Pioglitazone Attenuates the Effects of Peripheral Inflammation in a Human In Vitro Blood–Brain Barrier Model

Rocha, Gustavo Henrique Oliveira da; Loiola, Rodrigo Azevedo; Paula-Silva, Marina de; Shimizu, Fumitaka; Kanda, Takashi; Vieira, Andréa; Gosselet, Fabien; Farsky, Sandra Helena Poliselli

doi:10.3390/ijms232112781

Cited by 11 publications

(5 citation statements)

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“…The RNA-seq analysis revealed increases in IFITM3 expression in bEnd.3 cells co-cultured with LPS-activated Raw264.7 cells but such increases were not found at protein levels by western blot analysis ( Fig 4E and 4F ). Cytokines/chemokines and other secreted molecules during systemic inflammation may impair the BBB integrity [ 55 ]. At the BBB, the most abundant tight junction protein is claudin-5 that is involved in progression of neurodegenerative disorders including AD [ 56 ].…”

Section: Resultsmentioning

confidence: 99%

“…Catorce and Gevorkian [ 63 ] reviewed LPS-induced murine neuroinflammation models and suggested that peripherally induced inflammation by LPS may trigger neuroinflammation leading to Aβ and/or tau pathology, neurodegeneration and cognitive impairment. Considering increased BBB permeability by LPS [ 55 , 65 ] and fibrinogen infiltration via a leaky BBB [ 85 ], we investigated the BBB permeability by immunofluorescence microscopy using antibodies specific to fibrinogen and CD31, a marker for endothelial cells. We found that fibrinogen fluorescence signals were increased and exclusively limited to the areas positive for CD31 fluorescence signals in LPS-treated mice ( Fig 6 ), indicating that LPS treatment did not induce infiltration of fibrinogen into the brain parenchyma.…”

Section: Discussionmentioning

confidence: 99%

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A novel co-culture model for investigation of the effects of LPS-induced macrophage-derived cytokines on brain endothelial cells

Yang

Bhalla

et al. 2023

PLoS ONE

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In order to study effects of macrophage-derived inflammatory mediators associated with systemic inflammation on brain endothelial cells, we have established a co-culture system consisting of bEnd.3 cells and LPS-activated Raw 264.7 cells and performed its cytokine profiling. The cytokine profile of the co-culture model was compared to that of mice treated with intraperitoneal LPS injection. We found that, among cytokines profiled, eight cytokines/chemokines were similarly upregulated in both in vivo mouse and in vitro co-culture model. In contrast to the co-culture model, the cytokine profile of a common mono-culture system consisting of only LPS-activated bEnd.3 cells had little similarity to that of the in vivo mouse model. These results indicate that the co-culture of bEnd.3 cells with LPS-activated Raw 264.7 cells is a better model than the common mono-culture of LPS-activated bEnd.3 cells to investigate the molecular mechanism in endothelial cells, by which systemic inflammation induces neuroinflammation. Moreover, fibrinogen adherence both to bEnd.3 cells in the co-culture and to brain blood vessels in a LPS-treated animal model of Alzheimer’s disease increased. To the best of our knowledge, this is the first to utilize bEnd.3 cells co-cultured with LPS-activated Raw 264.7 cells as an in vitro model to investigate the consequence of macrophage-derived inflammatory mediators on brain endothelial cells.

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

A novel co-culture model for investigation of the effects of LPS-induced macrophage-derived cytokines on brain endothelial cells

Yang

Bhalla

et al. 2023

PLoS ONE

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“…Pioglitazone attenuates inflammation, 29 while both T2DM 30 and fatty liver disease 31 are associated with increased levels of inflammatory markers. Hence, the beneficial effects of pioglitazone on both diabetes and SLD may be the result of an attenuation of inflammation.…”

Section: Discussionmentioning

confidence: 99%

Factors associated with treatment responses to pioglitazone in patients with steatotic liver disease: A 3‐year prospective cohort study

