Deletion of VDAC1 Hinders Recovery of Mitochondrial and Renal Functions After Acute Kidney Injury

Nowak, Grażyna; Megyesi, Judit; Craigen, William J.

doi:10.3390/biom10040585

Cited by 17 publications

(15 citation statements)

References 47 publications

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“…Mitochondria lacking VDAC ( VDAC1 −/−) are characterized by increased size, irregular and compacted cristae, and altered oxygen consumption either in oxidative either in glycolytic muscle fibers [ 11 ]. Other alterations have been detected in specific tissue injuries or pathologies, such as Alzheimer’s disease [ 15 , 16 ]. Impaired oxidative phosphorylation was detected in muscle biopsies of child patients affected by encephalomyopathy.…”

Section: Introductionmentioning

confidence: 99%

Is the Secret of VDAC Isoforms in Their Gene Regulation? Characterization of Human VDAC Genes Expression Profile, Promoter Activity, and Transcriptional Regulators

Zinghirino

Pappalardo

Messina

et al. 2020

IJMS

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VDACs (voltage-dependent anion-selective channels) are pore-forming proteins of the outer mitochondrial membrane, whose permeability is primarily due to VDACs’ presence. In higher eukaryotes, three isoforms are raised during the evolution: they have the same exon–intron organization, and the proteins show the same channel-forming activity. We provide a comprehensive analysis of the three human VDAC genes (VDAC1–3), their expression profiles, promoter activity, and potential transcriptional regulators. VDAC isoforms are broadly but also specifically expressed in various human tissues at different levels, with a predominance of VDAC1 and VDAC2 over VDAC3. However, an RNA-seq cap analysis gene expression (CAGE) approach revealed a higher level of transcription activation of VDAC3 gene. We experimentally confirmed this information by reporter assay of VDACs promoter activity. Transcription factor binding sites (TFBSs) distribution in the promoters were investigated. The main regulators common to the three VDAC genes were identified as E2F-myc activator/cell cycle (E2FF), Nuclear respiratory factor 1 (NRF1), Krueppel-like transcription factors (KLFS), E-box binding factors (EBOX) transcription factor family members. All of them are involved in cell cycle and growth, proliferation, differentiation, apoptosis, and metabolism. More transcription factors specific for each VDAC gene isoform were identified, supporting the results in the literature, indicating a general role of VDAC1, as an actor of apoptosis for VDAC2, and the involvement in sex determination and development of VDAC3. For the first time, we propose a comparative analysis of human VDAC promoters to investigate their specific biological functions. Bioinformatics and experimental results confirm the essential role of the VDAC protein family in mitochondrial functionality. Moreover, insights about a specialized function and different regulation mechanisms arise for the three isoform gene.

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Section: Introductionmentioning

confidence: 99%

Is the Secret of VDAC Isoforms in Their Gene Regulation? Characterization of Human VDAC Genes Expression Profile, Promoter Activity, and Transcriptional Regulators

Zinghirino

Pappalardo

Messina

et al. 2020

IJMS

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“…In this study, sympathetic activation induces mitochondrial disorders, including the reduction of the mitochondrial membrane proteins (VADC1 and COX IV), the increase in abnormal mitochondrial morphology (swollen mitochondria and fractured mitochondrial crest), and the vanishment of the mitochondrial membrane potential ( Figure 7 ). Closed or lost VDAC1 destroyed the integrity of the mitochondrial outer membranes ( 51 ), inhibited mitochondrial respiration, and exacerbated mitochondrial division ( 52 ). Besides, the lack of electron transport chain proteins, such as the cytochrome c oxidase family (like COX IV) ( 53 ), led to electron leakage, which produced ROS-like superoxide free radicals to trigger cellular senescence ( 54 ).…”

Section: Discussionmentioning

confidence: 99%

Sympathetic Denervation Ameliorates Renal Fibrosis via Inhibition of Cellular Senescence

Deng

Liu

et al. 2022

Front. Immunol.

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ObjectiveContinuous overactivation of the renal sympathetic nerve is considered to be an important cause of renal fibrosis. Accumulated senescent cells in the damaged kidney have metabolic activities and secrete amounts of proinflammatory factors as part of the SASP (the senescence-associated secretory phenotype), which induce chronic inflammation and fibrosis. It is still unclear whether renal sympathetic nerves affect renal inflammation and fibrosis by regulating cellular senescence. Therefore, we hypothesize that sympathetic activation in the injured kidney induces cellular senescence, which contributes to progressive renal inflammation and fibrosis.MethodsRenal denervation was performed 2 days before the UUO (unilateral ureteral obstruction) and UIRI (unilateral ischemia-reperfusion injury) models. The effects of renal denervation on renal fibrosis and cellular senescence were observed. In vitro, cellular senescence was induced in renal proximal tubular epithelial cell lines (TKPTS cells) by treatment with norepinephrine (NE). The selective α2A-adrenergic receptor (α2A-AR) antagonists BRL44408 and β-arrestin2 siRNA, were administered to inhibit NE-induced cellular senescence. A significantly altered pathway was identified through immunoblotting, immunofluorescence, immunocytochemistry, and functional assays involved in mitochondrial function.ResultsRenal fibrosis and cellular senescence were significantly increased in UUO and UIRI models, which were partially reversed by renal denervation. In vitro, NE induced epithelial cells secreting proinflammatory cytokines and promoted cell senescence by activating α2A-AR. Importantly, the effects of NE during cellular senescence were blocked by α2A-AR selective antagonist and β-arrestin2 (downstream of α2A-AR) siRNA.ConclusionRenal sympathetic activation and cellular senescence are important neurometabolic and neuroimmune mechanisms in the development of renal fibrosis. Renal sympathetic neurotransmitter NE acting on the α2A-AR of epithelial cells promotes cellular senescence through the downstream β-arrestin2 signaling, which is a potential preventive target for renal fibrosis.

