Mitophagy Impairment Aggravates Cisplatin-Induced Ototoxicity

Cho, Sung Il; Jo, Eu-Ri; Song, Han

doi:10.1155/2021/5590973

Cited by 14 publications

(7 citation statements)

References 33 publications

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“…Studies have revealed a tight relationship between mitophagy and SNHL, as well as the signi cance of mitophagy in preserving inner ear homeostasis (Zhang et al 2023). According to several studies, impairment of mitophagy can worsen hearing loss brought on by medications and other variables (Cho et al 2021;Kim et al 2021;Li et al 2023a), and up-regulation of mitophagy can reduce drug-induced ototoxic damage (Han et al 2023). The process of mitochondrial ssion is critical for mitophagy.…”

Section: Discussionmentioning

confidence: 99%

Gipc3 Mutation Might Cause Sensorineural Hearing Loss by Inhibiting Mitophagy in Inner Ear Hair Cells

Li,

Wang,

Shi

et al. 2024

Preprint

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Sensory hearing loss (SNHL) has a high degree of genetic heterogeneity, and there are many mutated genes that cause deafness. GIPC3 gene is one of the mutated genes that can cause congenital hearing loss found in recent years, but the mechanism of its cause is still unclear. Mitophagy is the process of selectively encapsulating and lysing damaged or dysfunctional mitochondria in order to prevent accumulation of damaged mitochondria from damaging the cells and is of great importance in the maintenance of homeostasis in the inner ear. The aim of this paper is to observe the effect of Gipc3 expression on mitochondrial metabolism and autophagy in inner ear hair cells, and to explore the possible mechanism of sensorineural hearing loss caused by Gipc3 mutations. In this study, The House Ear Institute Organ of Corti 1(HEI-OC1) cells and cochlear explants were cultured to change the expression level of Gipc3 by transfection, and the knockdown efficiency was examined by quantitative polymerase chain reaction (qPCR) and Western Blot. Knockdown of Gipc3 inhibited cell viability and its proliferation ability. When t-BHP was used to induce oxidative stress injury and knockdown of Gipc3, inner ear hair cells had weakened ability to resist oxidative stress injury, mitochondrial metabolism was altered, and there was accumulation of reactive oxygen species and reduction of mitochondrial membrane potential. Immunofluorescence and Western Blot techniques revealed that the mitochondrial autophagy-related proteins, LC3B and P62, showed autophagy disorders. A PH domain, leucine zipper motif 1(APPL1) mediates early endosome-dependent mitophagy, and deletion of APPL1 impairs mitochondrial autophagy. We found that fluorescence co-localization exists between Gipc3 and APPL1, and that they interact with each other, with positive correlation in their trends. In summary, Gipc3 mutation may lead to decreased mitochondrial function by inhibiting the APPL1-mediated mitochondrial autophagy process, out of which impaired oxidative metabolism in hair cells may occur, which is a possible mechanism for the inhibition of mitochondrial autophagy by Gipc3 mutation.

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Section: Discussionmentioning

confidence: 99%

Gipc3 Mutation Might Cause Sensorineural Hearing Loss by Inhibiting Mitophagy in Inner Ear Hair Cells

Li,

Wang,

Shi

et al. 2024

Preprint

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“…Although low CUR and CUR-NP concentrations could protect OHCs from CDDP damage, the exact mechanism responsible for this protection remains unclear. CDDP is known to promote endogenous mitochondrial damage and HC apoptosis via upregulation of oxidative stress, which eventually leads to ototoxicity. , Additional reports revealed that enhanced ROS synthesis was a primary mechanism that regulates ototoxic drug-driven HC apoptosis. Excess ROS inhibits HC activity, impairs antioxidant defense, and promotes the mitochondrial release of the apoptotic factor cytochrome C. − Mitochondrial apoptosis involves regulation by both pro- and antiapoptotic members of the Bax family of proteins, and Caspase-3 is the ultimate target of this process .…”

Section: Discussionmentioning

confidence: 99%

Curcumin-Encapsulated Chitosan-Coated Nanoformulation as an Improved Otoprotective Strategy for Ototoxic Hearing Loss

