| Literature DB >> 31057614 |
Maribel Aguilar-Medina1, Mariana Avendaño-Félix1, Erik Lizárraga-Verdugo1, Mercedes Bermúdez1, José Geovanni Romero-Quintana1, Rosalío Ramos-Payan1, Erika Ruíz-García2, César López-Camarillo3.
Abstract
Transcriptional and epigenetic embryonic programs can be reactivated in cancer cells. As result, a specific subset of undifferentiated cells with stem-cells properties emerges and drives tumorigenesis. Recent findings have shown that ectoderm- and endoderm-derived tissues continue expressing stem-cells related transcription factors of the SOX-family of proteins such as SOX2 and SOX9 which have been implicated in the presence of cancer stem-like cells (CSCs) in tumors. Currently, there is enough evidence suggesting an oncogenic role for SOX9 in different types of human cancers. This review provides a summary of the current knowledge about the involvement of SOX9 in development and progression of cancer. Understanding the functional roles of SOX9 and clinical relevance is crucial for developing novel treatments targeting CSCs in cancer.Entities:
Year: 2019 PMID: 31057614 PMCID: PMC6463569 DOI: 10.1155/2019/6754040
Source DB: PubMed Journal: J Oncol ISSN: 1687-8450 Impact factor: 4.375
SOX9 expression and functions in human cancers.
| Type of cancer | Status of SOX9 | Sox9 participation | References |
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| Hepatocellular carcinoma | overexpression | Related whit poor prognosis | [ |
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| Breast cancer | overexpression | Promotes proliferation, tumorigenesis and metastasis Related with poor overall survival | [ |
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| Bladder cancer | overexpression | Promotes tumorigenesis | [ |
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| Gastric cancer | overexpression | Promotes chemoresistance | [ |
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| Prostate cancer | overexpression | Promotes cell proliferation and apoptosis resistance | [ |
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| Prostate cancer | downregulation | Promotes metastasis | [ |
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| Ovarian cancer | overexpression | Its coexpression with HIF-2 | [ |
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| Pancreatic cancer | overexpression | Promotes chemoresistance | [ |
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| colorectal cancer | overexpression | Promotes cell proliferation, senescence inhibition and chemoresistance | [ |
Sox9 is expressed during premalignant and malignant lesions in pancreatic cancer.
| Lesions | Model | Status of SOX9 | Effects | References |
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| Acinar-to-ductal metaplasia | Mice | Overexpressed | HNF6 induces Sox9 expression, which is characteristic of ADM in humans | [ |
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| Acinar-to-ductal metaplasia | Mice | Overexpressed | Aberrant expression of p27 induces the nuclear expression of Sox9 | [ |
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| Mucinous cystic neoplasias, intraductal papillary mucinous neoplasias, pancreatic intraepithelial neoplasias and pancreatic ductal adenocarcinoma | Mice | Overexpressed | SOX9 and Kras co-expression is associated with PDAC initiation | [ |
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| Pancreatic ductal adenocarcinoma | 88 tumors samples of PDAC | Overexpressed | Sox9 and p-Akt double-positive expression is related with an unfavorable prognosis, high TNM and distant metastasis | [ |
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| Pancreatic ductal adenocarcinoma | Patient-derived tumor organoids with PDAC | Overexpressed in cytoplasm | High expression of Sox9 in cytoplasm is related with a poor DFS, OS, higher tumor grade and worse disease-specific survival compared to patients with nuclear Sox9 expression | [ |
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| Pancreatic cancer | PANC1 and HPAC cell lines of pancreatic cancer | Overexpressed | Sox9 is highly expressed in pancreatic CSCs. Moreover, NF- | [ |
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| Pancreatic ductal adenocarcinoma | HD3 colon cancer cells | Overexpressed | ST6Gal-I induces expression of Sox9, promoting stem-like cell properties | [ |
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| Pancreatic cancer | PANC-1, Capan-1, BxPC-3, MiaPaCa-2 cell lines of pancreatic cancer | Expression depending on chemoresistance | High level of Sox9 is related to stronger chemoresistance to Gemcitabine | [ |
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| Pancreatic ductal adenocarcinoma | HPDE cell line of PDAC | Overexpressed | GLI1 induces the transcription of Sox9 promoting stem cell properties | [ |
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| Pancreatic cancer | PANC1 cell line of pancreatic cancer | Downregulated | Induction of EMT with TGF- | [ |
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| Pancreatic cancer | Mice | Overexpressed | p53-/- mice enhanced sphere formation, increased expression of the stemness regulator Bmi1 and Klf4, and pancreatic multipotent progenitor markers as Ptf1a, Pdx1, Cpa1, c-myc, Hnf1b and Sox9 | [ |
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| Pancreatic cancer | FG and L3.6pl cell lines of pancreatic cancer under hypoxia | Overexpressed | Under hypoxia conditions, FG cell line expresses high levels of Sox9 and L3.6pl. Besides, WNT, CXCR4, retinoic acid, and FAK signaling pathways are regulated by Sox9 in L3.6pI | [ |
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| Pancreatic ductal adenocarcinoma and anaplastic pancreatic cancer | 6 APC patients and 53 PDAC patients | Overexpressed | PDAC and APC have high expression of Sox9, being the expression of proteins related with CSCs and EMT process higher in APC samples than PDAC | [ |
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| Intraductal papillary mucinous neoplasm | 19 IPMN cases | Overexpressed | SOX9-positive cells were confined to the lower portions of the papillary structures of IPMN | [ |
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| Solid pseudopapillary tumor | 8 samples of SPT | Overexpressed | PDX1 and Sox9 are both expressed in the cytoplasm of SPT cell | [ |
Figure 1MiniSOX9 has an oncogenic behavior in CRC. (a) In normal conditions canonical Wnt/β-catenin pathway triggers SOX9 expression resulting in regulation of differentiation and homeostasis in intestinal epithelium. (b) Truncated version of SOX9, MiniSOX9, accumulates in the nucleus to inhibit SOX9 DNA-binding-dependent transcriptional activity and PKC-alpha expression.
