TGF-β signalling and PEG10 are mutually exclusive and inhibitory in chondrosarcoma cells

Shinohara, Naoyuki; Maeda, Shingo; Yahiro, Yuhei; Sakuma, Daisuke; Matsuyama, Kanehiro; Imamura, Katsuyuki; Kawamura, Ichiro; Setoguchi, Takao; Ishidou, Yasuhiro; Nagano, Satoshi; Komiya, Setsuro

doi:10.1038/s41598-017-13994-w

Cited by 16 publications

(12 citation statements)

References 60 publications

(60 reference statements)

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“…2 a, PEG10 is relatively highly expressed in placenta, adrenal, ovary, testis and brain, but the expression levels are pretty low in other tissues, which are consistent with the previous literature [ 1 , 7 – 9 ]. As shown in Table 1 , several studies have reported PEG10 is positively expressed in a variety of cancers such as hepatocellular carcinoma (HCC) [ 9 , 16 – 19 ], pancreatic carcinoma [ 20 ], breast cancer [ 10 ], prostate cancer [ 10 ], gallbladder carcinoma [ 21 ], thyroid cancer [ 22 ], oral squamous cell carcinoma [ 23 ], colon cancer [ 24 ], enchondromas [ 25 ] and B-cell chronic lymphocytic leukemia (B-CLL) [ 26 ]. Worth noting was that the amplification of PEG10 gene copy numbers detected in HCC also contributed to PEG10 overexpression [ 17 , 27 – 29 ].…”

Section: The Expression Levels Of Peg10 In Cancersmentioning

confidence: 99%

“…In HCC, PEG10 was increased after treating HepG2 cells with TGF-β1 [ 44 ]. However, the mutual inhibition effect of PEG10 and TGF-β signaling was found in chondrosarcoma and enchondroma [ 25 ]. Shinohara et al proposed that TGF-β might inhibit PEG10 expression through the downregulation of c-MYC [ 10 , 25 , 35 ].…”

Section: The Expression Levels Of Peg10 In Cancersmentioning

confidence: 99%

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PEG10 as an oncogene: expression regulatory mechanisms and role in tumor progression

Xie

Zheng

et al. 2018

Cancer Cell Int

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Cancer is a major public health problem as one of the leading causes of death worldwide. Deciphering the molecular regulation mechanisms of tumor progression can make way for tumor diagnosis and therapy. Paternally expressed gene 10 (PEG10), located on human chromosome 7q21.3, has turned out to be an oncogene implicated in the proliferation, apoptosis and metastasis of tumors. PEG10 has been found to be positively expressed in a variety of cancers with seemingly complex expression regulation mechanisms. In this review, we focus on the most vital factors influencing PEG10 expression and recapitulate some of the currently known and potential mechanisms of PEG10 affecting tumor progression, as understanding the molecular regulatory mechanisms of tumor progression can provide potential PEG10 related diagnosis and biomarker specific targeted therapies.

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Section: The Expression Levels Of Peg10 In Cancersmentioning

confidence: 99%

Section: The Expression Levels Of Peg10 In Cancersmentioning

confidence: 99%

PEG10 as an oncogene: expression regulatory mechanisms and role in tumor progression

Xie

Zheng

et al. 2018

Cancer Cell Int

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“… 41 In other report, SOX9 is dramatically decreased in grade 1 chondrosarcoma. 42 Taken these, SOX9 expression level may not be used as a prognostic marker, but can be used as a therapeutic target.…”

Section: Sox4 and Sox9mentioning

confidence: 99%

“… 43 44 BMPRs and runt-related transcription factor 2 (RUNX2) signalling in bone development and carcinogenesis are well known but not in chondrogenesis. Shinohara et al 42 have revealed that phosphorylated Smad3 and Smad1/5 is increased in chondrosarcoma, and Yang et al 45 have shown that BMPR2 and RUNX2 expression is correlated with poor prognosis in 57 patients with various grades chondrosarcoma. 45 BMPR2 downstream Smad1/5 signal promotes tumour growth of chondrosarcoma cells in vivo.…”

