BAY61‐3606 protects kidney from acute ischemia/reperfusion injury through inhibiting spleen tyrosine kinase and suppressing inflammatory macrophage response

Tan, Ruizhi; Li, Jianchun; Liu, Jian; Xin, Lei; Zhong, Xia; Wang, Chen; Yan, Yan; Ye, Lingyu Linda; Duan, Dayue Darrel; Lan, Hui‐Yao; Wang, Li

doi:10.1096/fj.202000261rrr

Cited by 14 publications

(16 citation statements)

References 72 publications

(124 reference statements)

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“…A recent study demonstrated that Mincle is essential for maintaining the M1 phenotype of macrophage in kidney of AKI, and down‐regulation of Mincle in macrophage relieved the renal injury, suggesting that Mincle is a key promotor for macrophagic inflammation in AKI 20 . Our previous research also proved that inhibition of Mincle‐related signal pathway protects kidney from AKI injury 21 . Therefore, drug intervention targeting Mincle may be the key to the treatment of AKI.…”

Section: Introductionmentioning

confidence: 81%

“…Bone marrow–derived macrophages (BMDM) were isolated from the tibia and femur of C57BL/6 mice and differentiated in low‐glucose DMEM medium containing 30% supernatant of L929 cell for 7 days following the protocol in our previous study. 21 To obtain the primary tubular epithelial cells (mTEC) from mouse, the kidney was digested with 3 mg/ml Collagen 4 at 37℃ for 15min, then filtered the suspension on a 70‐μm cell strainer and centrifuged at 120 g for 5 min, followed by culturing the tubular epithelial cells in F12/DMEM medium with 5% foetal bovine serum containing 50 ng/ml epidermal growth factor and 5 μl/ml ITS‐G for 5 days. All cells were incubated in a 37℃ incubator containing a constant 5% CO 2 .…”

Section: Methodsmentioning

confidence: 99%

“… 20 Our previous research also proved that inhibition of Mincle‐related signal pathway protects kidney from AKI injury. 21 Therefore, drug intervention targeting Mincle may be the key to the treatment of AKI.…”

Section: Introductionmentioning

confidence: 99%

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Artesunate relieves acute kidney injury through inhibiting macrophagic Mincle‐mediated necroptosis and inflammation to tubular epithelial cell

Xin

Tan

Jia

et al. 2021

J Cellular Molecular Medi

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Artesunate is a widely used derivative of artemisinin for malaria. Recent researches have shown that artesunate has a significant anti‐inflammatory effect on many diseases. However, its effect on acute kidney injury with a significant inflammatory response is not clear. In this study, we established a cisplatin‐induced AKI mouse model and a co‐culture system of BMDM and tubular epithelial cells (mTEC) to verify the renoprotective and anti‐inflammatory effects of artesunate on AKI, and explored the underlying mechanism. We found that artesunate strongly down‐regulated the serum creatinine and BUN levels in AKI mice, reduced the necroptosis of tubular cells and down‐regulated the expression of the tubular injury molecule Tim‐1. On the other hand, artesunate strongly inhibited the mRNA expression of inflammatory cytokines (IL‐1β, IL‐6 and TNF‐α), protein levels of inflammatory signals (iNOS and NF‐κB) and necroptosis signals (RIPK1, RIPK3 and MLKL) in kidney of AKI mouse. Notably, the co‐culture system proved that Mincle in macrophage can aggravate the inflammation and necroptosis of mTEC induced by LPS, and artesunate suppressed the expression of Mincle in macrophage of kidney in AKI mouse. Overexpression of Mincle in BMDM restored the damage and necroptosis inhibited by artesunate in mTEC, indicating Mincle in macrophage is the target of artesunate to protect tubule cells in AKI. Our findings demonstrated that artesunate can significantly improve renal function in AKI, which may be related to the inhibition of Mincle‐mediated macrophage inflammation, thereby reducing the damage and necroptosis to tubular cells that provide new option for the treatment of AKI.

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Section: Introductionmentioning

confidence: 81%

Section: Methodsmentioning

confidence: 99%

See 1 more Smart Citation

Artesunate relieves acute kidney injury through inhibiting macrophagic Mincle‐mediated necroptosis and inflammation to tubular epithelial cell

Xin

Tan

Jia

et al. 2021

J Cellular Molecular Medi

Self Cite

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“…The incision was then sutured and the mice were placed on a 36-37°C heat pad. Mice in the TBI + BAY and BAY groups were administered with BAY (3 mg/kg) intraperitoneally ( 30 ) for 7 days after TBI insult. Mice in the BAY group did not receive CCI insult.…”

Section: Methodsmentioning

confidence: 99%

BAY61‑3606 attenuates neuroinflammation and neurofunctional damage by inhibiting microglial Mincle/Syk signaling response after traumatic brain injury

Huang

Liu

et al. 2021

Int J Mol Med

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“…In kidney injury, oxidative stress and inflammation are the most significant characteristics, as well as pivotal pathological factors 4 . In response to injury, inflammation initially emerges as a reno-protective role.…”

Section: Introductionmentioning

confidence: 99%

Alternative polyadenylation trans-factor FIP1 exacerbates UUO/IRI-induced kidney injury and contributes to AKI-CKD transition via ROS-NLRP3 axis

et al. 2021

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NLRP3, a decisive role in inflammation regulation, is obviously upregulated by oxidative stress in kidney injury. The NLRP3 upregulation leads to unsolved inflammation and other pathological effects, contributing to aggravation of kidney injury and even transition to chronic kidney disease (CKD). However, the mechanism for NLRP3 upregulation and further aggravation of kidney injury remains largely elusive. In this study, we found NLRP3 3′UTR was shortened in response to kidney injury in vivo and oxidative stress in vitro. Functionally, such NLRP3 3′UTR shortening upregulated NLRP3 expression and amplified inflammation, fibrogenesis, ROS production and apoptosis, depending on stabilizing NLRP3 mRNA. Mechanistically, FIP1 was found to bind to pPAS of NLRP3 mRNA via its arginine-rich domain and to induce NLRP3 3′UTR shortening. In addition, FIP1 was upregulated in CKD specimens and negatively associated with renal function of CKD patients. More importantly, we found FIP1 was upregulated by oxidative stress and required for oxidative stress-induced NLRP3 upregulation, inflammation activation, cell damage and apoptosis. Finally, we proved that FIP1 silencing attenuated the inflammation activation, fibrogenesis, ROS production and apoptosis induced by UUO or IRI. Taken together, our results demonstrated that oxidative stress-upregulated FIP1 amplified inflammation, fibrogenesis, ROS production and apoptosis via inducing 3′UTR shortening of NLRP3, highlighting the importance of crosstalk between oxidative stress and alternative polyadenylation in AKI-CKD transition, as well as the therapeutic potential of FIP1 in kidney injury treatment.

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BAY61‐3606 protects kidney from acute ischemia/reperfusion injury through inhibiting spleen tyrosine kinase and suppressing inflammatory macrophage response

Cited by 14 publications

References 72 publications

Artesunate relieves acute kidney injury through inhibiting macrophagic Mincle‐mediated necroptosis and inflammation to tubular epithelial cell

Artesunate relieves acute kidney injury through inhibiting macrophagic Mincle‐mediated necroptosis and inflammation to tubular epithelial cell

BAY61‑3606 attenuates neuroinflammation and neurofunctional damage by inhibiting microglial Mincle/Syk signaling response after traumatic brain injury

Alternative polyadenylation trans-factor FIP1 exacerbates UUO/IRI-induced kidney injury and contributes to AKI-CKD transition via ROS-NLRP3 axis

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