论文信息 - Ubiquitination of Ku70 by Parkin promotes apoptosis of lens epithelial cells

Ubiquitination of Ku70 by Parkin promotes apoptosis of lens epithelial cells

Oxidative damage‐triggered apoptosis in lens epithelial cells is considered as a main risk factor in the pathogenesis of age‐related cataracts. Ku70 is a key factor in the DNA repair process of double‐strand breaks. In the present study, we aimed to investigate the role of Ku70 and its related E3 ubiquitin ligase in lens epithelial cell apoptosis. The levels of Ku70 in the anterior lens capsules of human cataracts and Emory mice were lower compared to controls. H2O2 treatment resulted in decreased expression of Ku70 through accelerating Ku70 ubiquitination. Parkin, an E3 ubiquitin ligase, could interact with Ku70 and promote the ubiquitination and degradation of this protein. In addition, ubiquitinated Ku70 was regulated by ubiquitin‐proteasome, autophagy‐lysosome and mitophagy pathways. Ectopic expression of Ku70 protected SRA01/04 cells from H2O2‐induced apoptosis, whereas silencing Ku70 exhibited the opposite trend. Co‐transfected with Parkin non‐ubiquitinatable Ku70 mutant could maintain its anti‐apoptosis ability, whereas wild‐type Ku70 failed. Moreover, Ku70 might facilitate mitochondrial fusion by increasing the expression of Mitofusin 1/2. The present study revealed that Parkin‐mediated Ku70 ubiquitination facilitated H2O2‐induced lens epithelial cell apoptosis through alleviating mitochondrial fusion, which could provide potential targets for age‐related cataract treatment.

[1] Jinglan Li,et al. Biliverdin Reductase A Protects Lens Epithelial Cells against Oxidative Damage and Cellular Senescence in Age-Related Cataract , 2022, Oxidative medicine and cellular longevity.

[2] Yi Luo,et al. Acetyl-11-Keto-Beta Boswellic Acid (AKBA) Protects Lens Epithelial Cells Against H2O2-Induced Oxidative Injury and Attenuates Cataract Progression by Activating Keap1/Nrf2/HO-1 Signaling , 2022, Frontiers in Pharmacology.

[3] J. Troncoso,et al. Neuronal NLRP3 is a parkin substrate that drives neurodegeneration in Parkinson’s disease , 2022, Neuron.

[4] Lin Chen,et al. Multifaceted regulation and functions of 53BP1 in NHEJ-mediated DSB repair (Review) , 2022, International journal of molecular medicine.

[5] W. Huang,et al. Cytosolic p53 Inhibits Parkin-Mediated Mitophagy and Promotes Acute Liver Injury Induced by Heat Stroke , 2022, Frontiers in Immunology.

[6] Y-J Chi,et al. MDM2-mediated ubiquitination of LKB1 contributes to the development of diabetic cataract. , 2022, Experimental cell research.

[7] H. Chen,et al. PINK1/Parkin-mediated mitophagy in cardiovascular disease: From pathogenesis to novel therapy. , 2022, International journal of cardiology.

[8] Y. Shao,et al. The E3 Ligase RNF157 Inhibits Lens Epithelial Cell Apoptosis by Negatively Regulating p53 in Age-Related Cataracts , 2022, Investigative Ophthalmology and Visual Science.

[9] M. Ji,et al. XRCC5 downregulated by TRIM25 is susceptible for lens epithelial cell apoptosis. , 2022, Cellular signalling.

[10] Qing-Jun Zhang,et al. Evaluation of Parkin in the Regulation of Myocardial Mitochondria-Associated Membranes and Cardiomyopathy During Endotoxemia , 2022, Frontiers in Cell and Developmental Biology.

[11] Yanjie Lu,et al. CIRKIL Exacerbates Cardiac Ischemia/Reperfusion Injury by Interacting With Ku70 , 2022, Circulation research.

[12] Wei-Chi Wu,et al. The Pathomechanism, Antioxidant Biomarkers, and Treatment of Oxidative Stress-Related Eye Diseases , 2022, International journal of molecular sciences.

[13] G. Ding,et al. Mfn2 Regulates High Glucose-Induced MAMs Dysfunction and Apoptosis in Podocytes via PERK Pathway , 2021, Frontiers in Cell and Developmental Biology.

[14] Toshiyuki Shimizu,et al. Structural Diversity of Ubiquitin E3 Ligase , 2021, Molecules.

[15] N. Ito,et al. HMGB1 signaling phosphorylates Ku70 and impairs DNA damage repair in Alzheimer’s disease pathology , 2021, Communications Biology.

[16] Daisy Y. Shu,et al. Hallmarks of lens aging and cataractogenesis. , 2021, Experimental eye research.

