CHFR and Paclitaxel Sensitivity of Ovarian Cancer

Author:

Wahner Hendrickson Andrea E.,Visscher Daniel W.,Hou Xiaonan,Goergen Krista M.,Atkinson Hunter J.,Beito Thomas G.,Negron Vivian,Lingle Wilma L.,Bruzek Amy K.,Hurley Rachel M.,Wagner Jill M.,Flatten Karen S.,Peterson Kevin L.,Schneider Paula A.,Larson Melissa C.,Maurer Matthew J.,Kalli Kimberly R.,Oberg Ann L.ORCID,Weroha S. John,Kaufmann Scott H.

Abstract

The poly(ADP-ribose) binding protein CHFR regulates cellular responses to mitotic stress. The deubiquitinase UBC13, which regulates CHFR levels, has been associated with better overall survival in paclitaxel-treated ovarian cancer. Despite the extensive use of taxanes in the treatment of ovarian cancer, little is known about expression of CHFR itself in this disease. In the present study, tissue microarrays containing ovarian carcinoma samples from 417 women who underwent initial surgical debulking were stained with anti-CHFR antibody and scored in a blinded fashion. CHFR levels, expressed as a modified H-score, were examined for association with histology, grade, time to progression (TTP) and overall survival (OS). In addition, patient-derived xenografts from 69 ovarian carcinoma patients were examined for CHFR expression and sensitivity to paclitaxel monotherapy. In clinical ovarian cancer specimens, CHFR expression was positively associated with serous histology (p = 0.0048), higher grade (p = 0.000014) and higher stage (p = 0.016). After correction for stage and debulking, there was no significant association between CHFR staining and overall survival (p = 0.62) or time to progression (p = 0.91) in patients with high grade serous cancers treated with platinum/taxane chemotherapy (N = 249). Likewise, no association between CHFR expression and paclitaxel sensitivity was observed in ovarian cancer PDXs treated with paclitaxel monotherapy. Accordingly, differences in CHFR expression are unlikely to play a major role in paclitaxel sensitivity of high grade serous ovarian cancer.

Funder

National Cancer Institute

Susan G. Komen Foundation

Publisher

MDPI AG

Subject

Cancer Research,Oncology

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