Reduced expression of SRY-box containing gene 17 correlates with an unfavorable melanoma patient survival
- Authors:
- Published online on: October 8, 2014 https://doi.org/10.3892/or.2014.3534
- Pages: 2571-2579
Abstract
Introduction
Melanoma is the most deadly form of skin cancer arising from the melanocytes in the skin epidermis. It is characterized by rapid tumor progression, metastasis and a poor prognosis (1). Although melanoma accounts for only 4% of all dermatological cancers, it is responsible for 80% of deaths from skin cancer; less than 10% of patients with metastatic melanoma survive for 5 years (1,2). The discovery and application of biomarkers, in conjunction with traditional cancer diagnosis, staging and prognosis, could be useful in improving early diagnosis, screening and subsequent management and treatment of melanoma patients (3–5). However, at present, reliable markers are still lacking and the prognosis of melanoma patients remains poor. Therefore, a better understanding of the regulating factors contributing to melanoma initiation, progression and metastasis is needed.
The Sox gene family was first identified by homology to the high mobility group (HMG) box of the sex-determining gene SRY (6). There are at least 30 members in the Sox family, which are expressed in various types of cells and tissues at different developmental stages (7). Sox17 encodes an HMG box transcription factor and has been demonstrated to play critical roles in the regulation of vascular development (8), differentiation of embryonic stem cells (9), hematopoietic development (10) and tumor progression (11,12).
Accumulating evidence indicates that activation of Wnt/β-catenin signaling is one of the direct causes of tumor development (13–15). The nuclear accumulation of β-catenin, a hallmark of Wnt activation, is particularly enhanced in the invasive front of tumors and metastasized colon cancer cells, suggesting that the activation of Wnt/β-catenin signaling is important for colon cancer progression (16). Notably, some research has demonstrated that Sox17 inhibits the canonical Wnt/β-catenin signaling in malignant tumors (10,11,17). Recombinant Sox17 not only promoted the level of the Wnt antagonist SFRP1, but also decreased the expression level of Wnt/Frizzled and endogenous β-catenin in HOG cells, leading to cell cycle exit and differentiation (10). On the other hand, Sox17 expression was found to be downregulated in colon cancer cells and Sox17 overexpression inhibited colon cancer cell proliferation and reduced the efficiency of colony formation (18). Other research has illustrated that Sox17 protects benign gastrointestinal tumors from malignant progression at an early stage of tumorigenesis and downregulation of Sox17 contributes to malignant progression through promotion of Wnt activity (19). These results suggest that Sox17 plays a tumor suppressor role in gastric and colorectal cancer development. However, to our knowledge, there is no report on the influence of Sox17 involvement in the biological regulation of human melanoma. Here, we investigated Sox17 expression in a large set of melanocytic lesions at different stages by tissue microarray, investigated the correlation of Sox17 expression to melanoma progression and determined its prognostic value in patients with melanoma.
The cyclin-dependent kinase (CDK) inhibitor p27, also known as Kip1, is an atypical tumor suppressor that regulates G0-S phase transitions and plays important roles in cell proliferation, motility and apoptosis (20). Reduced nuclear p27 expression is associated with a poor prognosis in several types of cancers (20,21). Our previous study also demonstrated that p27 expression is inversely associated with the survival of melanoma patients (22). Sox17-siRNA transfection of gastric cancer MKN45 cells led to observably increased expression of cyclin D1 while p27 expression was markedly decreased (12). Furthermore, p27 expression was found to be significantly induced in liver-specific β-catenin knockdown mice (23). Based on these findings, we further examined the correlation between Sox17 and p27 expression in melanoma biopsies and analyzed the combined effect of Sox17 and p27 expression in predicting patient outcome.
Materials and methods
Ethics statement
The use of human skin tissues in this study was approved by the Clinical Research Ethics Board of the University of British Columbia (24,25). The study was conducted according to the principles expressed in the Declaration of Helsinki.
Tissue microarray (TMA) construction
The collection of melanoma patient specimens and the construction of the TMA have been previously described (24,25). Briefly, formalin-fixed, paraffin-embedded tissues from 49 common acquired nevi, 100 dysplastic nevi, 402 primary melanomas and 162 metastatic melanomas were used for this TMA construction. All specimens were obtained from the 1990 to 2009 archives of the Department of Pathology, Vancouver General Hospital. The most representative tumor area was carefully selected and marked on the hematoxylin and eosin stained slides, and the TMAs were assembled using a tissue-array instrument (Beecher Instruments, Silver Spring, MD, USA). Due to loss of biopsy cores or insufficient tumor cells present in the cores, 33 common acquired nevi (CAN) which are prototypical benign melanocytic nevi, 59 dysplastic nevi, 291 primary melanomas, and 142 metastatic melanomas were able to be evaluated for Sox17 staining (Fig. 1).
