COMT. Possible target miRNAs and TFs, including hsa-mir-1292-5p, hsa-mir-4521, ESRRB and SREBF1, were predicted by constructing a miRNA-hub gene regulatory network analysis and TF-hub gene regulatory network. This investigation used bioinformatics methods to explore the molecular pathogenesis of HD, and identified potential molecular markers. These molecular markers might provide novel ideas and methods for the early diagnosis, treatment, and monitoring of HD.

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Section: Discussionmentioning

confidence: 99%

Identification of key genes and signaling pathway in the pathogenesis of Huntington's disease via bioinformatics and next generation sequencing data analysis

Vastrad,

Vastrad

2024

Preprint

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Early nuclear phenotypes and reactive transformation in human iPSC‐derived astrocytes from ALS patients with SOD1 mutations

Soubannier,

Chaineau,

Gursu

et al. 2024

Glia

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Amyotrophic lateral sclerosis (ALS) is a neurodegenerative disease characterized by the progressive death of motor neurons (MNs). Glial cells play roles in MN degeneration in ALS. More specifically, astrocytes with mutations in the ALS‐associated gene Cu/Zn superoxide dismutase 1 (SOD1) promote MN death. The mechanisms by which SOD1‐mutated astrocytes reduce MN survival are incompletely understood. To characterize the impact of SOD1 mutations on astrocyte physiology, we generated astrocytes from human induced pluripotent stem cell (iPSC) derived from ALS patients carrying SOD1 mutations, together with control isogenic iPSCs. We report that astrocytes harboring SOD1(A4V) and SOD1(D90A) mutations exhibit molecular and morphological changes indicative of reactive astrogliosis when compared to isogenic astrocytes. We show further that a number of nuclear phenotypes precede, or coincide with, reactive transformation. These include increased nuclear oxidative stress and DNA damage, and accumulation of the SOD1 protein in the nucleus. These findings reveal early cell‐autonomous phenotypes in SOD1‐mutated astrocytes that may contribute to the acquisition of a reactive phenotype involved in alterations of astrocyte‐MN communication in ALS.

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Activation of EphrinB2/EphB2 signaling in the spine cord alters glia-neuron interactions in mice with visceral hyperalgesia following maternal separation

Guo,

Wang,

Duan

et al. 2024

Front. Pharmacol.

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BackgroundSress early in life has been linked to visceral hyperalgesia and associated functional gastrointestinal disorders. In a mouse model of visceral hyperalgesia, we investigated whether the EphB2 receptor and its EphrinB2 ligand in spinal cord contribute to dysregulation of glia-neuron interactions.MethodsAn established mouse model of stress due to maternal separation (MS). Pups were separated from their mothers for 14 days during early development, then analyzed several weeks later in terms of visceral sensitivity based on the abdominal withdrawal reflex score and in terms of expression of c-fos, EphrinB2, EphB2, and phosphorylated MAP kinases (ERK, p38, JNK).ResultsVisceral hyperalgesia due to MS upregulated EphB2, EphrinB2 and c-fos in the spinal cord, and c-fos levels positively correlated with those of EphB2 and EphrinB2. Spinal astrocytes, microglia, and neurons showed upregulation of EphB2, EphrinB2 and phosphorylated MAP kinases. Blocking EphrinB2/EphB2 signaling in MS mice reduced visceral sensitivity, activation of neurons and glia, and phosphorylation of NMDA receptor. Activating EphrinB2/EphB2 signaling in unstressed mice induced visceral hyperalgesia, upregulation of c-fos, and activation of NMDA receptor similar to maternal separation.ConclusionThe stress of MS during early development may lead to visceral hyperalgesia by upregulating EphrinB2/EphB2 in the spinal cord and thereby altering neuron-glia interactions.

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EphrinB2 knockdown in cervical spinal cord preserves diaphragm innervation in a mutant SOD1 mouse model of ALS

Cited by 3 publications

References 70 publications

Identification of key genes and signaling pathway in the pathogenesis of Huntington's disease via bioinformatics and next generation sequencing data analysis

Identification of key genes and signaling pathway in the pathogenesis of Huntington's disease via bioinformatics and next generation sequencing data analysis

Early nuclear phenotypes and reactive transformation in human iPSC‐derived astrocytes from ALS patients with SOD1 mutations

Activation of EphrinB2/EphB2 signaling in the spine cord alters glia-neuron interactions in mice with visceral hyperalgesia following maternal separation

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