Tetramethylpyrazine Prevents Contrast-Induced Nephropathy via Modulating Tubular Cell Mitophagy and Suppressing Mitochondrial Fragmentation, CCL2/CCR2-Mediated Inflammation, and Intestinal Injury

Gong, Xuezhong; Duan, Yue; Zheng, Junli; Ye, Zi; Hei, Tom K.

doi:10.1155/2019/7096912

Cited by 35 publications

(32 citation statements)

References 42 publications

(72 reference statements)

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“…In rats, TMP prevents CIN kidney injury in vivo by reversing the associated pathological processes. Mechanistically, TMP efficiently reversed the CM-induced activation of the CCL2/CCR2 pathway, ameliorated renal oxidative stress and aberrant mitochondrial dynamics by restoring the alterations in Drp1 and Mfn2 expression, modulated mitophagy in tubular cells, and suppressed the expression of autophagy genes, including those encoding LC3B, Beclin-1, and p62 protein (Gong et al, 2019). In a cisplatin (a chemotherapeutic drug)-induced model of AKI, treatment of proximal tubule-specific autophagy-deficient mice with cisplatin led to severe mitochondrial damage and promoted ROS production, DNA damage, and p53 activation.…”

Section: Nephrotoxic Akimentioning

confidence: 96%

“…Thus far, studies on the role of autophagy in kidney proximal tubules have often yielded contradictory or unconvincing results (Periyasamy-Thandavan et al, 2008;Inoue et al, 2010;Kimura et al, 2011;Jiang et al, 2012;Liu et al, 2012;Livingston and Dong, 2014;Takabatake et al, 2014;Choi, 2019). We speculate that the reasons for such conflicting data include (1) the use of different autophagy agonists and inhibitors, which are not entirely specific and may have some unknown targets (Kimura et al, 2011;Livingston and Dong, 2014), and when administered at different doses, these autophagy agonists and inhibitors may exhibit different thresholds for autophagy intervention; (2) the differences in the function and degree of damage in different proximal tubule segments (for example, in the AKI mouse model, IRI epithelial cell damage is most apparent in the S3 segment of the proximal tubule, while mitochondrial density is the highest in the S1 segment, and the oxidative burst primarily occurs in the S2 segment; Bao et al, 2017;Gong et al, 2019; therefore, the role of autophagy genes in different proximal tubule segments may differ; one study reported that Atg5 deletion in the whole proximal tubule exacerbates kidney injury in AKI; Takahashi et al, 2012); and (3) the differences in the sex and strains of the experimental animals. Therefore, it is better to choose the same strain for breeding conditional knockout mice (such as the breeding of Cre/loxp recombinases or the insertion of fluorescent reporter in transgenic mice).…”

Section: Nephrotoxic Akimentioning

confidence: 99%

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Autophagy and Inflammation Regulation in Acute Kidney Injury

2020

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Autophagy at an appropriate juncture in the cell cycle exerts protective effects in acute kidney injury (AKI), whereas abnormal autophagy may lead to cell death. Inflammatory response plays a pivotal role in the pathophysiological process of kidney injury and repair during AKI. Several studies have reported an interaction between autophagy and inflammation in the pathogenesis of AKI. This review outlines recent advances in the investigation of the role of autophagy in inflammatory response regulation based on the following aspects. (1) Autophagy inhibits inflammatory responses induced in AKI through the regulation of mTOR and AMPK pathways and the inhibition of inflammasomes activation. (2) Autophagy can also help in the regulation of inflammatory responses through the nuclear factor kappa B pathway, which is beneficial to the recovery of kidney tissues. These studies reviewed here provide better insight into the mechanisms underlying the protective effects of the autophagy-inflammatory pathway. Through this review, we suggest that the autophagy-inflammatory pathway may serve as an alternative target for the treatment of AKI.