Immunohistochemistry of TMA
Immunohistochemistry was performed as described previously (24,25). TMA slides were dewaxed at 55°C for 30 min and then washed with xylene. Tissues were rehydrated by a series of washes in 100, 95 and 80% ethanol, followed by two washes in distilled water. Antigen retrieval was performed by heating the samples at 95°C for 30 min in 10 mmol/l sodium citrate (pH 6.0). After inactivating the endogenous peroxidase by incubation in 3% H2O2 for 30 min and blocking with universal blocking serum for 30 min, the slides were incubated with a primary anti-Sox17 antibody (1:100; EMD Millipore Corporation, Billerica, MA, USA) at 4°C overnight. Negative controls were constructed by omitting the Sox17 antibody during the primary antibody incubation. The slides were then incubated with biotin-labeled secondary antibody and streptavidin-peroxidase for 30 min each, followed by developing with a diaminobenzidine substrate kit (DAB; Dako, Glostrup, Denmark) and counterstaining with hematoxylin.
Evaluation of immunostaining
Positive Sox17 immunostaining was identified as a brown nuclear color and graded according to both intensity and percentage of cells with positive staining to eliminate the heterogeneous staining pattern. The evaluation of Sox17 staining was carried out blindly by microscopic examination of the tissue sections by two observers (including one pathologist). Sox17 staining intensity was scored as 0, 1+, 2+ and 3+. The percentage of Sox17-positive cells was also scored into 4 categories: 1 (0–25%), 2 (26–50%), 3 (51–75%), and 4 (76–100%). On the basis of the immunoreactive score, the staining pattern was defined as: negative (0), weak (1–4), moderate (6–8) and strong (9–12). The optimal cutoff point for staining score was calculated using MedCalc software for Windows, version 12.5 (MedCalc Software, Ostend, Belgium). The best area under the ROC curves (AUC) was used to determine the optimal cutoff point of staining. Based on the optimal value of the cutoff points for the Sox17 scores that was identified as 4, we grouped negative and weak staining as low expression and moderate and strong staining as high expression. The correlation between Sox17 and p27 expression was studied in 374 melanoma samples which were common to the present study and the previously published study on the prognostic significance of p27 expression in melanoma (22).
Statistical analysis
Differences in the patient demographic and clinical characteristics and Sox17 expression were evaluated by Kruskal-Wallis test and Chi-square (χ2) test between patient subgroups. Survival time was calculated from the date of melanoma diagnosis to the date of death or last follow-up. The effect of Sox17 expression on overall and disease-specific survival was evaluated by Kaplan-Meier analysis and log-rank test. Univariate and multivariate Cox proportional hazard regression models were performed to estimate the hazard ratios (HRs) or adjusted HRs and their 95% confidential intervals (CIs). A P-value of <0.05 was considered to indicate a statistically significant result. SPSS version 16 (SPSS Inc., Chicago, IL, USA) software was used for all analyses.
Results
Sox17 expression is inversely correlated with melanoma progression
Sox17 staining was stronger in common acquired nevi and dysplastic nevi biopsies than that in the primary and metastatic melanoma cases (Fig. 2A). Kruskal-Wallis test on the Sox17 scoring pattern in the patient samples revealed that Sox17 expression was significantly decreased from common acquired nevi (mean 8.3) and dysplastic nevi (mean 7.9) to primary melanoma (mean 5.8) and to metastatic melanoma (mean 3.6) (n=551; P<0.0001; Fig. 2B). Furthermore, the Chi-square test revealed that the percentage of high Sox17 staining was significantly reduced in primary melanoma (60%) and metastatic melanoma (28%) compared to the common acquired nevi (88%) and dysplastic nevi (85%) (n=551; P=2.4×10−17; Fig. 2C).
