Molecular Framework of Mouse Endothelial Cell Dysfunction during Inflammation: A Proteomics Approach

Rossi, Michael T.; Langston, Jordan C.; Singh, Narender; Merali, Carmen; Yang, Qingliang; Merali, Salim; Prabhakarpandian, Balabhaskar; Kilpatrick, Laurie E.; Kiani, Mohammad F.

doi:10.3390/ijms23158399

Cited by 7 publications

(17 citation statements)

References 64 publications

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“…The 716 downregulated genes in the kidney are enriched in tube morphogenesis, kidney development, GTPase-mediated signal transduction, regulation of TORC1 signaling, and glomerulus vasculature (Fig. 4 a, b, h–l and Additional file 4 : Table S3)—suggesting vascular functions are dysregulated in inflammation [ 57 – 59 ]. In summary, these data support the concept that over-activation of cytokine signaling and dysregulation of tube morphogenesis are evident in the kidney following infection and inflammatory response.…”

Section: Resultsmentioning

confidence: 99%

Commonly disrupted pathways in brain and kidney in a pig model of systemic endotoxemia

Olney,

de Ávila,

Todd

et al. 2024

J Neuroinflammation

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Sepsis is a life-threatening state that arises due to a hyperactive inflammatory response stimulated by infection and rarely other insults (e.g., non-infections tissue injury). Although changes in several proinflammatory cytokines and signals are documented in humans and small animal models, far less is known about responses within affected tissues of large animal models. We sought to understand the changes that occur during the initial stages of inflammation by administering intravenous lipopolysaccharide (LPS) to Yorkshire pigs and assessing transcriptomic alterations in the brain, kidney, and whole blood. Robust transcriptional alterations were found in the brain, with upregulated responses enriched in inflammatory pathways and downregulated responses enriched in tight junction and blood vessel functions. Comparison of the inflammatory response in the pig brain to a similar mouse model demonstrated some overlapping changes but also numerous differences, including oppositely dysregulated genes between species. Substantial changes also occurred in the kidneys following LPS with several enriched upregulated pathways (cytokines, lipids, unfolded protein response, etc.) and downregulated gene sets (tube morphogenesis, glomerulus development, GTPase signal transduction, etc.). We also found significant dysregulation of genes in whole blood that fell into several gene ontology categories (cytokines, cell cycle, neutrophil degranulation, etc.). We observed a strong correlation between the brain and kidney responses, with significantly shared upregulated pathways (cytokine signaling, cell death, VEGFA pathways) and downregulated pathways (vasculature and RAC1 GTPases). In summary, we have identified a core set of shared genes and pathways in a pig model of systemic inflammation.

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Section: Resultsmentioning

confidence: 99%

Commonly disrupted pathways in brain and kidney in a pig model of systemic endotoxemia

Olney,

de Ávila,

Todd

et al. 2024

J Neuroinflammation

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“…Nevertheless, the ECS exists within various peripheral immune cells like T cells, B cells, and macrophages, potentially influencing their operations 78–80 . Several studies demonstrate the ECS's capacity to manage immune responses, inflammation, and cytokine production in peripheral tissues 81–84 . Consequently, it seems reasonable to postulate that the ECS might also impact the non‐CNS immune system, but this premise requires further investigation.…”

Section: Discussionmentioning

confidence: 99%

Probing molecular pathways: Illuminating the connection between COVID‐19 and Alzheimer's disease through the endocannabinoid system dynamics

