USP9X stabilizes BRCA1 and confers resistance to DNA‐damaging agents in human cancer cells

Lu, Qiong; Zhang, Fanglin; Lu, Da Yong; Shao, Zhi‐Ming; Li, Da‐Qiang

doi:10.1002/cam4.2528

Cited by 26 publications

(23 citation statements)

References 67 publications

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“…However, the molecular interplay underlying such clinical effects remains unclear. USP9X has been shown to stabilize BRCA1 and confer resistance to DNA-damaging agents, and yet its downregulation rendered BC cells resistant to tamoxifen, while its up-modulation has been found to promote centrosome amplification, chromosome instability, and higher histologic grades of BC, as well as to enhance Hippo pathway-dependent cell proliferation [ 46 , 47 , 48 , 49 ]. The role of USP7, in turn, appears to be more established in the regulation of DNA replication and mitosis progression by affecting the stability of Aurora-A kinase and Geminin [ 50 , 51 ].…”

Section: Discussionmentioning

confidence: 99%

Mapping of Genomic Vulnerabilities in the Post-Translational Ubiquitination, SUMOylation and Neddylation Machinery in Breast Cancer

Fuentes-Antrás

Alcaráz-Sanabria

Morafraile

et al. 2021

Cancers

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The dysregulation of post-translational modifications (PTM) transversally impacts cancer hallmarks and constitutes an appealing vulnerability for drug development. In breast cancer there is growing preclinical evidence of the role of ubiquitin and ubiquitin-like SUMO and Nedd8 peptide conjugation to the proteome in tumorigenesis and drug resistance, particularly through their interplay with estrogen receptor signaling and DNA repair. Herein we explored genomic alterations in these processes using RNA-seq and mutation data from TCGA and METABRIC datasets, and analyzed them using a bioinformatic pipeline in search of those with prognostic and predictive capability which could qualify as subjects of drug research. Amplification of UBE2T, UBE2C, and BIRC5 conferred a worse prognosis in luminal A/B and basal-like tumors, luminal A/B tumors, and luminal A tumors, respectively. Higher UBE2T expression levels were predictive of a lower rate of pathological complete response in triple negative breast cancer patients following neoadjuvant chemotherapy, whereas UBE2C and BIRC5 expression was higher in luminal A patients with tumor relapse within 5 years of endocrine therapy or chemotherapy. The transcriptomic signatures of USP9X and USP7 gene mutations also conferred worse prognosis in luminal A, HER2-enriched, and basal-like tumors, and in luminal A tumors, respectively. In conclusion, we identified and characterized the clinical value of a group of genomic alterations in ubiquitination, SUMOylation, and neddylation enzymes, with potential for drug development in breast cancer.

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Section: Discussionmentioning

confidence: 99%

Mapping of Genomic Vulnerabilities in the Post-Translational Ubiquitination, SUMOylation and Neddylation Machinery in Breast Cancer

Fuentes-Antrás

Alcaráz-Sanabria

Morafraile

et al. 2021

Cancers

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show abstract

“…Consequently, USP9X processes function of both oncogene and tumor suppressor, depending on the type and stage of cancer. Recently, it was reported that loss of USP9X function prevented tamoxifen-induced proliferation arrest in estrogen receptor positive breast cancer cells, which suggested that USP9X is closely involved in the endocrine therapy resistance of breast cancer 58,59 . Therefore, the regulatory role of USP9X in tumor is diverse.…”

Section: Discussionmentioning

confidence: 99%

Stabilization of EGLN3 by USP9X Contributes to Antineoplastic Function in Cholangiocarcinoma