Chang,

Tai,

Cheng

et al. 2024

Diabetes Obesity Metabolism

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AimThe response rate to pioglitazone and the predictive factors for its effects on improving liver biochemistry in patients with steatotic liver disease (SLD) remain elusive, so we aimed to investigate these issues.MethodsA 3‐year prospective cohort study of 126 Taiwanese patients with SLD treated with pioglitazone (15‐30 mg/day) was conducted. Phospholipase domain‐containing protein 3 I148M rs738409, methylenetetrahydrofolate reductase rs1801133, aldehyde dehydrogenase 2 (ALDH2) rs671 and lipoprotein lipase rs10099160 single nucleotide polymorphisms were assessed in the patients.ResultsOf 126 patients, 78 (61.9%) were men, and the mean and median ages were 54.3 and 56.5 years, respectively. Pioglitazone responders were defined as those with decreased alanine aminotransferase (ALT) levels at 6 months post‐treatment, and 105 (83.3%) patients were responders. Compared with non‐responders, responders were more frequently women and had higher baseline ALT levels. The proportion of patients with the ALDH2 rs671 GG genotype was lower among responders (38.6% vs. 66.6%, p = .028). Female sex [odds ratio (OR): 4.514, p = .023] and baseline ALT level (OR: 1.015, p = .046; cut‐off level: ≥82 U/L) were associated with pioglitazone response. Among responders, the liver biochemistry and homeostasis model assessment of insulin resistance improved from 6 to 24 months post‐treatment. The total cholesterol levels decreased within 6 months, while increases in high‐density lipoprotein cholesterol levels and decreases in triglyceride levels and fibrosis‐4 scores were noted only at 24 months post‐treatment. The 2‐year cumulative incidences of cardiovascular events, cancers and hepatic events were similar between responders and non‐responders.ConclusionsRegarding liver biochemistry, over 80% of Taiwanese patients with SLD had a pioglitazone response, which was positively associated with female sex and baseline ALT levels. Insulin resistance improved as early as 6 months post‐treatment, while liver fibrosis improvement was not observed until 24 months post‐treatment. The link between the pioglitazone response and the ALDH2 genotype warrants further investigation.

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“…When ready, HBP were rinsed once with warm DMEM/HG/0.1% BSA and then incubated in DMEM/HG/0.1% BSA supplemented or not with 5 or 10 ng/mL of TNFα. These concentrations were selected based on previous in vitro studies published by us and others [ 64 , 65 , 66 , 67 ].…”

Section: Methodsmentioning

confidence: 99%

TNFα Activates the Liver X Receptor Signaling Pathway and Promotes Cholesterol Efflux from Human Brain Pericytes Independently of ABCA1

Dib

Loiola

Sevin

et al. 2023

IJMS

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Neuroinflammation and brain lipid imbalances are observed in Alzheimer’s disease (AD). Tumor necrosis factor-α (TNFα) and the liver X receptor (LXR) signaling pathways are involved in both processes. However, limited information is currently available regarding their relationships in human brain pericytes (HBP) of the neurovascular unit. In cultivated HBP, TNFα activates the LXR pathway and increases the expression of one of its target genes, the transporter ATP-binding cassette family A member 1 (ABCA1), while ABCG1 is not expressed. Apolipoprotein E (APOE) synthesis and release are diminished. The cholesterol efflux is promoted, but is not inhibited, when ABCA1 or LXR are blocked. Moreover, as for TNFα, direct LXR activation by the agonist (T0901317) increases ABCA1 expression and the associated cholesterol efflux. However, this process is abolished when LXR/ABCA1 are both inhibited. Neither the other ABC transporters nor the SR-BI are involved in this TNFα-mediated lipid efflux regulation. We also report that inflammation increases ABCB1 expression and function. In conclusion, our data suggest that inflammation increases HBP protection against xenobiotics and triggers an LXR/ABCA1 independent cholesterol release. Understanding the molecular mechanisms regulating this efflux at the level of the neurovascular unit remains fundamental to the characterization of links between neuroinflammation, cholesterol and HBP function in neurodegenerative disorders.

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Pioglitazone Attenuates the Effects of Peripheral Inflammation in a Human In Vitro Blood–Brain Barrier Model

Cited by 11 publications

References 68 publications

A novel co-culture model for investigation of the effects of LPS-induced macrophage-derived cytokines on brain endothelial cells

A novel co-culture model for investigation of the effects of LPS-induced macrophage-derived cytokines on brain endothelial cells

Factors associated with treatment responses to pioglitazone in patients with steatotic liver disease: A 3‐year prospective cohort study

TNFα Activates the Liver X Receptor Signaling Pathway and Promotes Cholesterol Efflux from Human Brain Pericytes Independently of ABCA1

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