Rap1b GTPase Ameliorates Glucose-Induced Mitochondrial Dysfunction

Sun, Lin; Xie, Ping; Wada, Jun; Kashihara, Naoki; Liu, Fu You; Zhao, Yanan; Kumar, Deepak; Chugh, Sumant S.; Danesh, Farhad R.; Kanwar, Yashpal S.

doi:10.1681/asn.2008030336

Cited by 68 publications

(88 citation statements)

References 38 publications

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“…Assessment of Cellular Distribution of Cytochrome c-Confocal microscopy was employed to delineate the distribution of cytochrome c, as described previously (41). Cells were incubated with 25 nM Mitotracker dye (Mitotracker Red, Molecular Probes, Inc.) at 37°C for 10 min.…”

Section: Determination Of the Source Of Intracellular Ros Generation mentioning

confidence: 99%

myo-Inositol Oxygenase Overexpression Accentuates Generation of Reactive Oxygen Species and Exacerbates Cellular Injury following High Glucose Ambience

Sun

Dutta

Xie

et al. 2016

Journal of Biological Chemistry

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increased ROS generation, depleted reduced glutathione, reduced GSH/GSSG ratio, and enhanced adaptive changes in the profile of the antioxidant defense system. These changes were also accompanied by mitochondrial dysfunctions, DNA damage and induction of apoptosis, accentuated activity of profibrogenic cytokine, and expression of fibronectin, the latter two being the major hallmarks of DN. These perturbations were largely blocked by various ROS inhibitors (Mito Q, diphenyleneiodonium chloride, and N-acetylcysteine) and MIOX/NOX4 siRNA. In conclusion, this study highlights a novel mechanism where MIOX under HG ambience exacerbates renal injury during the progression of diabetic nephropathy following the generation of excessive ROS via an unexplored G-X pathway.

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Section: Determination Of the Source Of Intracellular Ros Generation mentioning

confidence: 99%

myo-Inositol Oxygenase Overexpression Accentuates Generation of Reactive Oxygen Species and Exacerbates Cellular Injury following High Glucose Ambience

Sun

Dutta

Xie

et al. 2016

Journal of Biological Chemistry

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“…The features of tubulointerstitial histopathology include inflammation and apoptosis, which are not necessarily secondary to glomerular lesions. 7,[24][25][26] In addition, tubular injury alone is believed to be closely correlate with clinical manifestations of DKD, including the extent albumin excretion and its degradation in tubules. The latter may serve as a primary key site for the development of DKD, because tubular injury has been described to be a better predictor in the progression of the renal disease.…”

Section: Discussionmentioning

confidence: 99%

“…5,6 Although the pathogenesis of DKD still remains unclear, recent studies in animals and humans have led to an emerging concept that mitochondrial dysfunctions, which are pivotal events, lead to activation of various cellular processes and aberrant signaling in different cell types of the kidney. [7][8][9] Mitochondria are dynamic organelles that constantly undergo fusion and fission cycles to maintain a balance of cellular reticular network and mitochondrial turnover. 10 Their dynamics are regulated by profission proteins (Drp1 and Fis1) and profusion mediators (Mfn1/2 and OPA1).…”

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confidence: 99%

Disruption of Renal Tubular Mitochondrial Quality Control by Myo-Inositol Oxygenase in Diabetic Kidney Disease