Sox17 expression inversely correlates with American Joint Committee on Cancer (AJCC) stage, tumor thickness and ulceration
The Kruskal-Wallis test on the Sox17 scoring pattern in the melanoma samples revealed that Sox17 expression was significantly decreased from early stage (AJCC I and II; mean 5.9) to advanced stage (AJCC III and IV; mean 3.7) melanoma (P<0.0001, Fig. 3A). As shown in Fig. 3B and Table I, high expression of Sox17 was detected in 61% of melanomas at AJCC stage I and II compared to 28% of melanomas at AJCC III and IV (P=4.5×10−10), indicating that decreased Sox17 expression may play an important role in primary to metastatic melanoma transition. Next, we found that in primary melanoma, Sox17 expression was decreased in tumors with thickness >4.00 mm (mean 3.9), compared to melanomas with thickness ≤4.00 mm (mean 6.3) (P<0.0001, Fig. 3C). Moreover, high Sox17 expression was found in 66% of melanomas with thickness ≤4.00 mm, compared to 37% of tumors with thickness >4.00 mm (P=0.00004; Fig. 3D and Table I). Furthermore, Sox17 expression decreased in the melanomas with ulceration (mean 4.6), compared to the melanomas with no ulceration (mean 6.1) (P=0.003; Fig. 3E), which is consistent with the Chi-square test results that high Sox17 expression was found in 47% of melanomas with ulceration, compared to 63% of melanomas with no ulceration (P=0.03; Fig. 3F and Table I). Moreover, Sox17 expression was significantly different among the different subtypes of melanoma (P=0.00003; Table I). We did not find significant correlations between Sox17 expression and other variables (Table I).
Reduced Sox17 expression is associated with poor melanoma patient survival
In the 413 melanoma patients, Kaplan-Meier survival curve revealed that the patients with high Sox17 expression had a better overall and disease-specific 5-year survival than patients with low Sox17 expression (P=0.005 and 0.004, respectively; Fig. 4A). More meaningful, we further investigated whether Sox17 expression was associated with melanoma patient 10-year survival. We analyzed the 267 melanoma patients and found that the patients with high Sox17 expression also had a better overall and disease-specific 10-year survival than patients with low Sox17 expression (P=0.038 and 0.046, respectively; Fig. 4B).
Sox17 expression is an independent prognostic marker for melanoma
To further estimate the prognostic value of Sox17 expression in melanoma patients, univariate and multivariate Cox proportional hazard analyses were performed. When analyzed using univariate Cox regressive analysis, patients with high Sox17 expression had significantly better overall survival (HR, 0.65; 95% CI, 0.48–0.89; P=0.006) and disease-specific (HR, 0.63; 95% CI, 0.45–0.87; P=0.005; Table II) 5-year survival among the 413 melanoma patients. Concerning 10-year survival, univariate Cox regressive analysis further confirmed that patients with high Sox17 expression had significantly better overall survival (HR, 1.48; 95% CI, 1.02–2.14; P=0.04) and disease-specific (HR, 1.51; 95% CI, 1.00–2.28; P=0.05; Table II) 10-year survival in the 267 melanoma patients.
Table IIUnivariate and multivariate Cox regression analyses of the 5- or 10-year survival of the melanoma patients. |
Furthermore, multivariate Cox regressive analysis was carried out with age, gender and Sox17 expression together as the variables. The results indicated that Sox17 expression is an independent prognostic factor for both overall (HR, 1.52; 95% CI, 1.13–2.06; P=0.006) and disease-specific (HR, 1.59; 95% CI, 1.15–2.20; P=0.005; Table II) 5-year survival in the 413 melanoma patients. Concerning 10-year survival, multivariate Cox regressive analysis further demonstrated that Sox17 expression was also correlated with both overall (HR, 1.51; 95% CI, 1.04–2.19; P=0.03) and disease specific (HR, 1.54; 95% CI, 1.02–2.32; P=0.04; Table II) 10-year survival in the 267 melanoma patients.
Sox17 expression positively correlates with p27 expression, and their concomitant expression influences melanoma patient survival
Reduced p27 expression has been shown to be associated with increased invasion and unfavorable patient survival (20, 21). Since the TMA we used for Sox17 staining in this study was the same as that previously stained for p27 (22), we were able to analyze the correlation between Sox17 and p27 expression. As shown in Fig. 5A, high Sox17 was positively correlated with positive p27 expression (P=8.7×10−5). We then analyzed the effect of combined Sox17 and p27 expression on patient survival and found that patients with both high Sox17 and positive p27 expression showed a significantly increased 5-year overall and disease-specific survival, compared with the patients with other expression patterns of Sox17 and p27 using Kaplan-Meier survival curves (P=0.006 and 0.014, respectively; Fig. 5B). More meaningful, concerning 10-year survival, the analysis also demonstrated that a high Sox17 and positive p27 expression pattern exerted a more significant influence on melanoma patient survival (P=0.004 and 0.0003, respectively; Fig. 5C).
