The effects of telmisartan on the nuclear factor of activated T lymphocytes signalling pathway in hypertensive patients

Huang, Shasha; He, Si-Li; Zhang, Yuanming

doi:10.1177/1470320316655005

Cited by 6 publications

(11 citation statements)

References 29 publications

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“…The sample size calculation was carried out using the G * Power 3.1.9.2 software, and the following values and information were considered: [ 1 ] two groups (control and treatment) and [ 2 ] effect size d = 1.15 considering the variation of TNFα/βactin protein observed in the study by Huang et al (2016) [ 39 ]. In this study, the control group showed 0.45±0.04 (average of arbitrary units ± standard deviation) for TNFα while the telmisartan treated group showed 0.36±0.04 [ 39 ].…”

Section: Methodsmentioning

confidence: 99%

Omega-3 mechanism of action in inflammation and endoplasmic reticulum stress in mononuclear cells from overweight non-alcoholic fatty liver disease participants: study protocol for the “Brazilian Omega Study” (BROS)—a randomized controlled trial

Batista

Rios

Muñoz

et al. 2021

Trials

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The low-grade inflammation is pivotal in obesity and its comorbidities; however, the inflammatory proteins are out of target for traditional drug therapy. Omega-3 (ω3) fatty acids can modulate the downstream signaling of Toll-like receptor (TLR) and tumor necrosis factor-α receptor (TNFα) through GPR120, a G-protein-coupled receptor, a mechanism not yet elucidated in humans. This work aims to investigate if the ω3 supplementation, at a feasible level below the previously recommended level in the literature, is enough to disrupt the inflammation and endoplasmic reticulum stress (ER-stress), and also if in acute treatment (3 h) ω3 can activate the GPR120 in peripheral blood mononuclear cells (PBMC) and leukocytes from overweight non-alcoholic fatty liver disease (NAFLD) participants. The R270H variant of the Ffar4 (GPR120 gene) will also be explored about molecular responses and blood lipid profiles. A triple-blind, prospective clinical trial will be conducted in overweight men and women, aged 19–75 years, randomized into placebo or supplemented (2.2 g of ω3 [EPA+DHA]) groups for 28 days. For sample calculation, it was considered the variation of TNFα protein and a 40% dropout rate, obtaining 22 individuals in each group. Volunteers will be recruited among patients with NAFLD diagnosis. Anthropometric parameters, food intake, physical activity, total serum lipids, complete fatty acid blood profile, and glycemia will be evaluated pre- and post-supplementation. In the PBMC and neutrophils, the protein content and gene expression of markers related to inflammation (TNFα, MCP1, IL1β, IL6, IL10, JNK, and TAK1), ER-stress (ATF1, ATF6, IRE1, XBP1, CHOP, eIF2α, eIF4, HSP), and ω3 pathway (GPR120, β-arrestin2, Tab1/2, and TAK1) will be evaluated using Western blot and RT-qPCR. Participants will be genotyped for the R270H (rs116454156) variant using the TaqMan assay. It is hypothesized that attenuation of inflammation and ER-stress signaling pathways in overweight and NAFLD participants will be achieved through ω3 supplementation through binding to the GPR120 receptor. Trial registration ClinicalTrials.gov #RBR-7x8tbx. Registered on May 10, 2018, with the Brazilian Registry of Clinical Trials.

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Section: Methodsmentioning

confidence: 99%

Omega-3 mechanism of action in inflammation and endoplasmic reticulum stress in mononuclear cells from overweight non-alcoholic fatty liver disease participants: study protocol for the “Brazilian Omega Study” (BROS)—a randomized controlled trial

Batista

Rios

Muñoz

et al. 2021

Trials

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“…A growing body of literature suggests that the family of Ca 2+ /calcineurin-sensitive transcriptional factors of nuclear factor from activated T-cells (NFAT) may play an essential role as a molecular switch that initiates dysfunction in both the endothelium (Cockerill et al, 1995;Boss et al, 1998;Armesilla et al, 1999;Bochkov et al, 2002;Gonzalez Bosc et al, 2004;Zetterqvist et al, 2015;Huang et al, 2016) and vascular smooth muscle (Suzuki et al, 2002;Lipskaia et al, 2003;Amberg et al, 2004;Nilsson et al, 2006;Nieves-Cintrón et al, 2007;Orr et al, 2009;Pang and Sun, 2009;Nilsson-Berglund et al, 2010;Berglund et al, 2012;Shiny et al, 2016;Soudani et al, 2016;Govatati et al, 2019). NFATs regulate multiple downstream mechanisms that initiate vascular dysfunction.…”

