PAX8 activates a p53-p21-dependent pro-proliferative effect in high grade serous ovarian carcinoma

Ghannam-Shahbari, Dima; Jacob, Eyal; Kakun, Reli Rachel; Wasserman, Tanya; Korsensky, Lina; Sternfeld, Ofir; Kagan, Juliana; Bublik, Debora Rosa; Aviel‐Ronen, Sarit; Levanon, Keren; Sabo, Edmond; Larisch, Sarit; Oren, Moshe; Hershkovitz, Dov; Perets, Ruth

doi:10.1038/s41388-017-0040-z

Cited by 35 publications

(29 citation statements)

References 59 publications

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“…More importantly, we found that PAX8 silencing inhibited the proliferation and clonogencity of HCC cells in vitro and the growth of implanted HCC xenografts in vivo. Furthermore, PAX8 silencing induced HCC cell cycle arrest in S phase by downregulating E2F1, RB and P53 expression in HCC cells, consistent with previous reports [16,33]. Therefore, PAX8 may be a new biomarker and therapeutic target for prognosis and intervention of HCC.…”

Section: Discussionsupporting

confidence: 89%

“…PAX8 is important for embryogenesis, and morphogenesis of the thyroid and kidney [14]. Furthermore, PAX8 expression is upregulated in several types of cancers and is a valuable biomarker for diagnosis of glioma, ovarian carcinoma, gastric cancer and others [15][16][17]. A recent study has reported that single nuclear polymorphism of the PAX8 gene is associated with prognosis of Chinese patients with HCC [18].…”

Section: Introductionmentioning

confidence: 99%

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HBx regulates transcription factor PAX8 stabilization to promote the progression of hepatocellular carcinoma

Wang

Huang

et al. 2019

Oncogene

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Transcription factor PAX8 expression is upregulated in several types of cancers. However, little is known about the function of PAX8 in the progression of hepatoma and its regulatory mechanisms. Here, we show that PAX8 silencing inhibits the proliferation and clonogenicity of hepatoma cells and its growth in vivo. The HBV X protein (HBx) does not directly interacts, but stabilizes PAX8 by inhibiting proteasome-dependent ubiquitination and degradation. Furthermore, the E3 ubiquitin ligase complex component Skp2 through its LRR domain directly interacts with the Prd domain of PAX8 and targets PAX8 by recognizing its lysine 275 for ubiquitination and degradation in hepatoma cells. In addition, HBx directly interacts and is colocalized with Skp2 to inhibit its recognition and subsequent ubiquitination and degradation of PAX8 in hepatoma cells. Moreover, HBx upregulates the expression and phosphorylation of Aurora A, a serine-threonine kinase, which interacts with and phosphorylates PAX8 at S209 and T277, compromising the Skp2-recognized PAX8 ubiquitination and destabilization. Thus, HBx stabilizes PAX8 protein by inhibiting the Skp2 targeted PAX8 ubiquitination and enhancing the Aurora A-mediated its phosphorylation, contributing to the progression of hepatoma. Our findings suggest that PAX8 may a new target for design of therapies and uncover new insights into the pathogenesis of hepatoma.

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Section: Discussionsupporting

confidence: 89%

Section: Introductionmentioning

confidence: 99%

HBx regulates transcription factor PAX8 stabilization to promote the progression of hepatocellular carcinoma

Wang

Huang

et al. 2019

Oncogene

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“…The sustained expression of PAX8 in the adult FTSEC and in nearly all HGSOCs (16), previously led us to use the PAX8 promoter to develop a genetically engineered mouse model of HGSOC (17,18). Knockdown of PAX8 in ovarian cancer cells leads to apoptosis (19)(20)(21) supporting a definitive role for PAX8 in ovarian cancer growth and progression. However, it remains unclear how PAX8 drives the development of the Mullerian reproductive tract or how it supports neoplastic growth.…”

Section: Introductionmentioning

confidence: 99%

PAX8 orchestrates an angiogenic program through interaction with SOX17

Chaves-Moreira

Mitchell

Arruza

et al. 2020

Preprint

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Worldwide, the number of new ovarian cancer cases approaches 300,000 with more than 180,000 deaths every year. The low survival-rate reflects the limitations of current therapies and highlights the importance of identifying new therapeutic targets. Despite significant recent efforts to identify novel vulnerabilities in ovarian cancer, none have led to effective durable therapies with improvement in overall survival. PAX8, a lineage-transcription factor, whose expression is a major molecular feature of ovarian carcinomas, represents a novel therapeutic target. Herein, we have identified SOX17 as a bona fide PAX8-interacting partner and elucidated the impact of this interaction on the development of ovarian cancer. Importantly, we found that PAX8 and SOX17 regulate tumor angiogenesis in vitro and in vivo. The role of PAX8 and SOX17 in the regulation of angiogenesis reveals a novel function for these factors in regulating the tumor microenvironment and highlight this pathway as a viable therapeutic target.

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“…Some of the new protein coding associations involved alternative promoters of known cancer genes that were not represented in the hg19 version, such as epigenetic regulation of the PAX8 gene in a subset of CHOL tumors ( Figures 3D and 3E). While PAX8 activity has been associated with cancers originating from the thyroid, M€ ullerian, and renal tracts (Ghannam-Shahbari et al, 2018;Laury et al, 2011), neither this new isoform nor upregulation in cholangiocarcinoma have been previously described. In Supplemental Methods, we describe additional resources available at the GDC that can aid users in analyzing TCGA methylation data: (1) improved HM27/HM450 probe annotation (Zhou et al, 2017) and data generation pipelines (Zhou et al, 2018b), which are planned to become the default processing version in a forthcoming GDC data release; and Whole-Genome Bisulfite Sequence data for 47 TCGA samples (Zhou et al, 2018a), which can be used to investigate whole-genome methylation patterns.…”

Section: Dna Methylationmentioning

confidence: 97%

Before and After: Comparison of Legacy and Harmonized TCGA Genomic Data Commons’ Data

et al. 2019

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PAX8 activates a p53-p21-dependent pro-proliferative effect in high grade serous ovarian carcinoma

Cited by 35 publications

References 59 publications

HBx regulates transcription factor PAX8 stabilization to promote the progression of hepatocellular carcinoma

HBx regulates transcription factor PAX8 stabilization to promote the progression of hepatocellular carcinoma

PAX8 orchestrates an angiogenic program through interaction with SOX17

Before and After: Comparison of Legacy and Harmonized TCGA Genomic Data Commons’ Data

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