Discussion
A number of studies have demonstrated that Sox17 expression is downregulated in different types of human cancers and it appears to act as a tumor suppressor (17–19). However, a recent report demonstrated that Sox17 expressed in tumor endothelial cells promoted tumor angiogenesis and vascular destabilization by upregulation of VEGFR2 (26). To understand the role of Sox17 in melanoma progression, we used TMA technology and immunohistochemistry to investigate Sox17 expression in 525 cases of pigmented skin lesions at different stages.
Our results revealed that Sox17 expression was markedly decreased in primary melanoma when compared with the expression in common acquired nevi and dysplastic nevi and was further downregulated in metastatic melanoma compared with primary melanoma. This indicates that reduced Sox17 activity may have a relationship with the transformation from benign neoplasia to malignancy, as well as in tumor progression from primary to metastatic melanoma. This finding is consistent with previous research that found that Sox17 was rarely detected by immunohistochemistry in gastric and colon cancers, whereas strong nuclear staining of Sox17 was found in 70% of benign gastric and intestinal tumors (19). It is therefore conceivable that Sox17 protects benign tumors from malignant progression at an early stage of tumorigenesis, and downregulation of Sox17 contributes to malignant progression.
It was also reported that Sox17 methylation was found in 60.2% of primary human lung cancer samples. The promoter region methylation silenced the expression of Sox17, and re-expression of Sox17 inhibited Wnt signaling in lung cancer cells (27). The global analysis of CpG island hypermethylation and gene expression in colorectal cancer cell lines has revealed that Sox17 gene silencing is associated with DNA hypermethylation (18). Recent research demonstrated that loss of Sox17 expression is correlated to promoter region hypermethylation in esophageal cancer. Restoration of Sox17 expression suppresses TCF/β-catenin-dependent transcription and colony formation (28). Furthermore, Sox17 expression is often epigenetically silenced by DNA methylation in early gastric cancer and the introduction of Sox17 into cancer cells suppresses cancer cell growth (29).
In addition, we found that Sox17 expression was inversely correlated with AJCC stage, ulceration and tumor thickness (≤4.00 vs. >4.00 mm) of melanomas. A reflection of the intense metastatic propensity of melanomas is the fact that the metastatic potential is measured on a scale of millimeters, where a tumor thickness of 4.00 mm predicts a high risk of cancer dissemination and death (30). By constructing Kaplan-Meier survival curves, we found that reduced Sox17 was associated with the poor survival of melanoma patients and this correlation was further confirmed by univariate Cox regression analyses. Furthermore, after adjustment for age and gender in multivariate Cox regression models, the analysis further indicated that Sox17 expression is an independent prognostic marker for melanoma patients. To our knowledge, this is the first study to reveal the prognostic value of Sox17 expression in tumor patients by TMA technology.
p27, a cell-cycle inhibitory molecule, inhibits the catalytic activity of CDK4. Increased levels of the p27 protein typically cause cells to arrest in the G1 phase of the cell cycle (20). It has been reported that Sox17 overexpression in human colon cancer cell lines suppressed the hyperactive β-catenin activity as well as reduced cyclin D1 expression and repressed cell proliferation (18,31). Colony formation assays revealed that Sox17 suppressed lung cancer cell proliferation (27). Sox17 knockdown in gastric cancer cells enhanced cyclin D1 expression levels and reduced p27 expression levels (12). The expression of Sox17 and p27 increased in parallel before myelin basic protein expression in oligodendrocytes (32). In addition, it has been demonstrated that reduced nuclear p27 expression is associated with a worse cancer patient survival (20–22).
Here, our results revealed that in 374 melanoma samples, melanomas which had high Sox17 expression also had a significantly higher percentage of positive p27 staining. Notably, patients with both high Sox17 and positive p27 expression had an extended 5- and 10-year overall and disease-specific survival as compared to patients with both low Sox17 and negative p27 expression. Based on this, we speculate that Sox17 may be a positive regulator of p27 and therefore, reduced Sox17 expression has an inhibitory effect on melanoma progression.
