4.7 Article

HE4 (WFDC2) Promotes Tumor Growth in Endometrial Cancer Cell Lines

Journal

INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES
Volume 14, Issue 3, Pages 6026-6043

Publisher

MDPI AG
DOI: 10.3390/ijms14036026

Keywords

endometrial cancer; human epididymis protein 4 (HE4); HE4 variant; proliferation; invasion; colony formation; tumorigenesis

Funding

  1. Career Development Program of NIH/NCI MD Anderson Uterine Cancer SPORE
  2. Distinguished Cancer Scholar Program of Georgia Cancer Coalition
  3. Research Supplement from Mercer University School of Medicine
  4. Fraternal Order Of Eagles Cancer Research Fellow, Mayo Cancer Center
  5. Mercer University Seed Grant
  6. The Robert and Debra First Fund
  7. Mary Kay Foundation
  8. Sandy Rollman Ovarian Cancer Foundation
  9. NIH [2P50 CA098258-06]

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HE4, also known as WFDC2, is a useful biomarker for ovarian cancer when either used alone or in combination with CA125. HE4 is also overexpressed in endometrial cancer (EC), but its function in cancer cells is not clear. In this study, we investigate the role of HE4 in EC progression. An HE4-overexpression system was established by cloning the HE4 prototypic mRNA variant (HE4-V0) into a eukaryotic expression vector. Following transfection, stable clones in two EC cell lines were selected. The effects of HE4 overexpression on cell growth and function were measured with the use of cell proliferation assay, matrigel invasion, and soft agar gel colony formation assays. HE4-induced cancer cell proliferation in vivo was examined in a mouse xenograft model. HE4 overexpression significantly enhanced EC cell proliferation, matrigel invasion, and colony formation in soft agar. Moreover, HE4 overexpression promoted tumor growth in the mouse xenograft model. HE4 overexpression enhanced several malignant phenotypes in cell culture and in a mouse model. These results are consistent with our previous observation that high levels of serum HE4 closely correlate with the stage, myometrial invasion and tumor size in patients with EC. This study provides evidence that HE4 overexpression directly impacts tumor progression in endometrial cancer.

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