et al. 2022

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Overexpression of apoptotic factors in the inner ear is generally proven to induce ototoxicity. This has aroused research interest in various antiapoptotic drugs, the most representative of which is curcumin (CUR). In this study, two nanoformulations of CUR were developed with sustained-release behavior to improve their protective effects against ototoxic hearing loss (HL), which were the nanoparticles of CUR-loaded poly(lactic acid–glycolic acid) (CUR-PLGA NPs) and CUR-loaded chitosan-coated PLGA NPs (CUR-CS/PLGA NPs). The obtained results revealed that both CUR-NPs provided otoprotection in vitro and in vivo, and their effective doses in guinea pigs were much less than that of dexamethasone, which was clinically used to treat HL. Moreover, relative to CUR and CUR-PLGA NPs, CUR-CS/PLGA NPs exhibited the highest accumulation in HEI-OC1 cells and guinea pigs’ cochlea. In pharmacodynamic experiments, the optimal administration timing was investigated, and CUR-CS/PLGA NPs showed sustained efficacy and the best hearing improvement at all tested sound frequencies. Lastly, the protective effect of CUR nanoformulations was further validated via inhibition of Caspase-3 and Bax activation, thereby reducing the concentration of reactive oxygen species and protecting mitochondrial integrity in hair cells. Collectively, CUR-CS/PLGA NPs demonstrated potent and lasting effects against ototoxic HL, making our novel formulation a promising candidate for the alleviation of sensorineural HL.

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“…Currently,cisplatin induced ototoxicity is a major obstacles that limited the maximum e cacy for tumor patients.Previously studies demonstrated that miRNA was closely associated with hearing loss and considered as promising therapeutic targets [29] .A currently study reported mitophagy protected HEI-OC1 cells against cisplatin-induced ototoxicity [30] ,but the precise molecular mechanism remained to be further studied.In the present study,we investigated whether miR-34a/DRP1-meditaed mitophagy contributed to cisplatin-induced ototoxicity and sought to determined the underlying mechanism.…”

Section: Discussionmentioning

confidence: 99%

“…HEI-OC1 cells were treated with various concentration cisplatin (10,20,30, and 40 uM) and detected the cell viability at 8,16,24, and 48 h after exposure.CCK-8 assay indicated that cisplatin exposure induced cytotoxicity of HEI-OC1 Cells in a dose-time dependent manner (Fig. 3A ).The cell viability was appropriately 45.2% in HEI-OC1 cell treated with 20 uM cisplatin for 24 h.Therefore,we chose 20 um cisplatin for 24h as the exposure concentration and time of the subsequent experiments.…”

Section: Cisplatin Induced Cytotoxicity Via Mitochondrial Dysfunction...mentioning

confidence: 99%

miR-34a/DRP-1-mediated mitophagy participated in cisplatin-induced ototoxicity via increasing oxidative stress

Wang

Lin

Kang

et al. 2022

Preprint

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Purpose Cisplatin is a widely and effectively chemotherapy agent for most of solid malignant tumors. However,cisplatin induced ototoxicity is a common adverse effect,which limited the therapeutic efficacy of tumors in clinic.To date,the specific mechanism of ototoxicity is not fully elucidated and the management of cisplatin-induced ototoxicity also is an urgent challenge.Recently,some authors believed that miR34a and mitophagy played a role in age-related and drug-induced hearing loss.Our study is aimed at exploring the involvement of miR-34a/DRP-1 mediated mitophagy on cisplatin-induced ototoxicity. Methods In this study,C57BL/6 mices and HEI-OC1 cells were treated with cisplatin,miR-34a and DRP-1 level was analyzed by qRT-PCR and western blot,and assessed mitochondrial function via oxidative stress,JC-1 and ATP content.Subsequently,we detected DRP-1 level and observed mitochondrial function through modulating miR-34a expression in HEI-OC1 cells,to determine the effect of miR-34a on DRP-1 mediated mitophagy. Results MiR-34a expression increased and DRP-1 level decreased in C57BL/6 mice and HEI-OC1 cell treated with cisplatin,and mitochondria dysfunction was involved in the process.Furthermore,miR-34a mimic decreased DRP-1 expression,enhanced cisplatin-induced ototoxicity and aggravated mitochondrial dysfunction.We further verified that miR-34a inhibitor increased DRP-1 expression, partially protected aganist cisplatin-induced ototoxicity and improved mitochondrial function. Conclusion MiR-34a/DRP-1-mediated mitophagy was related to cisplatin induced ototoxicity and might be a novel target for investigating the treatement and protection of cisplatin-induced ototoxicity.

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Mitophagy Impairment Aggravates Cisplatin-Induced Ototoxicity

Cited by 14 publications

References 33 publications

Gipc3 Mutation Might Cause Sensorineural Hearing Loss by Inhibiting Mitophagy in Inner Ear Hair Cells

Gipc3 Mutation Might Cause Sensorineural Hearing Loss by Inhibiting Mitophagy in Inner Ear Hair Cells

Curcumin-Encapsulated Chitosan-Coated Nanoformulation as an Improved Otoprotective Strategy for Ototoxic Hearing Loss

miR-34a/DRP-1-mediated mitophagy participated in cisplatin-induced ototoxicity via increasing oxidative stress

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