[17] B. Zhao,et al. Ubiquitination Destabilizes Protein Sphingosine Kinase 2 to Regulate Glioma Malignancy , 2021, Frontiers in Cellular Neuroscience.

[18] J. Charbonnier,et al. The Multifaceted Roles of Ku70/80 , 2021, International journal of molecular sciences.

[19] S. Raghavan,et al. Nonhomologous end joining: new accessory factors fine tune the machinery. , 2021, Trends in genetics : TIG.

[20] Guowei Zhang,et al. MicroRNA Let-7c-5p-Mediated Regulation of ERCC6 Disrupts Autophagic Flux in Age-Related Cataract via the Binding to VCP , 2021, Current eye research.

[21] J. Salazar,et al. The Role of Autophagy in Eye Diseases , 2021, Life.

[22] Liang Ding,et al. Transcriptional network constituted of CBP, Ku70, NOX2, and BAX prevents the cell death of necrosis, paraptosis, and apoptosis in human melanoma , 2021, Cell death discovery.

[23] P. Humphrey,et al. Down-regulation of GP130 signaling sensitizes bladder cancer to cisplatin by impairing Ku70 DNA repair signaling and promoting apoptosis. , 2021, Cellular signalling.

[24] N. Afshari,et al. Cataract and systemic disease: A review , 2021, Clinical & experimental ophthalmology.

[25] Jianfeng Yu,et al. Ginsenoside Rg1 Prevents H2O2-induced Lens Opacity , 2021, Current eye research.

[26] Guowei Zhang,et al. Long non-coding RNA nuclear paraspeckle assembly transcript 1 protects human lens epithelial cells against H2O2 stimuli through the nuclear factor kappa b/p65 and p38/mitogen-activated protein kinase axis , 2020, Annals of translational medicine.

[27] Suna Kang,et al. Polygenetic-Risk Scores Related to Crystallin Metabolism Are Associated with Age-Related Cataract Formation and Interact with Hyperglycemia, Hypertension, Western-Style Diet, and Na Intake , 2020, Nutrients.

[28] M. Lieber,et al. The molecular basis and disease relevance of non-homologous DNA end joining , 2020, Nature Reviews Molecular Cell Biology.

[29] Qing Yang,et al. The role of ubiquitination and deubiquitination in cancer metabolism , 2020, Molecular Cancer.

[30] Jing-Bo Lu,et al. TTDA inhibited apoptosis by regulating the p53-Bax/Bcl2 axis in glioma , 2020, Experimental Neurology.

[31] Lei Sun,et al. MDM2 phosphorylation mediates H2O2-induced lens epithelial cells apoptosis and age-related cataract. , 2020, Biochemical and biophysical research communications.

[32] Jie Yang,et al. Parkin ubiquitinates GATA4 and attenuates the GATA4/GAS1 signaling and detrimental effects on diabetic nephropathy , 2020, FASEB journal : official publication of the Federation of American Societies for Experimental Biology.

[33] Xiaojing Liu,et al. Mitochondrial ROS-Modulated mtDNA: A Potential Target for Cardiac Aging , 2020, Oxidative medicine and cellular longevity.

[34] A. Dillin,et al. Mitochondrial , 2020, Definitions.

[35] A. Almasan,et al. USP14 is a deubiquitinase for Ku70 and critical determinant of non-homologous end joining repair in autophagy and PTEN-deficient cells , 2019, Nucleic acids research.

[36] A. García-Sáez,et al. The Incomplete Puzzle of the BCL2 Proteins , 2019, Cells.

[37] N. Willis,et al. DNA double-strand break repair-pathway choice in somatic mammalian cells , 2019, Nature Reviews Molecular Cell Biology.

[38] Wei Huang,et al. Sirt3 enhances glioma cell viability by stabilizing Ku70–BAX interaction , 2018, OncoTargets and therapy.

[39] T. Jiang,et al. MFN2 ameliorates cell apoptosis in a cellular model of Parkinson's disease induced by rotenone. , 2018, Experimental and therapeutic medicine.

[40] Junying Yuan,et al. Parkin regulates NF-κB by mediating site-specific ubiquitination of RIPK1 , 2018, Cell Death & Disease.

[41] R. Youle,et al. Mitophagy and Quality Control Mechanisms in Mitochondrial Maintenance , 2018, Current Biology.

[42] Jiangyue Zhao,et al. Embryonic Surface Ectoderm-specific Mitofusin 2 Conditional Knockout Induces Congenital Cataracts in Mice , 2018, Scientific Reports.