Sun,

Gao,

et al. 2024

Journal of Medical Virology

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Our study investigates the molecular link between COVID‐19 and Alzheimer's disease (AD). We aim to elucidate the mechanisms by which COVID‐19 may influence the onset or progression of AD. Using bioinformatic tools, we analyzed gene expression datasets from the Gene Expression Omnibus (GEO) database, including GSE147507, GSE12685, and GSE26927. Intersection analysis was utilized to identify common differentially expressed genes (CDEGs) and their shared biological pathways. Consensus clustering was conducted to group AD patients based on gene expression, followed by an analysis of the immune microenvironment and variations in shared pathway activities between clusters. Additionally, we identified transcription factor‐binding sites shared by CDEGs and genes in the common pathway. The activity of the pathway and the expression levels of the CDEGs were validated using GSE164805 and GSE48350 datasets. Six CDEGs (MAL2, NECAB1, SH3GL2, EPB41L3, MEF2C, and NRGN) were identified, along with a downregulated pathway, the endocannabinoid (ECS) signaling pathway, common to both AD and COVID‐19. These CDEGs showed a significant correlation with ECS activity (p < 0.05) and immune functions. The ECS pathway was enriched in healthy individuals' brains and downregulated in AD patients. Validation using GSE164805 and GSE48350 datasets confirmed the differential expression of these genes in COVID‐19 and AD tissues. Our findings reveal a potential pathogenetic link between COVID‐19 and AD, mediated by CDEGs and the ECS pathway. However, further research and multicenter evidence are needed to translate these findings into clinical applications.

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“…Both oxidative stress and inflammation are driven by hypoxia ( Biddlestone et al, 2015 ; McGarry et al, 2018 ; Korbecki et al, 2021 ; Mesentier-Louro et al, 2021 ), which could explain why anti-oxidative therapies alone cannot restore cellular redox homeostasis ( Tretter et al, 2021 ). Endothelial cell biology of functions and dysfunctions ( Charreau, 2022 ) is an emerging approach to understanding microvascular endothelial heterogeneity and inflammation ( Yang et al, 2021c ; Rossi et al, 2022 ). Impaired endothelial function is thought to contribute to the increased cardiovascular risk ( Craighead et al, 2020 ), vascular aging associated with atherosclerotic ischemic stroke ( Koutsaliaris et al, 2022 ), and oxidative stress–inflammation in chronic kidney disease ( Ebert et al, 2021 ).…”

Section: Discussionmentioning

confidence: 99%

Understanding human aging and the fundamental cell signaling link in age-related diseases: the middle-aging hypovascularity hypoxia hypothesis

Phua

2023

Front. Aging

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Aging-related hypoxia, oxidative stress, and inflammation pathophysiology are closely associated with human age-related carcinogenesis and chronic diseases. However, the connection between hypoxia and hormonal cell signaling pathways is unclear, but such human age-related comorbid diseases do coincide with the middle-aging period of declining sex hormonal signaling. This scoping review evaluates the relevant interdisciplinary evidence to assess the systems biology of function, regulation, and homeostasis in order to discern and decipher the etiology of the connection between hypoxia and hormonal signaling in human age-related comorbid diseases. The hypothesis charts the accumulating evidence to support the development of a hypoxic milieu and oxidative stress-inflammation pathophysiology in middle-aged individuals, as well as the induction of amyloidosis, autophagy, and epithelial-to-mesenchymal transition in aging-related degeneration. Taken together, this new approach and strategy can provide the clarity of concepts and patterns to determine the causes of declining vascularity hemodynamics (blood flow) and physiological oxygenation perfusion (oxygen bioavailability) in relation to oxygen homeostasis and vascularity that cause hypoxia (hypovascularity hypoxia). The middle-aging hypovascularity hypoxia hypothesis could provide the mechanistic interface connecting the endocrine, nitric oxide, and oxygen homeostasis signaling that is closely linked to the progressive conditions of degenerative hypertrophy, atrophy, fibrosis, and neoplasm. An in-depth understanding of these intrinsic biological processes of the developing middle-aged hypoxia could provide potential new strategies for time-dependent therapies in maintaining healthspan for healthy lifestyle aging, medical cost savings, and health system sustainability.

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Molecular Framework of Mouse Endothelial Cell Dysfunction during Inflammation: A Proteomics Approach

Cited by 7 publications

References 64 publications

Commonly disrupted pathways in brain and kidney in a pig model of systemic endotoxemia

Commonly disrupted pathways in brain and kidney in a pig model of systemic endotoxemia

Probing molecular pathways: Illuminating the connection between COVID‐19 and Alzheimer's disease through the endocannabinoid system dynamics

Understanding human aging and the fundamental cell signaling link in age-related diseases: the middle-aging hypovascularity hypoxia hypothesis

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