AUY922 induces retinal toxicity through attenuating TRPM1

Shen, Che-Hung; Hsieh, Chi-Hsun; Jiang, Kuan-Ying; Lin, Chih‐Yu; Chiang, Nai‐Jung; Li, Tingwei; Yen, Chen‐Tung; Chen, Wan-Ju; Hwang, Daw-Yang; Chen, Li-Tzong

doi:10.1186/s12929-021-00751-5

Cited by 11 publications

(13 citation statements)

References 75 publications

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“…The stained tissues were photographed using a light microscope (the gain was set to 1.0x, saturation to 1.00, and gamma to 1.01, Leica DM2000), and their histopathological characteristics were interpreted by two independent investigators. The expression of pCHK2T68 was semiquantitatively evaluated using the H-score [ 24 ] by two independent investigators. The staining intensity was classified into no staining (0), weakly positive [ 1 ], moderately positive [ 2 ] and strongly positive [ 3 ].…”

Section: Methodsmentioning

confidence: 99%

CHK2 activation contributes to the development of oxaliplatin resistance in colorectal cancer

et al. 2022

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Background Colorectal cancer (CRC), the most common cancer type, causes high morbidity and mortality. Patients who develop drug resistance to oxaliplatin-based regimens have short overall survival. Thus, identifying molecules involved in the development of oxaliplatin resistance is critical for designing therapeutic strategies. Methods A proteomic screen was performed to reveal altered protein kinase phosphorylation in oxaliplatin-resistant (OR) CRC tumour spheroids. The function of CHK2 was characterised using several biochemical techniques and evident using in vitro cell and in vivo tumour models. Results We revealed that the level of phospho-CHK2(Thr68) was elevated in OR CRC cells and in ~30% of tumour samples from patients with OR CRC. We demonstrated that oxaliplatin activated several phosphatidylinositol 3-kinase-related kinases (PIKKs) and CHK2 downstream effectors and enhanced CHK2/PARP1 interaction to facilitate DNA repair. A phosphorylation mimicking CHK2 mutant, CHK2T68D, but not a kinase-dead CHK2 mutant, CHK2D347A, promoted DNA repair, the CHK2/PARP1 interaction, and cell growth in the presence of oxaliplatin. Finally, we showed that a CHK2 inhibitor, BML-277, reduced protein poly(ADP-ribosyl)ation (PARylation), FANCD2 monoubiquitination, homologous recombination and OR CRC cell growth in vitro and in vivo. Conclusion Our findings suggest that CHK2 activity is critical for modulating oxaliplatin response and that CHK2 is a potential therapeutic target for OR CRC.

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Section: Methodsmentioning

confidence: 99%

CHK2 activation contributes to the development of oxaliplatin resistance in colorectal cancer

et al. 2022

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“…Despite the plethora of evidence that Hsp90 inhibition can provide protection in the diseased retina as described above, reports from clinical trials in oncology highlight ocular toxicities that have emerged as an important clinical concern ( Table 2 ). Hsp90 N-terminal inhibitors, including ansamycin derivatives (17-dimethylaminoethylamino-17-demethoxygeldanamycin (17-DMAG)), resorcinol derivatives (AT13387, AUY922), and benzamide derivatives (SNX-5422 (PF-04929113)), have been associated with visual disturbances, such as blurred vision, photopsia, night blindness, photophobia, and retinopathy [ 47 , 48 , 49 , 50 , 51 , 52 , 53 , 54 , 55 , 56 , 57 ]. In addition, some preclinical studies have reported that severe retinal degeneration occurred in rats and beagle dogs after treatment with Hsp90 inhibitors [ 46 , 58 , 59 ].The oral administration of the Hsp90 scaffold N-terminal inhibitor CH5164840 led to a loss of pupillary light reflex, abnormal electroretinographic (ERG) responses, and histological changes in the photoreceptor outer nuclear layer, including photoreceptor degeneration, in beagle dogs [ 58 ].…”

Section: The Role Of Hsp90 In Retinal Diseasementioning

confidence: 99%

“…As described previously, GRK1 biosynthesis requires Hsp90, and prolonged Hsp90 inhibition via systemic administration of HSP990 reduced GRK1 and PDE6 levels post-translationally, suggesting that the Hsp90 client list includes important components of the phototransduction cascade. More recently, Transient Receptor Potential cation channel subfamily M member 1 (TRPM1) has been identified as another potential Hsp90 client protein in the retina [ 57 ]. TRPM1 is a constitutively open calcium entry channel primarily expressed in skin melanocytes and retinal ON-bipolar cells in the inner nuclear layer.…”

Section: The Role Of Hsp90 In Retinal Diseasementioning

confidence: 99%

“…TRPM1 is a constitutively open calcium entry channel primarily expressed in skin melanocytes and retinal ON-bipolar cells in the inner nuclear layer. The treatment of mice with AUY922 resulted in increased apoptosis in the photoreceptor outer nuclear layer, disorganization of the photoreceptor outer segments, disruption of RPE cells, and a dose-dependent decrease in TRPM1 via disruption of the interaction with Hsp90 [ 57 ].…”

