Abstract
BackgroundHigh HOX gene expression has been described in many cancers, including oral squamous cell carcinoma and the functional roles of these genes are gradually being understood. The pattern of overexpression suggests that inhibition may be useful therapeutically. Inhibition of HOX protein binding to PBX cofactors by the use of synthetic peptides, such as HXR9, results in apoptosis in multiple cancers.MethodsActivity of the HOX-PBX inhibiting peptide HXR9 was tested in immortalised normal oral (NOK), potentially-malignant (PMOL) and squamous cell carcinoma (OSCC) cells, compared to the inactive peptide CXR9. Cytotoxicity was assessed by LDH assay. Expression of PBX1/2 and c-Fos was assessed by qPCR and western blotting. Apoptosis was assessed by Annexin-V assay.ResultsPMOL and OSCC cells expressed PBX1/2. HOX-PBX inhibition by HXR9 caused death of PMOL and OSCC cells, but not NOKs. HXR9 treatment resulted in apoptosis and increased expression of c-Fos in some cells, whereas CXR9 did not. A correlation was observed between HOX expression and resistance to HXR9.ConclusionInhibition of HOX-PBX interactions causes selective apoptosis of OSCC/PMOL, indicating selective toxicity that may be useful clinically.
Highlights
High HOX gene expression has been described in many cancers, including oral squamous cell carcinoma and the functional roles of these genes are gradually being understood
Their dysregulation has been implicated in the development of a variety of cancers [3,4,5], including oral squamous cell carcinoma (OSCC) and we have shown that these changes occur in cells from potentially malignant oral lesions (PMOLs) [6, 7]
PMOL and OSCC cells express PBX1 and PBX2 Investigation of PBX1 and PBX2 mRNA and protein expression in PMOL and OSSC cells demonstrated that all cell lines express both PBX1 and PBX2 (Fig. 1a and b)
Summary
High HOX gene expression has been described in many cancers, including oral squamous cell carcinoma and the functional roles of these genes are gradually being understood. The HOX proteins are an important family of transcription factors that control a wide array of functions in embryogenesis and the maintenance of normal tissue [1, 2]. Their dysregulation has been implicated in the development of a variety of cancers [3,4,5], including oral squamous cell carcinoma (OSCC) and we have shown that these changes occur in cells from potentially malignant oral lesions (PMOLs) [6, 7]. Recent studies have highlighted the therapeutic potential of inhibiting the interaction between HOX proteins and a common group. This project aimed to determine whether targeting HOX-PBX interactions has therapeutic potential in OSCCs and PMOLs by assessing the expression of PBX1 and PBX2 in PMOL and OSCC cells and investigating the effect of HOX-PBX inhibition on these cells and in normal oral keratinocytes.
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