SOX9 roles in CRC as oncogene and tumor suppressor.
| Model | Status of SOX9 | Effects | References |
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| 353 tumors samples of CRC | SOX9 mutated and WT are overexpressed | Truncating SOX9 mutations are associated with SOX9 overexpression, KRAS mutation, and TP53 wild type | [ |
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| DLD-1 cell line of CRC | Loss of SOX9 transcriptional activity by L142P mutation | Restoration of wild type SOX9 expression inhibits cell growth, clonal capacity and colonosphere formation; besides, the expression of the c-MYC and the activity of Wnt/ß-catenin signaling pathway are affected | [ |
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| 17 tumors samples of CRC | High levels of SOX9 and MiniSOX9 | Overexpression of MiniSOx9 is found in CCR tissues whereas SOX9 is also expressed in normal and adjacent tissues | [ |
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| 188 tumors samples of CRC from Chinese population | Overexpressed | Does not show significant correlation between SOX9 and | [ |
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| 144 primary tumors from patients diagnosed in stage II CRC | Downregulated | Low levels of SOX9 have been shown as an independent predictor of relapse in stage II colon cancer patients | [ |
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| 45 tumors samples of CRC from African Americans population | Hypermethylated | SOX9, GATA6, TET1, GLIS1, and FAT1 are differentially hypermethylated in APC-negative CRC | [ |
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| CaCo2, SW480, HCT116 and HT29 cell lines of CRC | Overexpressed | The synthetic PPAR | [ |
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| HT29 and HCT116 cell lines of CRC | Cofactor of NF-Y | SOX9 is necessary for the function of NF-Y in activating expression of cyclin B1, cyclin B2, cyclin dependent kinase 1 and topoisomerase II | [ |
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| HCT116, SW480, SW620, DLD-1 cell lines of CRC | Overexpressed | Sox9 promotes proliferation through FOXK2 | [ |
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| HCT116 cell line of CRC | Overexpressed | Sox9 promotes invasiveness and metastasis in CRC through S100P | [ |
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| CCD 841 CoN, DLD-1, HCT-116, and HT-29 cell lines of CRC under hypoxia | Overexpressed | Sox9 upregulates the expression of USP47 promoting EMT under hypoxia | [ |
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| SW620 and SW480 cell lines of CRC | Overexpressed | SOX9 mediates the acquisition and maintenance of CR-CSCs | [ |
Role of SOX9 and associated transcription factors in diverse types of cancer.
| Type of cancer | TF | Effects | References |
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| Breast cancer | SLUG (SNAI2) | Induction and maintenance of tumor initiating capacity in breast cancer cells | [ |
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| Breast cancer | TP53 | Increased proliferation | [ |
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| Pancreatic cancer | HNF6 (ONECUT1) | Produces ectopic expression of Sox9 in acinar cells converting them in ductal cells | [ |
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| Pancreatic cancer | NF- | NF- | [ |
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| Pancreatic cancer | GLI1 | Induces the transcription of SOX9 | [ |
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| Pancreatic cancer | PDX1 | Co-expressed in the cytoplasm with Sox9 in solid pseudopapillary tumors | [ |
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| Prostate cancer | AR | Downstream target of SOX9 | [ |
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| Prostate cancer | TCF4 | It is positively regulated by SOX9 | [ |
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| Prostate cancer | ZBTB7A (POKEMON) | It is lost in advance prostate cancer facilitating the oncogenic activity of SOX9 | [ |
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| Ovarian cancer | HIF2A (EPAS1) | Hif-2 | [ |
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| Colorectal cancer | TCF4 | Positively regulates SOX9 | [ |
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| Colorectal cancer | PPAR | In cell lines ligand-dependent PPAR | [ |
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| Colorectal cancer | NF-Y | SOX9 is necessary for the function of NF-Y in activating expression of cyclin B1, cyclin B2, cyclin dependent kinase 1 and topoisomerase II | [ |
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| Colorectal cancer | FOXK2 | Is a SOX9 target and promotes proliferation | [ |