Section: The Role Of Hsp90 In Retinal Diseasementioning

confidence: 99%

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The Role of Hsp90 in Retinal Proteostasis and Disease

Ziaka¹,

Spuy²

2022

Biomolecules

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Photoreceptors are sensitive neuronal cells with great metabolic demands, as they are responsible for carrying out visual phototransduction, a complex and multistep process that requires the exquisite coordination of a large number of signalling protein components. Therefore, the viability of photoreceptors relies on mechanisms that ensure a well-balanced and functional proteome that maintains the protein homeostasis, or proteostasis, of the cell. This review explores how the different isoforms of Hsp90, including the cytosolic Hsp90α/β, the mitochondrial TRAP1, and the ER-specific GRP94, are involved in the different proteostatic mechanisms of photoreceptors, and elaborates on Hsp90 function when retinal homeostasis is disturbed. In addition, several studies have shown that chemical manipulation of Hsp90 has significant consequences, both in healthy and degenerating retinae, and this can be partially attributed to the fact that Hsp90 interacts with important photoreceptor-associated client proteins. Here, the interaction of Hsp90 with the retina-specific client proteins PDE6 and GRK1 will be further discussed, providing additional insights for the role of Hsp90 in retinal disease.

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“…2 (IL-2) can regulate the expression of inflammatory cytokines in RPE cells through JAK2 and reduce the activity of RPE cells(27). Glycosylated serum protein can promote the secretion of inflammatory cytokines (IL-8) and the expression of MCP-1 by RPE cells through JAK2, thus affecting the function and activity of RPE cells(28). At the same time, a study has shown that the expression level of JAK2 is closely related to mitochondrial function, and extracellular IL-6 can affect the physiological function of intracellular mitochondria by regulating the expression of JAK2(29).…”

mentioning

confidence: 99%

Genipin protects against mitochondrial damage of the retinal pigment epithelium under hyperglycemia through the AKT pathway mediated by the miR-4429/JAK2 signaling axis

Chen¹,

Zhang²,

Zhao³

et al. 2022

Ann Transl Med

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Background: To investigate the protective effect and mechanism of genipin (GE) on mitochondrial damage in retinal pigment epithelial (RPE) cells induced by high glucose.Methods: Differential genes of GE in the treatment of diabetic retinopathy (DR) were screened by the Gene Expression Omnibus (GEO) database. Differential genes located in the AKT pathway were obtained. TargetScan, miRDB, and DIANA databases were used to predict the targeted microRNAs (miRNAs) of differential genes. A high-fat diet combined with streptomycin (STZ) intraperitoneal injection were used to establish a diabetic mouse model. Diabetic mice were treated with GE by intragastric administration. The functional and molecular changes of the retina were detected by electroretinogram (ERG) and reverse transcription-polymerase chain reaction (RT-PCR). ARPE-19 cells were cultured under hyperglycemic conditions with AKT and JAK2 inhibitors. MiR-4429 was knocked down/overexpressed to detect changes in cell function, activity, and mitochondrial function.The dual luciferase reporter assay confirmed the targeted binding of miR-4429 with JAK2.Results: Bioinformatics analysis finally yielded JAK2 as the research target gene. miR-4429 was predicted to be the targeted miRNA of JAK2 by online databases. The results of animal experiments showed that the retinal function of mice recovered after GE administration (P<0.05), the expression of AKT and miR-4429 in RPE cells was significantly increased (P<0.05), and the expression of JAK2 was significantly decreased (P<0.05). The results of cell experiments showed that the functions of cells and mitochondria recovered after the addition of GE under hyperglycemia (P<0.05). Cell and mitochondrial functions were decreased after the addition of AKT inhibitor (P<0.05). Overexpression of miR-4429 or inhibition of JAK2 increased cell activity and mitochondrial function (P<0.05). The results of the dual luciferase reporter assay showed that miR-4429 had a targeted binding site with JAK2.Conclusions: GE protects ARPE-19 cell functional activity, inflammatory responses, and mitochondrial damage by promoting the AKT signaling pathway and regulating the expression of the miR-4429/JAK2 signaling axis.

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AUY922 induces retinal toxicity through attenuating TRPM1

Cited by 11 publications

References 75 publications

CHK2 activation contributes to the development of oxaliplatin resistance in colorectal cancer

CHK2 activation contributes to the development of oxaliplatin resistance in colorectal cancer

The Role of Hsp90 in Retinal Proteostasis and Disease

Genipin protects against mitochondrial damage of the retinal pigment epithelium under hyperglycemia through the AKT pathway mediated by the miR-4429/JAK2 signaling axis

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