In conclusion, this study shows that Sox17 expression is significantly decreased in association with progression of human melanoma. Strikingly, reduced Sox17 expression correlates with a worse 5- and 10-year survival of melanoma patients and is an independent prognostic factor for melanoma patients. Moreover, there is a significant positive correlation between Sox17 and p27 expression in melanoma biopsies, and their concomitant reduced expression is inversely correlated with melanoma patient survival. These data suggest that Sox17 plays an important role in melanoma pathogenesis and it may serve as a promising prognostic marker for melanoma patients.
Acknowledgements
We acknowledge Dr Guangdi Chen for his previous research on p27. This study was supported by the Canadian Institutes of Health Research (CCI-117958), the Cancer Research Society and the Canadian Dermatology Foundation. Dr Jing Lu is supported by the National Natural Science Foundation of China (81101731).
References
Miller AJ and Mihm MC Jr: Melanoma. N Engl J Med. 355:51–65. 2006. View Article : Google Scholar | |
Trinh VA: Current management of metastatic melanoma. Am J Health Syst Pharm. 65:S3–S8. 2008. View Article : Google Scholar : PubMed/NCBI | |
Geller AC, Swetter SM, Brooks K, Demierre MF and Yaroch AL: Screening, early detection, and trends for melanoma: current status (2000–2006) and future directions. J Am Acad Dermatol. 57:555–576. 2007.PubMed/NCBI | |
Geller AC, Swetter SM, Oliveria S, Dusza S and Halpern AC: Reducing mortality in individuals at high risk for advanced melanoma through education and screening. J Am Acad Dermatol. 65:S87–S94. 2011. View Article : Google Scholar : PubMed/NCBI | |
Turner RM, Bell KJ, Morton RL, et al: Optimizing the frequency of follow-up visits for patients treated for localized primary cutaneous melanoma. J Clin Oncol. 29:4641–4646. 2011. View Article : Google Scholar : PubMed/NCBI | |
Gubbay J, Collignon J, Koopman P, et al: A gene mapping to the sex-determining region of the mouse Y chromosome is a member of a novel family of embryonically expressed genes. Nature. 346:245–250. 1990. View Article : Google Scholar : PubMed/NCBI | |
Wegner M: From head to toes: the multiple facets of Sox proteins. Nucleic Acids Res. 27:1409–1420. 1999. View Article : Google Scholar : PubMed/NCBI | |
Burtscher I, Barkey W, Schwarzfischer M, Theis FJ and Lickert H: The Sox17-mCherry fusion mouse line allows visualization of endoderm and vascular endothelial development. Genesis. 50:496–505. 2012. View Article : Google Scholar : PubMed/NCBI | |
Niakan KK, Ji H, Maehr R, et al: Sox17 promotes differentiation in mouse embryonic stem cells by directly regulating extraembryonic gene expression and indirectly antagonizing self-renewal. Genes Dev. 24:312–326. 2010. View Article : Google Scholar : PubMed/NCBI | |
Chen HL, Chew LJ, Packer RJ and Gallo V: Modulation of the Wnt/beta-catenin pathway in human oligodendroglioma cells by Sox17 regulates proliferation and differentiation. Cancer Lett. 335:361–371. 2013. View Article : Google Scholar : PubMed/NCBI | |
Jia Y, Yang Y, Liu S, Herman JG, Lu F and Guo M: SOX17 antagonizes WNT/β-catenin signaling pathway in hepatocellular carcinoma. Epigenetics. 5:743–749. 2010. | |
Ye YW, Wu JH, Wang CM, et al: Sox17 regulates proliferation and cell cycle during gastric cancer progression. Cancer Lett. 307:124–131. 2011. View Article : Google Scholar : PubMed/NCBI | |
Li D, Beisswenger C, Herr C, et al: Myeloid cell RelA/p65 promotes lung cancer proliferation through Wnt/β-catenin signaling in murine and human tumor cells. Oncogene. 33:1239–1248. 2013.PubMed/NCBI | |
Yang L, Chen Y, Cui T, et al: Desmoplakin acts as a tumor suppressor by inhibition of the Wnt/β-catenin signaling pathway in human lung cancer. Carcinogenesis. 33:1863–1870. 2012.PubMed/NCBI | |
