Abstract
BackgroundFolate receptor alpha (FOLR1/FRA) is expressed in a number of epithelial cancers and in particular epithelial ovarian cancer (EOC), especially of the serous histotype. Recent studies have shown that EOC originates from the fallopian tube fimbriae rather than from epithelial cells lining the ovary. We have previously shown by immunohistochemistry a strong correlation between FRA expression in EOC and normal and fallopian adenocarcinoma. Folate receptor beta (FOLR2/FRB) has been described to be expressed by macrophages both in inflammatory disorders and certain epithelial cancers. Given the high sequence identity of these two folate receptor family members we sought to investigate the architectural and cell-specific expression of these two receptors in gynecologic tissues.MethodsRNA scope, a novel chromogenic in situ hybridization assay tool, was used to examine expression of the alpha (FOLR1) and beta (FOLR2) isoforms of folate receptor relative to each other as well as to the macrophage markers CD11b and CD68, in samples of normal fallopian tube and fallopian adenocarcinoma as well as normal ovary and EOC.ResultsWe demonstrated expression of both FOLR1 and FOLR2 in EOC, normal fallopian tube and fallopian adenocarcinoma tissue while very little expression of either marker was observed in normal ovary. Furthermore, FOLR2 was shown to be expressed almost exclusively in macrophages, of both the M1 and M2 lineages, as determined by co-expression of CD11b and/or CD68, with little or no expression in epithelial cells.ConclusionsThese findings further substantiate the hypothesis that the cell of origin of EOC is tubal epithelium and that the beta isoform of folate receptor is primarily restricted to macrophages. Further, macrophages expressing FOLR2 may represent tumor associated or infiltrating macrophages (TAMs) in epithelial cancers.
Highlights
Folate receptor alpha (FOLR1/folate receptor alpha (FRA)) is expressed in a number of epithelial cancers and in particular epithelial ovarian cancer (EOC), especially of the serous histotype
FOLR1 expression in fallopian tube adenocarcinoma appeared more highly expressed relative to normal fallopian tube, suggesting the potential of increased expression of FOLR1 mRNA (Fig. 2d)
Epithelial cells of both fallopian adenocarcinoma and EOC showed high levels of FOLR1 expression. These data are consistent with previous studies, using both immunohistochemistry [13] and global RNA expression analyses [14], and support the contention that FRA is normally expressed in fallopian tube, but not ovary, and that EOC derives from fallopian fimbriae
Summary
Folate receptor alpha (FOLR1/FRA) is expressed in a number of epithelial cancers and in particular epithelial ovarian cancer (EOC), especially of the serous histotype. Recent studies have shown that EOC originates from the fallopian tube fimbriae rather than from epithelial cells lining the ovary. We have previously shown by immunohistochemistry a strong correlation between FRA expression in EOC and normal and fallopian adenocarcinoma. Folate receptor beta (FOLR2/FRB) has been described to be expressed by macrophages both in inflammatory disorders and certain epithelial cancers. It was previously thought that epithelial ovarian cancer (EOC) derived from epithelial cells covering the ovary [5, 6]. Recent studies have shown that most EOCs do not exhibit characteristics typical of mesodermal epithelium from which the ovaries develop. The tubal epithelium, along with other reproductive organs, derives from the müllerian duct, which in turn is derived from the mesoderm
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