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“…Plasma levels of creatinine were used as a marker of renal function. Blood was drawn while mice were euthanized, spun down and plasma was used to determine creatinine concentration using the Creatinine Reagent Set from Biotron Diagnostics (Hemet, CA, USA) and the manufacturer’s protocol, as reported previously [ 56 , 57 , 58 ]. Plasma creatinine levels were determined in all mice used in the four experimental groups described on page 3.…”

Section: Methodsmentioning

confidence: 99%

“…; Ovation Pharmaceuticals, Deerfield, IL, USA) and all surgical procedures were performed under sterile conditions. Following a midline incision of the abdomen, kidneys were exposed and decapsulated, and both renal hila were clamped for 35 min with small vascular clamps to induce bilateral renal ischemia as described previously [55][56][57][58]. While renal arteries of both kidneys were clamped, mice were placed on a heating pad that maintained a temperature of 37 • C. During that time, approximately 0.5 mL sterile saline was applied intraperitoneally to prevent fluid loss and dehydration.…”

Section: Ischemia/reperfusion Injurymentioning

confidence: 99%

“…Immediately after mice were euthanized, both kidneys were harvested, submerged in an ice-cold isolation buffer (10 mM Hepes, 225 mM mannitol, 75 mM sucrose, 2 mM EGTA, and 0.1% BSA, fatty acid free, pH 7.4) and dissected on ice as described previously [56][57][58]. Cortical tissue separated from the kidneys was homogenized in ice-cold isolation buffer and the homogenate was spun down at 1000× g 5 min at 4 • C. The supernatant resulting from this centrifugation was spun down at 15,000× g 15 min at 4 • C to obtain a mitochondrial pellet.…”

Section: Isolation Of Mitochondriamentioning

confidence: 99%

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γ-Tocotrienol Protects against Mitochondrial Dysfunction, Energy Deficits, Morphological Damage, and Decreases in Renal Functions after Renal Ischemia

Nowak

Megyesi

2021

IJMS

Self Cite

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Ischemia-induced mitochondrial dysfunction and ATP depletion in the kidney result in disruption of primary functions and acute injury of the kidney. This study tested whether γ-tocotrienol (GTT), a member of the vitamin E family, protects mitochondrial function, reduces ATP deficits, and improves renal functions and survival after ischemia/reperfusion injury. Vehicle or GTT (200 mg/kg) were administered to mice 12 h before bilateral kidney ischemia, and endpoints were assessed at different timepoints of reperfusion. GTT treatment reduced decreases in state 3 respiration and accelerated recovery of this function after ischemia. GTT prevented decreases in activities of complexes I and III of the respiratory chain, and blocked ischemia-induced decreases in F0F1-ATPase activity and ATP content in renal cortical tissue. GTT improved renal morphology at 72 h after ischemia, reduced numbers of necrotic proximal tubular and inflammatory cells, and enhanced tubular regeneration. GTT treatment ameliorated increases in plasma creatinine levels and accelerated recovery of creatinine levels after ischemia. Lastly, 89% of mice receiving GTT and 70% of those receiving vehicle survived ischemia. Conclusions: Our data show novel observations that GTT administration improves mitochondrial respiration, prevents ATP deficits, promotes tubular regeneration, ameliorates decreases in renal functions, and increases survival after acute kidney injury in mice.

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Deletion of VDAC1 Hinders Recovery of Mitochondrial and Renal Functions After Acute Kidney Injury

Cited by 17 publications

References 47 publications

Is the Secret of VDAC Isoforms in Their Gene Regulation? Characterization of Human VDAC Genes Expression Profile, Promoter Activity, and Transcriptional Regulators

Is the Secret of VDAC Isoforms in Their Gene Regulation? Characterization of Human VDAC Genes Expression Profile, Promoter Activity, and Transcriptional Regulators

Sympathetic Denervation Ameliorates Renal Fibrosis via Inhibition of Cellular Senescence

γ-Tocotrienol Protects against Mitochondrial Dysfunction, Energy Deficits, Morphological Damage, and Decreases in Renal Functions after Renal Ischemia

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