Section: Transforming Growth Factor-beta and Bone Morphogenetic Protementioning

confidence: 99%

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Biomarkers of chondrosarcoma

Jeong

Kim

2018

J Clin Pathol

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Clinical outcome prediction is major concern to patients with cancer. Various molecular markers in various carcinomas have been identified in the past few decades. However, accurate predictors in chondrosarcoma have not been developed, even though chondrosarcoma is the second most common primary bone tumour. Chondrosarcoma is the cartilage-forming malignancy and shows a wide spectrum of clinicopathological behaviours. The majority of chondrosarcoma grows slowly and rarely metastasises, and adequate surgery leads to a good prognosis. However, wide surgical excision is acquired in high-grade chondrosarcoma, because this tumour is highly resistant to chemotherapy and radiotherapy. To decide best therapy, accurate diagnostic markers are also necessary in chondrosarcoma. It is reported that angiogenesis and lymphangiogenesis increase by chondrosarcoma staging, and they are promoted by leptin and adiponectin. Several microRNAs to regulate vascular endothelial growth factor (VEGF)-A and VEGF-C are also reported. Alpha-methylacyl-CoA racemase and periostin are proposed as new biomarkers for differential diagnosis of enchondroma and chondrosarcoma. This review summarises that chondrosarcoma diagnostic markers are currently reported.

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Metabolic profiling of serum in patients with cartilage tumours using ¹H‐NMR spectroscopy: A pilot study

López-Garrido

Bañuelos-Hernández

Pérez-Hernández

et al. 2019

Magnetic Reson in Chemistry

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Cartilage‐forming lesions include tumours that can vary in severity from benign enchondromas to high‐grade malignant chondrosarcomas. Chondrosarcoma is the second most frequent malignant bone tumour, accounting for 20–30% of all malignant bone neoplasms. Surgery is the standard treatment for cartilage tumours (CTs); however, their incidental diagnosis and the difficult differentiation of low‐grade lesions like chondrosarcoma grade I from benign entities like enchondroma are challenges for clinical management. In this sense, the search for circulating biomarkers for early detection and prognosis is an ongoing interest. Targeted metabolomics is a powerful tool that can propose potential biomarkers in biological fluids as well as help to discover disturbed metabolic pathways to reveal tumour pathogenesis. In this context, the aim of this study was to investigate the 1H nuclear magnetic resonance metabolomic serum profile of patients with CTs contrasted with healthy controls. Forty‐one metabolites were identified and quantified; the multivariate statistical methods principal component analysis and partial least squares discriminant analysis reveal a clear separation of the CT group, that is, the differential metabolites that were involved in two main metabolic pathways: the taurine and hypotaurine metabolism and synthesis and degradation of ketone bodies. Our results represent preliminary work for emergent serum‐based diagnostics or prognostic methods for patients with chondrogenic tumours.

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TGF-β signalling and PEG10 are mutually exclusive and inhibitory in chondrosarcoma cells

Cited by 16 publications

References 60 publications

PEG10 as an oncogene: expression regulatory mechanisms and role in tumor progression

PEG10 as an oncogene: expression regulatory mechanisms and role in tumor progression

Biomarkers of chondrosarcoma

Metabolic profiling of serum in patients with cartilage tumours using ¹H‐NMR spectroscopy: A pilot study

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TGF-β signalling and PEG10 are mutually exclusive and inhibitory in chondrosarcoma cells

Cited by 16 publications

References 60 publications

PEG10 as an oncogene: expression regulatory mechanisms and role in tumor progression

PEG10 as an oncogene: expression regulatory mechanisms and role in tumor progression

Biomarkers of chondrosarcoma

Metabolic profiling of serum in patients with cartilage tumours using 1H‐NMR spectroscopy: A pilot study

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Product

Resources

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Metabolic profiling of serum in patients with cartilage tumours using ¹H‐NMR spectroscopy: A pilot study