Neuroinflammatory processes are augmented in mice overexpressing human heat-shock protein B1 following ethanol-induced brain injury

Dukay, Brigitta; Walter, Fruzsina R.; Vigh, Judit P.; Barabási, Beáta; Hajdu, Petra; Balassa, Tamás; Migh, Ede; Kincses, András; Hoyk, Zsófia; Szögi, Titanilla; Borbély, Emöke; Csoboz, Bálint; Horváth, Péter; Fülöp, Lívia; Penke, Botond; Vı́gh, László; Deli, Mária A.; Sántha, Miklós; Tóth, Melinda E.

doi:10.1186/s12974-020-02070-2

Cited by 18 publications

(13 citation statements)

References 97 publications

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“…A heat map indicating relative expression of the downstream target molecules identified in our proteomic analysis for all three regions is depicted in Figure 3b. Many of the mapped strongly elevated proteins common to the hippocampus and thalamus are specifically expressed in astrocytes, including Hspb1, S100a6, Clu, Htra1, and GFAP (Dukay et al, 2021;Launay et al, 2008;Morgan et al, 1995;Nafar et al, 2016;Yamashita et al, 1999), while other markers such as Vim and ApoE can be expressed in both astrocytes and microglia (Graeber et al, 1988;O'Leary et al, 2020). Activation of TGF-β1 is consistent with our recent findings that its mRNA expression is significantly elevated in 12 M rTg-DI rats (Zhu, Hatfield, et al, 2020).…”

Section: Ipa Reveals Distinct Upstream Regulators and Casual Networksupporting

confidence: 89%

Distinct brain regional proteome changes in the rTg‐DI rat model of cerebral amyloid angiopathy

Schrader

Nostrand

2021

Journal of Neurochemistry

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calcium binding protein A4; S100A6, S100 calcium binding protein A6; SVD, small vessel disease; SWATH-MS, Sequential Window Acquisition of all Theoretical Mass Spectra-MS; Syt2, synaptotagmin-2; TGF-β1, transforming growth factor β1; TNFα, tumor necrosis factor α; TOF-MS, time of flight MS; TPA, total protein approach; UPLC, ultra performance liquid chromatography; VCID, vascular cognitive impairment and dementia; Vim, vimentin; XIC, extracted ion current chromatogram.

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Section: Ipa Reveals Distinct Upstream Regulators and Casual Networksupporting

confidence: 89%

Distinct brain regional proteome changes in the rTg‐DI rat model of cerebral amyloid angiopathy

Schrader

Nostrand

2021

Journal of Neurochemistry

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“…Previous studies have shown that sHsps are anti-inflammatory proteins. Overexpression of HspB1 ameliorates neuroinflammation caused by ethanol-induced brain injury in mice ( Dukay et al, 2021 ). HspB5 reduces inflammation by decreasing the secretion of proinflammatory cytokines in animal models of multiple sclerosis, ischemia, or nerve crush injury ( Kurnellas et al, 2012 ; Rothbard et al, 2012 ; Lim et al, 2021 ).…”

Section: Introductionmentioning

confidence: 99%

Small Heat Shock Proteins in Retinal Diseases

Rajeswaren

Wong

Yabroudi

et al. 2022

Front. Mol. Biosci.

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This review summarizes the latest findings on small heat shock proteins (sHsps) in three major retinal diseases: glaucoma, diabetic retinopathy, and age-related macular degeneration. A general description of the structure and major cellular functions of sHsps is provided in the introductory remarks. Their role in specific retinal diseases, highlighting their regulation, role in pathogenesis, and possible use as therapeutics, is discussed.

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“…As_9, over-represented in the E3 LPS brain, exhibited hallmark genes associated with scar formation and wound healing ( Cspg5, Htra1 ), 25,26 , while E4 LPS-enriched As_8/11 subtypes clustered similarly together and expressed genes associated with pro-inflammatory response ( Lcn2, Cxcl10 ), as well as oxidative stress and metal cation buffering (Fig. 1d; Hsbp1, S100a6, Mt1, Mt2 ) 27–29 . Using Monocle2 as an alternate analysis pipeline, we demonstrate via pseudotime trajectory that several of the hallmark genes from As_8/11 are highly expressed in the E4_LPS condition (Fig 1e; purple).…”

Section: Resultsmentioning

confidence: 98%

APOE4drives transcriptional heterogeneity and maladaptive immunometabolic responses of astrocytes

Lee

Williams

Gorman

et al. 2023

Preprint

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Apolipoprotein E4 (APOE4) is the strongest risk allele associated with the development of late onset Alzheimers disease (AD). Across the CNS, astrocytes are the predominant expressor of ApoE while also being critical mediators of neuroinflammation and cerebral metabolism. APOE4 has been consistently linked with dysfunctional inflammation and metabolic processes, yet insights into the molecular constituents driving these responses remain unclear. Utilizing complementary approaches across humanized APOE mice and isogenic human iPSC astrocytes, we demonstrate that ApoE4 alters the astrocyte immunometabolic response to pro-inflammatory stimuli. Our findings demonstrate that ApoE4-expressing astrocytes acquire distinct transcriptional repertoires at single-cell and spatially-resolved domains, which are driven in-part by preferential utilization of the cRel transcription factor. Further, inhibiting cRel translocation in ApoE4 astrocytes abrogates inflammatory-induced glycolytic shift and in tandem mitigates production of multiple pro-inflammatory cytokines. Altogether, our findings elucidate novel cellular underpinnings by which ApoE4 drives maladaptive immunometabolic responses of astrocytes.

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Neuroinflammatory processes are augmented in mice overexpressing human heat-shock protein B1 following ethanol-induced brain injury

Cited by 18 publications

References 97 publications

Distinct brain regional proteome changes in the rTg‐DI rat model of cerebral amyloid angiopathy

Distinct brain regional proteome changes in the rTg‐DI rat model of cerebral amyloid angiopathy

Small Heat Shock Proteins in Retinal Diseases

APOE4drives transcriptional heterogeneity and maladaptive immunometabolic responses of astrocytes

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