GADD45B mediates podocyte injury in zebrafish by activating the ROS-GADD45B-p38 pathway

Chen, Z; Wan, Xiaoyang; Hou, Qi; Shi, Shaolin; Wang, L; Chen, P; Zhu, Xiaodong; Zeng, Caihong; Qin, Weisong; Zhou, Weibin; Liu, Fei

doi:10.1038/cddis.2015.300

Cited by 38 publications

(36 citation statements)

References 39 publications

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“…Our study demonstrated that integrin α6β4, another integrin family heterodimer, also activated FAK and induced actin filament rearrangements. Consistent with the results of our investigation, the results of studies involving other cell lines have shown that activated integrin α6β4 can recruit FAK, thereby inducing autophosphorylation at Y397, a critical tyrosine site that plays a role in the activation of downstream effectors, such as p38.P38 has been demonstrated to mediate podocyte injury in various models of renal disease; moreover, p38 inhibition has been shown to protect podocytes from injury in vitro and ameliorate proteinuria in vivo . A recent study showed that the FAK/p38 axis contributed to foot process effacement and proteinuria development in a rat model of short‐term hypercholesterolaemia by modulating podocyte apoptosis and F‐actin reorganization .…”

Section: Discussionsupporting

confidence: 90%

“…Consistent with the results of our investigation, the results of studies involving other cell lines have shown that activated integrin α6β4 can recruit FAK, thereby inducing autophosphorylation at Y397, 21 a critical tyrosine site that plays a role in the activation of downstream effectors, such as p38.P38 has been demonstrated to mediate podocyte injury in various models of renal disease; moreover, p38 inhibition has been shown to protect podocytes from injury in vitro and ameliorate proteinuria in vivo. 29,53 A recent study showed that the FAK/p38 axis contributed to foot process effacement and proteinuria development in a rat model of short-term hypercholesterolaemia by modulating podocyte apoptosis and F-actin reorganization. 4 Consistent with this finding, the results of our study demonstrated that the FAK/p38 axis plays an important role in ADR-induced podocyte injury and showed that plectin and integrin α6ß4 are the upstream inducers of this axis.…”

Section: Moreover the Expression Levels Of The Podocyte Apoptosis Mamentioning

confidence: 99%

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Plectin protects podocytes from adriamycin‐induced apoptosis and F‐actin cytoskeletal disruption through the integrin α6β4/FAK/p38 MAPK pathway

Wang

Yin³

et al. 2018

J Cellular Molecular Medi

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Podocyte injury is an early pathological change characteristic of various glomerular diseases, and apoptosis and F‐actin cytoskeletal disruption are typical features of podocyte injury. In this study, we found that adriamycin (ADR) treatment resulted in typical podocyte injury and repressed plectin expression. Restoring plectin expression protected against ADR‐induced podocyte injury whereas siRNA‐mediated plectin silencing produced similar effects as ADR‐induced podocyte injury, suggesting that plectin plays a key role in preventing podocyte injury. Further analysis showed that plectin repression induced significant integrin α6β4, focal adhesion kinase (FAK) and p38 MAPK phosphorylation. Mutating Y1494, a key tyrosine residue in the integrin β4 subunit, blocked FAK and p38 phosphorylation, thereby alleviating podocyte injury. Inhibitor studies demonstrated that FAK Y397 phosphorylation promoted p38 activation, resulting in podocyte apoptosis and F‐actin cytoskeletal disruption. In vivo studies showed that administration of ADR to rats resulted in significantly increased 24‐hour urine protein levels along with decreased plectin expression and activated integrin α6β4, FAK, and p38. Taken together, these findings indicated that plectin protects podocytes from ADR‐induced apoptosis and F‐actin cytoskeletal disruption by inhibiting integrin α6β4/FAK/p38 pathway activation and that plectin may be a therapeutic target for podocyte injury‐related glomerular diseases.

