Polysulfide-mediated sulfhydration of SIRT1 prevents diabetic nephropathy by suppressing phosphorylation and acetylation of p65 NF-κB and STAT3

Sun, Hai-Jian; Xiong, Shaojun; Cao, Xu; Cao, Lei; Zhu, Mengyuan; Wu, Zhiyuan; Bian, Jun

doi:10.1016/j.redox.2020.101813

Cited by 110 publications

(50 citation statements)

References 99 publications

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“…Also, the role of SS31 has been associated with CD36 ( 58 ). Besides, Na2S4, a polysulfide donor that directly sulfhydrates SIRT1, reduces high glucose-induced oxidative stress, cell apoptosis, inflammatory response in renal tubular epithelial cells, and the progression of epithelial-to-mesenchymal transition (EMT) ( 59 ). Also, Carnosine has been shown to significantly decrease the production of ROS, alleviate oxidative stress, and inhibit apoptosis through mitochondrial pathway in vitro ( 60 ) and in vivo ( 61 ).…”

Section: Mitochondrial Dysfunctionmentioning

confidence: 99%

Update on the Mechanisms of Tubular Cell Injury in Diabetic Kidney Disease

Chang

Yan

et al. 2021

Front. Med.

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Increasing evidence supports a role of proximal tubular (PT) injury in the progression of diabetic kidney disease (DKD), in patients with or without proteinuria. Research on the mechanisms of the PT injury in DKD could help us to identify potential new biomarkers and drug targets for DKD. A high glucose transport state and mismatched local hypoxia in the PT of diabetes patients may be the initiating factors causing PT injury. Other mechanism such as mitochondrial dysfunction, reactive oxygen species (ROS) overproduction, ER stress, and deficiency of autophagy interact with each other leading to more PT injury by forming a vicious circle. PT injury eventually leads to the development of tubulointerstitial inflammation and fibrosis in DKD. Many downstream signaling pathways have been demonstrated to mediate these diseased processes. This review focuses mostly on the novel mechanisms of proximal renal tubular injury in DKD and we believe such review could help us to better understand the pathogenesis of DKD and identify potential new therapies for this disease.

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Section: Mitochondrial Dysfunctionmentioning

confidence: 99%

Update on the Mechanisms of Tubular Cell Injury in Diabetic Kidney Disease

Chang

Yan

et al. 2021

Front. Med.

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“…The pathological processes that drive podocyte dysfunction involve sirtuin 1 (SIRT1), a deacetylase that regulates cell inflammation, apoptosis, proliferation, autophagy, energy metabolism, and oxidative stress [ 13 ]. SIRT1 appears to exert a renoprotective effect in kidney diseases, including DN [ 14 – 16 ]. 3,5-Diiodothyronine can inhibit mesangial cell proliferation and decrease proteinuria by activating SIRT1 in rat mesangial cells [ 17 ].…”

Section: Introductionmentioning

confidence: 99%

Inhibition of miRNA-155 Alleviates High Glucose-Induced Podocyte Inflammation by Targeting SIRT1 in Diabetic Mice

Wang

Gao

et al. 2021

Journal of Diabetes Research

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Objective. Microinflammation plays a crucial role in podocyte dysfunction in diabetic nephropathy, but its regulatory mechanism is still unclear. This study is aimed at discussing the mechanisms underlying the effect of miRNA-155 on podocyte injury to determine its potential as a therapeutic target. Methods. Cultured immortalized mouse podocytes and diabetic KK-Ay mice models were treated with a miR-155 inhibitor. Western blotting, real-time PCR, ELISA, immunofluorescence, and Luciferase reporter assay were used to analyze markers of inflammation cytokines and podocyte injury. Results. miRNA-155 was found to be highly expressed in serum and kidney tissue of mice with diabetic nephropathy and in cultured podocytes, accompanied by elevated levels of inflammatory factors. Inhibition of miRNA-155 can reduce proteinuria and ACR levels, diminish the secretion of inflammatory molecules, improve kidney function, inhibit podocyte foot fusion, and reverse renal pathological changes in diabetic nephropathy mice. Overexpression of miRNA-155 in vitro can increase inflammatory molecule production in podocytes and aggravates podocyte injury, while miRNA-155 inhibition suppresses inflammatory molecule production in podocytes and reduces podocyte injury. A luciferase assay confirmed that miRNA-155 could selectively bind to 3 ′ -UTR of SIRT1, resulting in decreased SIRT1 expression. In addition, SIRT1 siRNA could offset SIRT1 upregulation and enhance inflammatory factor secretion in podocytes, induced by the miRNA-155 inhibitor. Conclusions. These findings strongly support the hypothesis that miRNA-155 inhibits podocyte inflammation and reduces podocyte injury through SIRT1 silencing. miRNA-155 suppression therapy may be useful for the management of diabetic nephropathy.

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“…H 2 S regulates diverse cellular signaling pathways through persulfidation (S-sulfhydration) [ 3 , 32 , 33 , 34 , 35 , 36 , 37 , 38 , 39 , 40 , 41 , 42 , 43 , 44 , 45 ]. This novel and reversible posttranslational modification covalently adds a thiol group (-SH) to active cysteine residue (PSH/PS - ) in its target protein, which forms protein persulfidation (PSSH/PSS - ) ( Figure 1 A) [ 46 ].…”

Section: Hydrogen Sulfide Mediated Protein Persulfidationmentioning

confidence: 99%

The Hidden Role of Hydrogen Sulfide Metabolism in Cancer

Wang

Chu

Lin

2021

IJMS

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Hydrogen Sulfide (H2S), an endogenously produced gasotransmitter, is involved in various important physiological and disease conditions, including vasodilation, stimulation of cellular bioenergetics, anti-inflammation, and pro-angiogenesis. In cancer, aberrant up-regulation of H2S-producing enzymes is frequently observed in different cancer types. The recognition that tumor-derived H2S plays various roles during cancer development reveals opportunities to target H2S-mediated signaling pathways in cancer therapy. In this review, we will focus on the mechanism of H2S-mediated protein persulfidation and the detailed information about the dysregulation of H2S-producing enzymes and metabolism in different cancer types. We will also provide an update on mechanisms of H2S-mediated cancer progression and summarize current options to modulate H2S production for cancer therapy.

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Polysulfide-mediated sulfhydration of SIRT1 prevents diabetic nephropathy by suppressing phosphorylation and acetylation of p65 NF-κB and STAT3

Cited by 110 publications

References 99 publications

Update on the Mechanisms of Tubular Cell Injury in Diabetic Kidney Disease

Update on the Mechanisms of Tubular Cell Injury in Diabetic Kidney Disease

Inhibition of miRNA-155 Alleviates High Glucose-Induced Podocyte Inflammation by Targeting SIRT1 in Diabetic Mice

The Hidden Role of Hydrogen Sulfide Metabolism in Cancer

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