Sodium butyrate attenuates angiotensin II‐induced cardiac hypertrophy by inhibiting COX2/PGE2 pathway via a HDAC5/HDAC6‐dependent mechanism

Zhang, Linlin; Deng, Mokan; Lu, Aihua; Chen, Yanting; Yang, Chen; Wu, Chun-Ying; Tan, Zhi; Boini, Krishna M.; Yang, Tianxin; Zhu, Qing; Wang, Lei

doi:10.1111/jcmm.14684

Cited by 67 publications

(73 citation statements)

References 43 publications

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“…For quantitative reverse transcription PCR (qRT-PCR), total RNA isolation was performed as previously described 33 . Reverse transcription and SYBR green based quantitative polymerase chain reaction were performed as the manufacturer's instructions (TsingKe Biological Technology, TSE202).…”

Section: Quantitative Reverse Transcriptase Pcrmentioning

confidence: 99%

ELABELA attenuates deoxycorticosterone acetate/salt-induced hypertension and renal injury by inhibition of NADPH oxidase/ROS/NLRP3 inflammasome pathway

Chen

Liu

et al. 2020

Cell Death Dis

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ELABELA (ELA), a 32-residue hormone peptide abundantly expressed in adult kidneys, has been identified as a novel endogenous ligand for APJ/Apelin receptor. The aim of this study was to investigate the role of ELA in deoxycorticosterone acetate (DOCA)/salt-induced hypertension and further explore the underlying mechanism. In DOCA/salt-treated rats, the mRNA level of ELA greatly decreased in the renal medulla. Next, overexpression of ELA in the kidney was found to attenuate DOCA/salt-induced hypertension and renal injury, including lower blood pressure, reversed glomerular morphological damage, decreased blood urea nitrogen (BUN), and blocked the accumulation of fibrotic markers. Mechanistically, ELA overexpression inhibited renal nicotinamide adenine dinucleotide phosphate (NADPH) oxidase activity and subsequent reactive oxygen species (ROS) production, thus resulted in the blockade of formation and activation of Nod-like receptor protein 3 (NLRP3) inflammasome. The inhibitory effects of ELA on Aldosterone-stimulated NADPH oxidase/ROS/NLRP3 inflammasome pathway were confirmed in the human renal tubular cells. Furthermore, our in vivo and in vitro results showed that the deficiency of the apelin receptor APJ did not influence the antihypertensive effect and blockage to NADPH oxidase/ROS/NLRP3 pathway of ELA. Moreover, in heterozygous ELA knockout mice (ELA+/−), the ELA deficiency remarkably accelerated the onset of DOCA/salt-induced hypertension. Our data demonstrate that ELA prevents DOCA/salt-induced hypertension by inhibiting NADPH oxidase/ROS/NLRP3 pathway in the kidney, which is APJ independent. Pharmacological targeting of ELA may serve as a novel therapeutic strategy for the treatment of hypertensive kidney disease.

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Section: Quantitative Reverse Transcriptase Pcrmentioning

confidence: 99%

ELABELA attenuates deoxycorticosterone acetate/salt-induced hypertension and renal injury by inhibition of NADPH oxidase/ROS/NLRP3 inflammasome pathway

Chen

Liu

et al. 2020

Cell Death Dis

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“…8, Fig. 4B) simultaneously using reported relative changes in LV mass from VO [29,42,48,[55][56][57][58][59][60] and AngII infusion [19][20][21][22][23][24][25][26] experiments in rats. To simulate VO, we set the circulatory parameters to the fitted acute VO values and maintained them throughout growth.…”

Section: Calibrating the Multiscale Model: Vo Angii E2 P4mentioning

confidence: 92%

“…Notably, the Stretch input increased acutely and gradually decreased in our VO simulations while it remained relatively constant near baseline for AngII, E2, and P4. [19][20][21][22][23][24][25][26], Progesterone (P4) infusion [28], and Estrogen (E2) infusion [53,[64][65][66]. A.)…”

Section: Uncertainty Analysismentioning

confidence: 99%

“…An increase in aortic resistance due to constriction (pressure overload, PO) leads to mass increase and wall thickening, while an increase in cardiac output due to an arteriovenous fistula or valvular regurgitation (volume overload, VO) leads to mass increase and LV cavity dilation. Infusion of isoproterenol leads to LV mass increase [7][8][9][10][11][12][13][14][15][16][17][18], as does infusion with angiotensin [19][20][21][22][23][24][25][26]. Pregnancy hormones also influence heart growth.…”

Section: Introductionmentioning

confidence: 99%

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Multiscale model of heart growth during pregnancy: Integrating mechanical and hormonal signaling