Chen¹,

Song²,

Liu³

et al. 2020

Preprint

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Background: Cholangiocarcinoma represents the second most common primary liver malignancy. The incidence rate has constantly increased over the last decades. Cholangiocarcinoma silent nature limits early diagnosis and prevents efficient treatment. Methods: Immunoblotting and immunohistochemistry were used to assess the expression profiling of USP9X and EGLN3 in cholangiocarcinoma patients. ShRNA was used to silence gene expression. Cell apoptosis, cell cycle, CCK8, clone formation, shRNA interference and xenograft mouse model were used to explore biological function of USP9X and EGLN3. The underlying molecular mechanism of USP9X in cholangiocarcinoma was determined by immunoblotting, co-immunoprecipitation and quantitative real time PCR (qPCR).Results: Here we demonstrated that USP9X is downregulated in cholangiocarcinoma which contributes to tumorigenesis. The expression of USP9X in cholangiocarcinoma inhibited cell proliferation and colony formation in vitro as well as xenograft tumorigenicity in vivo. Clinical data demonstrated that expression levels of USP9X were positively correlated with favorable clinical outcomes. Mechanistic investigations further indicated that USP9X was involved in the deubiquitination of EGLN3, a member of 2-oxoglutarate and iron-dependent dioxygenases. USP9X elicited tumor suppressor role by preventing degradation of EGLN3. Importantly, knockdown of EGLN3 impaired USP9X-mediated suppression of proliferation. USP9X positively regulated the expression level of apoptosis pathway genes KIF1Bβ through EGLN3 thus involved in apoptosis of cholangiocarcinoma. Conclusion: These findings help to understand that USP9X alleviates the malignant potential of cholangiocarcinoma through upregulation of EGLN3. Consequently, we provided novel insight into that USP9X is a potential biomarker or serves as a therapeutic or diagnostic target for cholangiocarcinoma.

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“…Consequently, USP9X processes function of both oncogene and tumor suppressor, depending on the type and stage of cancer. Recently, it was reported that loss of USP9X function prevented tamoxifen-induced proliferation arrest in estrogen receptor positive breast cancer cells, which suggested that USP9X is closely involve in the endocrine therapy resistance of breast cancer 58,59 . Therefore, the regulatory role of USP9X in tumor is diverse.…”

Section: Dicussionmentioning

confidence: 99%

USP9X promotes apoptosis in cholangiocarcinoma by modulation expression of KIF1Bβ via deubiquitinating EGLN3

Chen

Song

Liu

et al. 2021

Preprint

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Cholangiocarcinoma represents the second most common primary liver malignancy. The incidence rate has constantly increased over the last decades. Cholangiocarcinoma silent nature limits early diagnosis and prevents efficient treatment. Here we demonstrated that USP9X is downregulated in cholangiocarcinoma which contributes to tumorigenesis. The expression of USP9X in cholangiocarcinoma inhibited cell proliferation and colony formation in vitro as well as xenograft tumorigenicity in vivo. Clinical data demonstrated that expression levels of USP9X were positively correlated with favorable clinical outcomes. Mechanistic investigations further indicated that USP9X was involved in the deubiquitination of EGLN3, a member of 2-oxoglutarate and iron-dependent dioxygenases. USP9X elicited tumor suppressor role by preventing degradation of EGLN3. Importantly, knockdown of EGLN3 impaired USP9X-mediated suppression of proliferation. USP9X positively regulated the expression level of apoptosis pathway genes KIF1Bβ through EGLN3 thus involved in apoptosis of cholangiocarcinoma. Together, these findings help to understand that USP9X alleviates the malignant potential of cholangiocarcinoma through upregulation of EGLN3. Consequently, we provided novel insight into that USP9X is a potential biomarker or serves as a therapeutic or diagnostic target for cholangiocarcinoma.

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USP9X stabilizes BRCA1 and confers resistance to DNA‐damaging agents in human cancer cells

Cited by 26 publications

References 67 publications

Mapping of Genomic Vulnerabilities in the Post-Translational Ubiquitination, SUMOylation and Neddylation Machinery in Breast Cancer

Mapping of Genomic Vulnerabilities in the Post-Translational Ubiquitination, SUMOylation and Neddylation Machinery in Breast Cancer

Stabilization of EGLN3 by USP9X Contributes to Antineoplastic Function in Cholangiocarcinoma

USP9X promotes apoptosis in cholangiocarcinoma by modulation expression of KIF1Bβ via deubiquitinating EGLN3

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