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Section: Nephrotoxic Akimentioning

confidence: 96%

Section: Nephrotoxic Akimentioning

confidence: 99%

Autophagy and Inflammation Regulation in Acute Kidney Injury

2020

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“…Similar to cisplatin, TUNEL-positivity was observed in tubular epithelium in 3–7 days after administration of these drugs [ 66 , 78 ]. Other toxic AKIs induced by heavy metal (i.e., mercury) exposure [ 47 , 60 ], nanomaterial consumption [ 79 , 80 ], or associated with rhabdomyolysis [ 81 ] or contrast-induced nephropathy [ 54 , 82 , 83 ] resulted in TUNEL-positivity in tubular epithelium within hours and up to the first week after exposure. Sepsis-induced AKI is multifactorial and includes microcirculatory dysfunction and renal inflammation.…”

Section: Tunel Applicationsmentioning

confidence: 99%

“…Methods of TUNEL quantification vary. In the majority of reports, TUNEL-positive cells/nuclei are quantified as the percent of total cells/nuclei [ 83 , 116 , 117 ]. This seems the right thing to do, although the number of TUNEL-positive cells likely do not correspond exactly to the number of dead cells.…”

Section: Tunel Quantification and Colocalization Techniquesmentioning

confidence: 99%

TUNEL Assay: A Powerful Tool for Kidney Injury Evaluation

Moore

Savenka

Basnakian

2021

IJMS

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Terminal deoxynucleotidyl transferase dUTP nick-end labeling (TUNEL) assay is a long-established assay used to detect cell death-associated DNA fragmentation (3’-OH DNA termini) by endonucleases. Because these enzymes are particularly active in the kidney, TUNEL is widely used to identify and quantify DNA fragmentation and cell death in cultured kidney cells and animal and human kidneys resulting from toxic or hypoxic injury. The early characterization of TUNEL as an apoptotic assay has led to numerous misinterpretations of the mechanisms of kidney cell injury. Nevertheless, TUNEL is becoming increasingly popular for kidney injury assessment because it can be used universally in cultured and tissue cells and for all mechanisms of cell death. Furthermore, it is sensitive, accurate, quantitative, easily linked to particular cells or tissue compartments, and can be combined with immunohistochemistry to allow reliable identification of cell types or likely mechanisms of cell death. Traditionally, TUNEL analysis has been limited to the presence or absence of a TUNEL signal. However, additional information on the mechanism of cell death can be obtained from the analysis of TUNEL patterns.

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“…The latest work by Gong et al verified the activation of mitophagy in CI-induced AKI in rats. The natural anti-oxidant tetramethylpyrazine suppressed ROS production, mitophagy, mitochondrial fragmentation, and renal tubular cell apoptosis in CI-induced AKI [126]. In addition, Mitophagy was also noticed in renal tubules in FA-induced AKI in rats [127], and in diatrizoic acid (DA)-induced renal tubular cell injury [128], but the precise role and regulation of mitophagy in these settings remain unknown.…”

Section: Mitophagy In Other Types Of Akimentioning

confidence: 99%

Mitophagy in Acute Kidney Injury and Kidney Repair

Wang

Cai

Tang

et al. 2020

Cells

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Acute kidney injury (AKI) is a major kidney disease characterized by rapid decline of renal function. Besides its acute consequence of high mortality, AKI has recently been recognized as an independent risk factor for chronic kidney disease (CKD). Maladaptive or incomplete repair of renal tubules after severe or episodic AKI leads to renal fibrosis and, eventually, CKD. Recent studies highlight a key role of mitochondrial pathology in AKI development and abnormal kidney repair after AKI. As such, timely elimination of damaged mitochondria in renal tubular cells represents an important quality control mechanism for cell homeostasis and survival during kidney injury and repair. Mitophagy is a selective form of autophagy that selectively removes redundant or damaged mitochondria. Here, we summarize our recent understanding on the molecular mechanisms of mitophagy, discuss the role of mitophagy in AKI development and kidney repair after AKI, and present future research directions and therapeutic potential.

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Tetramethylpyrazine Prevents Contrast-Induced Nephropathy via Modulating Tubular Cell Mitophagy and Suppressing Mitochondrial Fragmentation, CCL2/CCR2-Mediated Inflammation, and Intestinal Injury

Cited by 35 publications

References 42 publications

Autophagy and Inflammation Regulation in Acute Kidney Injury

Autophagy and Inflammation Regulation in Acute Kidney Injury

TUNEL Assay: A Powerful Tool for Kidney Injury Evaluation

Mitophagy in Acute Kidney Injury and Kidney Repair

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