[43] T. Shinohara,et al. Age-related cataracts: Role of unfolded protein response, Ca2+ mobilization, epigenetic DNA modifications, and loss of Nrf2/Keap1 dependent cytoprotection , 2017, Progress in Retinal and Eye Research.

[44] I. Dikič. Proteasomal and Autophagic Degradation Systems. , 2017, Annual review of biochemistry.

[45] Guowei Zhang,et al. MiR-2964a-5p binding site SNP regulates ATM expression contributing to age-related cataract risk. , 2017, Oncotarget.

[46] M. Koike,et al. Cloning, localization and focus formation at DNA damage sites of canine Ku70 , 2017, The Journal of veterinary medical science.

[47] G. Krasnov,et al. Mitochondrial dysfunction and oxidative stress in aging and cancer , 2016, Oncotarget.

[48] L. Krejci,et al. Cancer TARGETases: DSB repair as a pharmacological target. , 2016, Pharmacology & therapeutics.

[49] Yosvany López,et al. HitPredict version 4: comprehensive reliability scoring of physical protein–protein interactions from more than 100 species , 2015, Database J. Biol. Databases Curation.

[50] R. Bowater,et al. Ku80 Counters Oxidative Stress-Induced DNA Damage and Cataract Formation in the Human Lens. , 2015, Investigative ophthalmology & visual science.

[51] S. Jackson,et al. Neddylation Promotes Ubiquitylation and Release of Ku from DNA-Damage Sites , 2015, Cell reports.

[52] Yuanbin Li,et al. Expression of the microRNAs hsa-miR-15a and hsa-miR-16-1 in lens epithelial cells of patients with age-related cataract. , 2015, International journal of clinical and experimental medicine.

[53] S. Rowan,et al. Altered ubiquitin causes perturbed calcium homeostasis, hyperactivation of calpain, dysregulated differentiation, and cataract , 2015, Proceedings of the National Academy of Sciences.

[54] T. Peng,et al. Effect of Ku70 expression on radiosensitivity in renal carcinoma 786-O cells , 2014, Cancer Cell International.

[55] W. Curran,et al. Role of Ku70 in deubiquitination of Mcl-1 and suppression of apoptosis , 2014, Cell Death and Differentiation.

[56] M. Koike,et al. The defect of Ku70 affects sensitivity to x-ray and radiation-induced caspase-dependent apoptosis in lung cells. , 2013, The Journal of veterinary medical science.

[57] D R Mani,et al. Refined Preparation and Use of Anti-diglycine Remnant (K-ε-GG) Antibody Enables Routine Quantification of 10,000s of Ubiquitination Sites in Single Proteomics Experiments* , 2012, Molecular & Cellular Proteomics.

[58] O. Ates,et al. Oxidative DNA damage in patients with cataract , 2010, Acta ophthalmologica.

[59] D. Green,et al. Mitochondria and cell death: outer membrane permeabilization and beyond , 2010, Nature Reviews Molecular Cell Biology.

[60] Ó. Teijido,et al. Upregulation of Bcl2 inhibits apoptosis‐driven BAX insertion but favors BAX relocalization in mitochondria , 2010, FEBS letters.

[61] J. King,et al. Ubiquitin proteasome pathway-mediated degradation of proteins: effects due to site-specific substrate deamidation. , 2010, Investigative ophthalmology & visual science.

[62] A. Haas,et al. Hdm2 is an Ubiquitin Ligase of Ku70 -Akt Promotes Cell Survival by Inhibiting Hdm2-dependent Ku70 Destabilization , 2008, Cell Death and Differentiation.

[63] R. Youle,et al. Mitochondrial dynamics and apoptosis. , 2008, Genes & development.

[64] Avigail D. Amsel,et al. Regulation of the proapoptotic factor Bax by Ku70-dependent deubiquitylation , 2008, Proceedings of the National Academy of Sciences.

[65] Arturo Carta,et al. Oxidative Stress and Age-Related Cataract , 2000, Ophthalmologica.

[66] M. Kantorow,et al. Parkin elimination of mitochondria is important for maintenance of lens epithelial cell ROS levels and survival upon oxidative stress exposure. , 2017, Biochimica et biophysica acta. Molecular basis of disease.

[67] R. Hartmann-Petersen,et al. The Ku70/80 ring in Non-Homologous End-Joining: easy to slip on, hard to remove. , 2016, Frontiers in bioscience.

[68] C. Schild-Poulter,et al. The Ku heterodimer: function in DNA repair and beyond. , 2015, Mutation research. Reviews in mutation research.

[69] F. Shang,et al. Role of the ubiquitin-proteasome in protein quality control and signaling: implication in the pathogenesis of eye diseases. , 2012, Progress in molecular biology and translational science.