Yoshida

Saucerman

Holmes

2020

Preprint

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Pregnancy stands at the interface of mechanics and biology. The growing fetus continuously loads the maternal organs as circulating hormone levels surge, leading to significant changes in mechanical and hormonal cues during pregnancy. In response to these cues, maternal soft tissues undergo remarkable growth and remodeling to support both mother and baby for a healthy pregnancy. We focus here on the maternal left ventricle, which increases its cardiac output and mass during pregnancy. The objective of this study is to build a multiscale cardiac growth model for pregnancy to understand how mechanical and hormonal cues interact to drive this growth process. Towards this objective, we coupled a cell signaling network model that predicts cell-level hypertrophy in response to hormones and stretch, to a compartmental model of the rat heart and circulation that predicts organ-level growth in response to hemodynamic changes. Since pregnancy is associated with a volume overloaded state and elevated hormones, we first calibrated the coupled, multiscale model to data from experimental volume overload (VO) and hormonal infusion of angiotensin 2 (AngII), estrogen (E2), and progesterone (P4). We then validated the ability of our model to capture interactions between inputs by comparing model predictions against published observations for the combinations of VO+E2 and AngII+E2. Finally, we simulated pregnancy-induced changes in hormones and hemodynamics to predict heart growth during pregnancy. Our multiscale model produced realistic heart growth consistent with experimental data. Overall, our analysis suggests that much of heart growth during pregnancy is driven by the early rise in P4, particularly during the first half of gestation. We conclude with suggestions for future experimental studies that will provide a better understanding of how hormonal and mechanical cues interact to drive pregnancy-induced heart growth.

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“…17 In similar contexts, HDAC6 has been proposed as a therapeutic target for treatment of cardiovascular diseases. [15][16][17][18][19] We also recently reported that tubastatin A, an HDAC6-specific inhibitor, could increase CSE acetylation and enhance its protein levels and H 2 S production, thereby helping to attenuate the vasoconstriction and hypertension induced by AngII. 20 Moreover, HDAC6, a member of the class IIb HDAC family, exhibits distinct characters compared to other HDAC family members in that it has unique specificity for protein deacetylation of non-histone substrates such as α-tubulin, cortactin and heat-shock protein 90.…”

Section: Introductionmentioning

confidence: 92%

Honokiol ameliorates angiotensin II‐induced hypertension and endothelial dysfunction by inhibiting HDAC6‐mediated cystathionine γ‐lyase degradation

Chi

Lee

et al. 2020

J Cellular Molecular Medi

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Hypertension and endothelial dysfunction are associated with various cardiovascular diseases. Hydrogen sulphide (H2S) produced by cystathionine γ‐lyase (CSE) promotes vascular relaxation and lowers hypertension. Honokiol (HNK), a natural compound in the Magnolia plant, has been shown to retain multifunctional properties such as anti‐oxidative and anti‐inflammatory activities. However, a potential role of HNK in regulating CSE and hypertension remains largely unknown. Here, we aimed to demonstrate that HNK co‐treatment attenuated the vasoconstriction, hypertension and H2S reduction caused by angiotensin II (AngII), a well‐established inducer of hypertension. We previously found that histone deacetylase 6 (HDAC6) mediates AngII‐induced deacetylation of CSE, which facilitates its ubiquitination and proteasomal degradation. Our current results indicated that HNK increased endothelial CSE protein levels by enhancing its stability in a sirtuin‐3‐independent manner. Notably, HNK could increase CSE acetylation levels by inhibiting HDAC6 catalytic activity, thereby blocking the AngII‐induced degradative ubiquitination of CSE. CSE acetylation and ubiquitination occurred mainly on the lysine 73 (K73) residue. Conversely, its mutant (K73R) was resistant to both acetylation and ubiquitination, exhibiting higher protein stability than that of wild‐type CSE. Collectively, our findings suggested that HNK treatment protects CSE against HDAC6‐mediated degradation and may constitute an alternative for preventing endothelial dysfunction and hypertensive disorders.

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Sodium butyrate attenuates angiotensin II‐induced cardiac hypertrophy by inhibiting COX2/PGE2 pathway via a HDAC5/HDAC6‐dependent mechanism

Cited by 67 publications

References 43 publications

ELABELA attenuates deoxycorticosterone acetate/salt-induced hypertension and renal injury by inhibition of NADPH oxidase/ROS/NLRP3 inflammasome pathway

ELABELA attenuates deoxycorticosterone acetate/salt-induced hypertension and renal injury by inhibition of NADPH oxidase/ROS/NLRP3 inflammasome pathway

Multiscale model of heart growth during pregnancy: Integrating mechanical and hormonal signaling

Honokiol ameliorates angiotensin II‐induced hypertension and endothelial dysfunction by inhibiting HDAC6‐mediated cystathionine γ‐lyase degradation

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