Abstract:Transcription factor SRY-box 9 (SOX9) is a key regulator of chondrocyte differentiation and sex determination, and it is also involved in the progression of various types of human cancer. However, its putative association with oral squamous cell carcinoma (OSCC) remains elusive. The aim of the present study was to investigate the expression profiles of SOX9 in various oral epithelial lesions, including OSCC. We performed immunohistochemical analysis of SOX9 expression in surgical specimens of OSCC, which simul… Show more
“…The presence of α-SMA-positive CAFs in the cancer stroma was significantly correlated with the score of the mode of invasion ( p < 0.01), SOX9 positivity in cancer nests ( p < 0.01) and regional recurrence ( p < 0.05). Moreover, as previously shown [18] , high expression of SOX9 was also associated with regional recurrence ( p < 0.05) (data not shown). In the survival analysis, the presence of α-SMA-positive CAFs was significantly correlated with relapse-free survival ( p < 0.01), but was not significantly correlated with disease-specific survival ( p = 0.06) ( Fig.…”
Section: Resultssupporting
confidence: 81%
“…Antibodies and reagents [26] , immunofluorescence [18] , TGF-β1 enzyme-linked immunosorbent assay (ELISA), 2D migration assay, MTT cell viability assay, western blot analysis [27] , siRNA transfection, evaluation of the depth of invasion and invasion index in 3D cancer-CAF and cancer-NOF models [28] , xenograft models, immunohistochemistry and evaluation of the localisation of CAFs and SOX9 expression in surgical specimens were available in the supplementary materials and methods.…”
Section: Methodsmentioning
confidence: 99%
“…Both the high density of macrophages and SOX9 expression are associated with poor prognosis [15] . We recently conducted a histological investigation of SOX9 expression levels in patients with OSCC and demonstrated a correlation between SOX9 expression and poor clinical outcomes [18] . However, the interaction between CAFs and cancer cells through the TGF-β/SOX9 axis has not been thoroughly investigated, especially in OSCC.…”
Highlights
TGF-β1 secreted from CAFs promote the migration and invasion of OSCC cells.
CAFs upregulate SOX9 expression of OSCC cells, possibly through inducing EMT.
The presence of CAFs is correlated with SOX9 expression in the invasive cancer nests.
The TGF-β/SOX9 axis between CAFs and OSCC cells facilitates cancer progression.
Targeting the TGF-β/SOX9 axis could be a potential novel target for OSCC.
“…The presence of α-SMA-positive CAFs in the cancer stroma was significantly correlated with the score of the mode of invasion ( p < 0.01), SOX9 positivity in cancer nests ( p < 0.01) and regional recurrence ( p < 0.05). Moreover, as previously shown [18] , high expression of SOX9 was also associated with regional recurrence ( p < 0.05) (data not shown). In the survival analysis, the presence of α-SMA-positive CAFs was significantly correlated with relapse-free survival ( p < 0.01), but was not significantly correlated with disease-specific survival ( p = 0.06) ( Fig.…”
Section: Resultssupporting
confidence: 81%
“…Antibodies and reagents [26] , immunofluorescence [18] , TGF-β1 enzyme-linked immunosorbent assay (ELISA), 2D migration assay, MTT cell viability assay, western blot analysis [27] , siRNA transfection, evaluation of the depth of invasion and invasion index in 3D cancer-CAF and cancer-NOF models [28] , xenograft models, immunohistochemistry and evaluation of the localisation of CAFs and SOX9 expression in surgical specimens were available in the supplementary materials and methods.…”
Section: Methodsmentioning
confidence: 99%
“…Both the high density of macrophages and SOX9 expression are associated with poor prognosis [15] . We recently conducted a histological investigation of SOX9 expression levels in patients with OSCC and demonstrated a correlation between SOX9 expression and poor clinical outcomes [18] . However, the interaction between CAFs and cancer cells through the TGF-β/SOX9 axis has not been thoroughly investigated, especially in OSCC.…”
Highlights
TGF-β1 secreted from CAFs promote the migration and invasion of OSCC cells.
CAFs upregulate SOX9 expression of OSCC cells, possibly through inducing EMT.
The presence of CAFs is correlated with SOX9 expression in the invasive cancer nests.
The TGF-β/SOX9 axis between CAFs and OSCC cells facilitates cancer progression.
Targeting the TGF-β/SOX9 axis could be a potential novel target for OSCC.
“…SOX proteins may either maintain or antagonize tumorigenesis 38 – 42 . Cytoplasmic SOX9 correlates with poor clinical cancer outcomes, including both shorter disease-specific survival and relapse-free survival 19 . SOX9 is localized in the cytoplasm of 25–30% invasive ductal carcinomas and lymph node metastases, and its cytoplasmic accumulation significantly correlates with enhanced proliferation in breast tumors 43 .…”
Section: Discussionmentioning
confidence: 99%
“…This arrangement is conserved across all SOX family members (Fig. 1 ), and mutations within these regions can impair nuclear localization, cause severe developmental disease, and are associated with poor prognosis in cancer 9 , 16 – 19 (see also “Abstract” section). Fig.…”
SOX (SRY-related HMG-box) transcription factors perform critical functions in development and cell differentiation. These roles depend on precise nuclear trafficking, with mutations in the nuclear targeting regions causing developmental diseases and a range of cancers. SOX protein nuclear localization is proposed to be mediated by two nuclear localization signals (NLSs) positioned within the extremities of the DNA-binding HMG-box domain and, although mutations within either cause disease, the mechanistic basis has remained unclear. Unexpectedly, we find here that these two distantly positioned NLSs of SOX2 contribute to a contiguous interface spanning 9 of the 10 ARM domains on the nuclear import adapter IMPα3. We identify key binding determinants and show this interface is critical for neural stem cell maintenance and for Drosophila development. Moreover, we identify a structural basis for the preference of SOX2 binding to IMPα3. In addition to defining the structural basis for SOX protein localization, these results provide a platform for understanding how mutations and post-translational modifications within these regions may modulate nuclear localization and result in clinical disease, and also how other proteins containing multiple NLSs may bind IMPα through an extended recognition interface.
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