Zhan

Usman

Sun

et al. 2015

Journal of the American Society of Nephrology

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241

251

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Diabetic kidney disease (DKD) is associated with oxidative stress and mitochondrial injury. Myo-inositol oxygenase (MIOX), a tubular-specific enzyme, modulates redox imbalance and apoptosis in tubular cells in diabetes, but these mechanisms remain unclear. We investigated the role of MIOX in perturbation of mitochondrial quality control, including mitochondrial dynamics and autophagy/mitophagy, under highglucose (HG) ambience or a diabetic state. HK-2 or LLC-PK1 cells subjected to HG exhibited an upregulation of MIOX accompanied by mitochondrial fragmentation and depolarization, inhibition of autophagy/ mitophagy, and altered expression of mitochondrial dynamic and mitophagic proteins. Furthermore, dysfunctional mitochondria accumulated in the cytoplasm, which coincided with increased reactive oxygen species generation, Bax activation, cytochrome C release, and apoptosis. Overexpression of MIOX in LLC-PK1 cells enhanced the effects of HG, whereas MIOX siRNA or D-glucarate, an inhibitor of MIOX, partially reversed these perturbations. Moreover, decreasing the expression of MIOX under HG ambience increased PTEN-induced putative kinase 1 expression and the dependent mitofusin-2-Parkin interaction. In tubules of diabetic mice, increased MIOX expression and mitochondrial fragmentation and defective autophagy were observed. Dietary supplementation of D-glucarate in diabetic mice decreased MIOX expression, attenuated tubular damage, and improved renal functions. Notably, D-glucarate administration also partially attenuated mitochondrial fragmentation, oxidative stress, and apoptosis and restored autophagy/mitophagy in the tubular cells of these mice. These results suggest a novel mechanism linking MIOX to impaired mitochondrial quality control during tubular injury in the pathogenesis of DKD and suggest D-glucarate as a potential therapeutic agent for the amelioration of DKD.

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“…29 In addition, diabetic mouse models and in vitro studies have demonstrated that hyperglycemia induced mitochondrial fragmentation in podocytes, endothelial cells, and renal tubular cells. 7,30 Finally, WBCs are involved in the kidney's response to injury as evidenced by leukocyte infiltration in kidney tissues of patients with CKD and in experimental models. [31][32][33] Lower mtDNA copy number might alter the role of WBCs and platelets in injury response.…”

Section: Main Findingsmentioning

confidence: 99%

“…[3][4][5] Molecules that target mitochondrial function, including thiazolidinediones, have been proposed as therapeutic agents for protecting kidney function. [6][7][8][9] However, studies on measures of mitochondrial dysfunction and CKD at the population level have been limited.…”

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confidence: 99%

Association between Mitochondrial DNA Copy Number in Peripheral Blood and Incident CKD in the Atherosclerosis Risk in Communities Study

Tin

Grams²,

Ashar

et al. 2016

JASN

118

115

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Mitochondrial dysfunction in kidney cells has been implicated in the pathogenesis of CKD. Mitochondrial DNA (mtDNA) copy number is a surrogate measure of mitochondrial function, and higher mtDNA copy number in peripheral blood has been associated with lower risk of two important risk factors for CKD progression, diabetes and microalbuminuria. We evaluated whether mtDNA copy number in peripheral blood associates with incident CKD in a population-based cohort of middle-aged adults. We estimated mtDNA copy number using 25 high-quality mitochondrial single nucleotide polymorphisms from the Affymetrix 6.0 array. Among 9058 participants, those with higher mtDNA copy number had a lower rate of prevalent diabetes and lower C-reactive protein levels and white blood cell counts. Baseline eGFR did not differ significantly by mtDNA copy number. Over a median follow-up of 19.6 years, 1490 participants developed CKD. Higher mtDNA copy number associated with lower risk of incident CKD (highest versus lowest quartile: hazard ratio 0.65; 95% confidence interval, 0.56 to 0.75; P,0.001) after adjusting for age, sex, and race. After adjusting for additional risk factors of CKD, including prevalent diabetes, hypertension, C-reactive protein level, and white blood cell count, this association remained significant (highest versus lowest quartile: hazard ratio 0.75; 95% confidence interval, 0.64 to 0.87; P,0.001). In conclusion, higher mtDNA copy number associated with lower incidence of CKD independent of traditional risk factors and inflammation biomarker levels in this cohort. Further research on modifiable factors influencing mtDNA copy number may lead to improvement in the prevention and treatment of CKD.

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Rap1b GTPase Ameliorates Glucose-Induced Mitochondrial Dysfunction

Cited by 68 publications

References 38 publications

myo-Inositol Oxygenase Overexpression Accentuates Generation of Reactive Oxygen Species and Exacerbates Cellular Injury following High Glucose Ambience

myo-Inositol Oxygenase Overexpression Accentuates Generation of Reactive Oxygen Species and Exacerbates Cellular Injury following High Glucose Ambience

Disruption of Renal Tubular Mitochondrial Quality Control by Myo-Inositol Oxygenase in Diabetic Kidney Disease

Association between Mitochondrial DNA Copy Number in Peripheral Blood and Incident CKD in the Atherosclerosis Risk in Communities Study

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