Abstract
BackgroundWe previously identified TrkB as an oncogene involved in promoting metastasis in endometrial carcinoma (EC). Here, we sought to delineate the effect of changes in TrkB expression on the global profile of microRNAs (miRNAs) in EC cells and further investigated the correlation between the expression of certain miRNA and TrkB in the clinicopathologic characteristics of EC patients.Methods and resultsUsing quantitative reverse transcription-PCR (qRT-PCR), we found that expression of TrkB mRNA has no significant difference in transcript levels between normal endometrium and EC cells captured by laser capture microdissection, while immunohistochemistry results demonstrated a markedly higher expression of TrkB protein in EC tissues. The microRNA array showed that ectopic overexpression and knockdown of TrkB expression caused global changes in miRNA expression in EC cells. qRT-PCR results showed that elevated TrkB repressed miR-204-5p expression in EC cells. Furthermore, immunoblotting assays revealed that TrkB overexpression in IshikawaTrkB cells noticeably increased JAK2 and STAT3 phosphorylation, which, however, was aborted by TrkB knockdown in HEC-1BshTrkB cells. Moreover, ChIP assays showed that phospho-STAT3 could directly bind to STAT3-binding sites near the TRPM3 promoter region upstream of miR-204-5p. Interestingly, using bioinformatics analysis and luciferase assays, we identified TrkB was a novel target of miR-204-5p. Functionally, the MTT assays, clonogenic and Transwell assays showed that miR-204-5p significantly suppressed the clonogenic growth, migration and invasion of EC cells. Furthermore, miR-204-5p also inhibited the growth of tumor xenografts bearing human EC cells. Importantly, we found lower miR-204-5p expression was associated with advanced FIGO stages, lymph node metastasis and probably a lower chance for survival in EC patients.ConclusionsThis study uncovers a new regulatory loop involving TrkB/miR-204-5p that is critical to the tumorigenesis of EC and proposes that reestablishment of miR-204-5p expression could be explored as a potential new therapeutic target for this disease.
Highlights
We previously identified tyrosine kinase B (TrkB) as an oncogene involved in promoting metastasis in endometrial carcinoma (EC)
This study uncovers a new regulatory loop involving TrkB/miR-204-5p that is critical to the tumorigenesis of EC and proposes that reestablishment of miR-204-5p expression could be explored as a potential new therapeutic target for this disease
TrkB overexpression is associated with global changes in miRNA expression in endometrial cancer cells We examined TrkB protein and messenger RNA (mRNA) expression in the normal endometrium and endometrial cancer tissues using laser capture microdissection (LCM)/quantitative reverse transcription polymerase chain reaction and immunohistochemistry
Summary
We previously identified TrkB as an oncogene involved in promoting metastasis in endometrial carcinoma (EC). Endometrial cancer was originally classified according to a dualistic model [3]. This model has been challenged because tumors seen in daily practice occasionally show overlapping or combined morphologic and molecular characteristics of both classification types or exhibit ambiguous features [4]. Myometrial invasion and lymph node metastasis are considered the most important prognostic factors [5]. For these processes to occur, epithelial tumor cells need to undergo an epithelial to mesenchymal transition (EMT) [6]. As an additional receptor tyrosine kinase, TrkB activates diverse downstream signaling cascades that induce cellular proliferation and pro-survival mechanisms through the AKT, STAT3 and MAPK signaling pathways [10,11]
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