Section: Nuclear Factor Kappa-light-chain-enhancer Of Activated B Cells and Nuclear Factor From Activated T Cellsmentioning

confidence: 99%

“…Specifically, NFATs (I) impair endothelial function through NO-dependent mechanisms (Armesilla et al, 1999;Bochkov et al, 2002;Johnson et al, 2003;Norata et al, 2007;Garcia-Vaz et al, 2020;Wang et al, 2020), (II) increase the expression of inflammatory mediators in the arterial wall promoting atherosclerosis (Pierce et al, 1996;Pang and Sun, 2009;Nilsson-Berglund et al, 2010;Berglund et al, 2012;Zetterqvist et al, 2014;Weng et al, 2017), and (III) initiate pathogenic VSM proliferation (Suzuki et al, 2002;Lipskaia et al, 2003;Nilsson et al, 2006;Nieves-Cintrón et al, 2007;Donato et al, 2009;Orr et al, 2009;Pang and Sun, 2009;Nilsson-Berglund et al, 2010;Yan et al, 2015;Shiny et al, 2016;Soudani et al, 2016;Govatati et al, 2019). In preclinical models, inhibition of NFAT has prevented the activation of inflammatory cytokines (Kiani et al, 2000;Zetterqvist et al, 2014;Bretz et al, 2015;Huang et al, 2016), enhanced eNOS expression (Smith et al, 2011), increased NO bioavailability (Friedman et al, 2014;Zetterqvist et al, 2014Zetterqvist et al, , 2015Garcia-Vaz et al, 2020), prevented VSM proliferation (Lipskaia et al, 2003;Berglund et al, 2012;Shiny et al, 2016…”

Section: Nuclear Factor Kappa-light-chain-enhancer Of Activated B Cells and Nuclear Factor From Activated T Cellsmentioning

confidence: 99%

“…Currently, these investigations/findings are limited to cellular and animal models. There are promising approaches, including examining NFATs in the skin microcirculation and in peripheral blood mononuclear cells, for investigating the role of NFATs in humans (Huang et al, 2016). Elucidation of the role of NFATs and their putative upstream contributions to the vascular health triad in humans is still needed.…”

Section: Nuclear Factor Kappa-light-chain-enhancer Of Activated B Cells and Nuclear Factor From Activated T Cellsmentioning

confidence: 99%

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Vascular Health Triad in Humans With Hypertension—Not the Usual Suspects

2021

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Hypertension (HTN) affects more than one-third of the US population and remains the top risk factor for the development of cardiovascular disease (CVD). Identifying the underlying mechanisms for developing HTN are of critical importance because the risk of developing CVD doubles with ∼20 mmHg increase in systolic blood pressure (BP). Endothelial dysfunction, especially in the resistance arteries, is the primary site for initiation of sub-clinical HTN. Furthermore, inflammation and reactive oxygen and nitrogen species (ROS/RNS) not only influence the endothelium independently, but also have a synergistic influence on each other. Together, the interplay between inflammation, ROS and vascular dysfunction is referred to as the vascular health triad, and affects BP regulation in humans. While the interplay of the vascular health triad is well established, new underlying mechanistic targets are under investigation, including: Inducible nitric oxide synthase, hydrogen peroxide, hydrogen sulfide, nuclear factor kappa-light-chain-enhancer of activated B cells (NF-κB) and nuclear factor activated T cells. This review outlines the role of these unusual suspects in vascular health and function in humans. This review connects the dots using these unusual suspects underlying inflammation, ROS and vascular dysfunction especially in individuals at risk of or with diagnosed HTN based on novel studies performed in humans.

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“…It was reported that NFATC1 was highly expressed in hypertension, carcinomas, osteoporosis, and other age-associated diseases [15][16][17][18]. It has been shown in an animal study that the hair follicle stem cells of aged mice could maintain cell activity, generate hair and make the hair stay in youth when NFATC1 was inhibited [19].…”

Section: Introductionmentioning

confidence: 99%

DNA Methylation in NFATC1 Gene Promoter is Related to Longevity in Chinese Population

Li¹,

Xi²,

Zhang³

et al. 2017

Hereditary Genet

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The effects of telmisartan on the nuclear factor of activated T lymphocytes signalling pathway in hypertensive patients

Cited by 6 publications

References 29 publications

Omega-3 mechanism of action in inflammation and endoplasmic reticulum stress in mononuclear cells from overweight non-alcoholic fatty liver disease participants: study protocol for the “Brazilian Omega Study” (BROS)—a randomized controlled trial

Omega-3 mechanism of action in inflammation and endoplasmic reticulum stress in mononuclear cells from overweight non-alcoholic fatty liver disease participants: study protocol for the “Brazilian Omega Study” (BROS)—a randomized controlled trial

Vascular Health Triad in Humans With Hypertension—Not the Usual Suspects

DNA Methylation in NFATC1 Gene Promoter is Related to Longevity in Chinese Population

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