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Section: Discussionsupporting

confidence: 90%

Section: Moreover the Expression Levels Of The Podocyte Apoptosis Mamentioning

confidence: 99%

Plectin protects podocytes from adriamycin‐induced apoptosis and F‐actin cytoskeletal disruption through the integrin α6β4/FAK/p38 MAPK pathway

Wang

Yin³

et al. 2018

J Cellular Molecular Medi

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“…If GADD45B inhibits autophagy, it logically promotes apoptosis so that tumor cell growth is inhibited, especially in the system of cultured cells. Previous studies have also shown that GADD45B is a potent tumor suppressor . However, autophagy defects enhances pyroptosis and promotes death of tumor cells as well as host cells surrounding tumor cells so that the survivals of animals will be reduced .…”

Section: Discussionmentioning

confidence: 99%

Matrine inhibits the progression of prostate cancer by promoting expression of GADD45B

Huang

Wang

et al. 2018

The Prostate

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“…15, 16, 37 In addition, the p38 MAPK pathway was shown to have an important role in podocyte injury. 38, 39 The data obtained in this study showed that the expression of p-p38 is significantly enhanced in the DN glomeruli and HG-induced MPC5 cells, and it is accompanied by the increase in the expression of Bax and cleaved caspase 3. The inhibition of Mtdh led to the suppression of the activation of p38 MAPK pathway following the HG treatment, which suggests a possible link between Mtdh and p38 MAPK activation.…”

Section: Discussionmentioning

confidence: 57%

Metadherin facilitates podocyte apoptosis in diabetic nephropathy

Liu

Peng

et al. 2016

Cell Death Dis

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Apoptosis, one of the major causes of podocyte loss, has been reported to have a vital role in diabetic nephropathy (DN) pathogenesis, and understanding the mechanisms underlying the regulation of podocyte apoptosis is crucial. Metadherin (MTDH) is an important oncogene, which is overexpressed in most cancers and responsible for apoptosis, metastasis, and poor patient survival. Here we show that the expression levels of Mtdh and phosphorylated p38 mitogen-activated protein kinase (MAPK) are significantly increased, whereas those of the microRNA-30 family members (miR-30s) are considerably reduced in the glomeruli of DN rat model and in high glucose (HG)-induced conditionally immortalized mouse podocytes (MPC5). These levels are positively correlated with podocyte apoptosis rate. The inhibition of Mtdh expression, using small interfering RNA, but not Mtdh overexpression, was shown to inhibit HG-induced MPC5 apoptosis and p38 MAPK pathway, and Bax and cleaved caspase 3 expression. This was shown to be similar to the effects of p38 MAPK inhibitor (SB203580). Furthermore, luciferase assay results demonstrated that Mtdh represents the target of miR-30s. Transient transfection experiments, using miR-30 microRNA (miRNA) inhibitors, led to the increase in Mtdh expression and induced the apoptosis of MPC5, whereas the treatment with miR-30 miRNA mimics led to the reduction in Mtdh expression and apoptosis of HG-induced MPC5 cells in comparison with their respective controls. Our results demonstrate that Mtdh is a potent modulator of podocyte apoptosis, and that it represents the target of miR-30 miRNAs, facilitating podocyte apoptosis through the activation of HG-induced p38 MAPK-dependent pathway.

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GADD45B mediates podocyte injury in zebrafish by activating the ROS-GADD45B-p38 pathway

Cited by 38 publications

References 39 publications

Plectin protects podocytes from adriamycin‐induced apoptosis and F‐actin cytoskeletal disruption through the integrin α6β4/FAK/p38 MAPK pathway

Plectin protects podocytes from adriamycin‐induced apoptosis and F‐actin cytoskeletal disruption through the integrin α6β4/FAK/p38 MAPK pathway

Matrine inhibits the progression of prostate cancer by promoting expression of GADD45B

Metadherin facilitates podocyte apoptosis in diabetic nephropathy

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