Abstract
Wnt5A signals through various receptors that confer versatile biological functions. Here, we used Wnt5A overexpressing human ovarian SKOV-3 and OVCAR-3 stable clones for assessing integrin expression, cell proliferation, migration, invasion, and the ability of multicellular aggregates (MCAs) formation. We found here, that Wnt5A regulates differently the expression of its receptors in the stable Wnt5A overexpressing clones. The expression levels of Frizzled (FZD)-2 and -5, were increased in different clones. However ROR-1, -2 expression levels were differently regulated in clones. Wnt5A overexpressing clones showed increased cell proliferation, migration, and clonogenicity. Moreover, Wnt5A overexpressing SKOV-3 clone showed increased MCAs formation ability. Cell invasion had been increased in OVCAR-3-derived clones, while this was decreased in SKOV-3-derived clone. Importantly, αv integrin expression levels were increased in all assessed clones, accompanied by increased cell attachment to fibronectin and focal adhesion kinase activity. Moreover, the treatment of clones with Box5 as a Wnt5A/FZD5 antagonist abrogates ITGAV increase, cell proliferation, migration, and their attachment to fibronectin. Accordingly, we observed significantly higher expression levels of ITGAV and ITGB3 in human high-grade serous ovarian cancer specimens and ITGAV correlated positively with Wnt5A in metastatic serous type ovarian cancer. In summary, we hypothesize here, that Wnt5A/FZD-5 signaling modulate αv integrin expression levels that could be associated with ovarian cancer cell proliferation, migration, and fibronectin attachment.
Highlights
Wnt5A signals through various receptors that confer versatile biological functions
C9/SKOV-3, C3/OVCAR-3, and C2/OVCAR-3 clones were transfected with siRNA against Wnt5A showed a reduction of Wnt5A at protein levels compared to scramble. (B,C) Wnt5A regulates its receptors as revealed by room temperature (RT)-qPCR analysis of frizzled-2 (FZD-2), frizzled-4 (FZD-4), frizzled-5 (FZD-5), ROR-1 and ROR-2 expression levels in C9/SKOV-3 and C3/OVCAR-3 clones in Wnt5A knock-down or Box[5] treated clones relative to mock or scrambled
Clone 9 in SKOV-3 cells named as C9/SKOV-3 clone and clone 3 in OVCAR-3 named as C3/OVCAR-3 clone with 4.5-fold increased Wnt5A expression levels (Fig. 1A, left, right and lower panel) and C2/OVCAR-3 clone cells with twofold increased levels of Wnt5A (Fig. 1, right and lower panels) were selected for further experiments
Summary
We used Wnt5A overexpressing human ovarian SKOV-3 and OVCAR-3 stable clones for assessing integrin expression, cell proliferation, migration, invasion, and the ability of multicellular aggregates (MCAs) formation. Wnt5A overexpressing clones showed increased cell proliferation, migration, and clonogenicity. The treatment of clones with Box[5] as a Wnt5A/FZD5 antagonist abrogates ITGAV increase, cell proliferation, migration, and their attachment to fibronectin. We hypothesize here, that Wnt5A/FZD-5 signaling modulate αv integrin expression levels that could be associated with ovarian cancer cell proliferation, migration, and fibronectin attachment. (B,C) Wnt5A regulates its receptors as revealed by RT-qPCR analysis of frizzled-2 (FZD-2), frizzled-4 (FZD-4), frizzled-5 (FZD-5), ROR-1 and ROR-2 expression levels in C9/SKOV-3 and C3/OVCAR-3 clones in Wnt5A knock-down or Box[5] treated clones relative to mock or scrambled (scr). Several studies demonstrated the importance of Wnt5A on cellto-substrate attachment in various cells and models 21–26, though; its exact molecular mechanism is still not understood
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