Zeitlin BD, Ellis LM and Nor JE: Inhibition of vascular endothelial growth factor receptor-1/Wnt/{beta}-catenin crosstalk leads to tumor cell death. Clin Cancer Res. 15:7453–7455. 2009. View Article : Google Scholar : PubMed/NCBI | |
Fodde R and Brabletz T: Wnt/β-catenin signaling in cancer stemness and malignant behavior. Curr Opin Cell Biol. 19:150–158. 2007. | |
Fu DY, Wang ZM, Li C, et al: Sox17, the canonical Wnt antagonist, is epigenetically inactivated by promoter methylation in human breast cancer. Breast Cancer Res Treat. 119:601–612. 2010. View Article : Google Scholar : PubMed/NCBI | |
Zhang W, Glockner SC, Guo M, et al: Epigenetic inactivation of the canonical Wnt antagonist SRY-box containing gene 17 in colorectal cancer. Cancer Res. 68:2764–2772. 2008. View Article : Google Scholar : PubMed/NCBI | |
Du YC, Oshima H, Oguma K, et al: Induction and down-regulation of Sox17 and its possible roles during the course of gastrointestinal tumorigenesis. Gastroenterology. 137:1346–1357. 2009. View Article : Google Scholar : PubMed/NCBI | |
Chu IM, Hengst L and Slingerland JM: The Cdk inhibitor p27 in human cancer: prognostic potential and relevance to anticancer therapy. Nat Rev Cancer. 8:253–267. 2008. View Article : Google Scholar : PubMed/NCBI | |
Wander SA, Zhao D and Slingerland JM: p27: a barometer of signaling deregulation and potential predictor of response to targeted therapies. Clin Cancer Res. 17:12–18. 2011. View Article : Google Scholar : PubMed/NCBI | |
Chen G, Cheng Y, Zhang Z, Martinka M and Li G: Prognostic significance of cytoplasmic p27 expression in human melanoma. Cancer Epidemiol Biomarkers Prev. 20:2212–2221. 2011. View Article : Google Scholar : PubMed/NCBI | |
Tao GZ, Lehwald N, Jang KY, et al: Wnt/β-catenin signaling protects mouse liver against oxidative stress-induced apoptosis through the inhibition of forkhead transcription factor FoxO3. J Biol Chem. 288:17214–17224. 2013. | |
Dai DL, Martinka M and Li G: Prognostic significance of activated Akt expression in melanoma: a clinicopathologic study of 292 cases. J Clin Oncol. 23:1473–1482. 2005. View Article : Google Scholar : PubMed/NCBI | |
Lin H, Wong RP, Martinka M and Li G: Loss of SNF5 expression correlates with poor patient survival in melanoma. Clin Cancer Res. 15:6404–6411. 2009. View Article : Google Scholar : PubMed/NCBI | |
Yang H, Lee S, Kim K, et al: Sox17 promotes tumor angiogenesis and destabilizes tumor vessels in mice. J Clin Invest. 123:418–431. 2013. View Article : Google Scholar : PubMed/NCBI | |
Yin D, Jia Y, Yu Y, et al: SOX17 methylation inhibits its antagonism of Wnt signaling pathway in lung cancer. Discov Med. 14:33–40. 2012.PubMed/NCBI | |
Jia Y, Yang Y, Zhan Q, et al: Inhibition of SOX17 by microRNA 141 and methylation activates the WNT signaling pathway in esophageal cancer. J Mol Diagn. 14:577–585. 2012. View Article : Google Scholar : PubMed/NCBI | |
Oishi Y, Watanabe Y, Yoshida Y, et al: Hypermethylation of Sox17 gene is useful as a molecular diagnostic application in early gastric cancer. Tumour Biol. 33:383–393. 2012. View Article : Google Scholar : PubMed/NCBI | |
Tarhini AA and Agarwala SS: Cutaneous melanoma: available therapy for metastatic disease. Dermatol Ther. 19:19–25. 2006. View Article : Google Scholar : PubMed/NCBI | |
Sinner D, Kordich JJ, Spence JR, et al: Sox17 and Sox4 differentially regulate β-catenin/T-cell factor activity and proliferation of colon carcinoma cells. Mol Cell Biol. 27:7802–7815. 2007.PubMed/NCBI | |
Sohn J, Natale J, Chew LJ, et al: Identification of Sox17 as a transcription factor that regulates oligodendrocyte development. J Neurosci. 26:9722–9735. 2006. View Article : Google Scholar : PubMed/NCBI |