Abstract
BackgroundWnt5A, which is a member of the non-transforming Wnt protein family, is implicated in inflammatory processes. It is also highly expressed by ovarian cancer cells. ROR2, which is a member of the Ror-family of receptor tyrosine kinases, acts as a receptor or co-receptor for Wnt5A. The Wnt5A–ROR2 signaling pathway plays essential roles in the migration and invasion of several types of tumor cell and influences their cell polarity. We investigated the modulation of Wnt5A–ROR2 by inflammatory mediators and its involvement in the migration of the human ovarian cancer cell line SKOV-3.MethodsSKOV-3 cells were treated with LPS (lipopolysaccharide), LTA (lipoteichoic acid) and recombinant human IL-6 alone or in combination with STAT3 inhibitor (S1155S31-201) or NF-kB inhibitor (BAY11-7082) for 4, 8, 12, 24 and 48 h. The Wnt5A and ROR2 expression levels were determined at the gene and protein levels. Cells were transfected with specific siRNA against Wnt5A in the absence or presence of human anti-ROR2 antibody and cell migration was assessed using transwells.ResultsThere was a strong downregulation of Wnt5A expression in the presence of STAT3 or NF-kB inhibitors. Cell stimulation with LTA or IL-6 for 8 h led to significantly increased levels of Wnt5A (5- and 3-fold higher, respectively). LPS, LTA or IL-6 treatment significantly increased ROR2 expression (2-fold after 48 h). LPS- or LTA-induced Wnt5A or ROR2 expression was abrogated in the presence of STAT3 inhibitor (p < 0.001). IL-6-induced Wnt5A expression was abrogated by both STAT3 and NF-kB inhibitors (p < 0.001). Although not significant, IL-6-induced ROR2 expression showed a modest decrease when STAT3 inhibitor was used. Moreover, cell migration was decreased by 80 % in siRNA Wnt5A-transfected cells in the presence of anti-human ROR2 antibody (p < 0.001).ConclusionsThis study revealed for the first time that inflammatory mediators modulate Wnt5A and ROR2 through NF-kB and STAT3 transcription factors and this may play a role in ovarian cancer cell migration. The results described here provide new insight into the role of the Wnt5A–ROR2 complex in ovarian cancer progression in relation to inflammation.
Highlights
Wingless-type MMTV integration site family member 5A (Wnt5A), which is a member of the non-transforming Wnt protein family, is implicated in inflammatory processes
Wnt5A and Receptor tyrosine kinase-like Orphan Receptor 2 (ROR2) expression are induced by LPS, lipoteichoic acid (LTA) and IL-6 To study the modulation of Wnt5A–ROR2 signaling by inflammatory mediators, cells were stimulated with LPS, LTA and IL-6 for 4, 8, 12, 24 and 48 h
Wnt5A–ROR2 expression is mediated by Nuclear Factor KappaB (NF-kB) and Signal Transducer and Activator of Transcription 3 (STAT3) signaling pathways NF-kB and STAT3 have been implicated in the regulation of Wnt5A transcription [17, 18]
Summary
Wnt5A, which is a member of the non-transforming Wnt protein family, is implicated in inflammatory processes. It is highly expressed by ovarian cancer cells. The Wnt5A–ROR2 signaling pathway plays essential roles in the migration and invasion of several types of tumor cell and influences their cell polarity. We investigated the modulation of Wnt5A–ROR2 by inflammatory mediators and its involvement in the migration of the human ovarian cancer cell line SKOV-3. It has been demonstrated that in addition to associations between inflammatory conditions and particular human tumors, there is a direct link between chronic inflammation and tumorigenesis, through activation of the NF-kB and STAT3 signaling pathways [3]
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