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Gynecologic Oncology | 2014

Preoperative genetic testing affects surgical decision-making in breast cancer patients

Elizabeth Lokich; Ashley Stuckey; Christina Raker; Jennifer Scalia Wilbur; Jessica Laprise; Jennifer Gass

OBJECTIVES Our aim was to determine if BRCA mutation status changes surgical decision making in women who undergo genetic testing after the diagnosis of breast cancer. METHODS This is a retrospective cohort study of breast cancer patients who had BRCA mutation testing performed prior to surgery. We compared surgical choice and change in surgical choice in women who tested positive for a BRCA mutation with those who tested negative. Surgery was considered the most definitive surgery within a year of diagnosis. Other data collected included age, race, stage, histology, receptor status, adjuvant treatment, gravity, parity, and family history. Variables were compared by BRCA status using Fishers exact test and logistic regression. RESULTS Three hundred and two women were included. Thirty-two (10.6%) were identified as carrying a BRCA mutation. Most women had early stage disease (55.6% T1 lesions, 72.8% node negative); 55.6% had breast-conserving surgery, and the remaining had unilateral or bilateral mastectomy. BRCA mutation carriers were more likely to have both a personal history of breast cancer (RR 2.74, 95% CI=1.08-6.98) and hormone receptor-negative tumors (56.0% vs. 26.2%, p=0.002). BRCA mutation carriers were more likely to choose bilateral mastectomy with reconstruction (56.3% vs. 15.9%, p<0.0001); 71.9% of BRCA mutation carriers opted for a different surgery than what was initially planned by their surgeon as compared to 29% of mutation-negative patients (p<0.0001). CONCLUSIONS BRCA mutation testing strongly influences surgical decision making in newly diagnosed breast cancer patients. For women who meet NCCN referral guidelines, genetic evaluation should be performed prior to surgical intervention.


Scientific Reports | 2015

HE4 expression is associated with hormonal elements and mediated by importin-dependent nuclear translocation

Elizabeth Lokich; Rakesh K. Singh; Alex Han; Nicole Romano; Naohiro Yano; Kyu Kwang Kim; Richard G. Moore

Antiestrogens including tamoxifen and fulvestrant have been evaluated as chemotherapeutics for ovarian cancer, particularly in cases of platinum resistant disease. Human epididymis protein 4 (HE4) is highly overexpressed in women with ovarian cancer and overexpression of HE4 has been found to correlate with platinum resistance. However, the role of HE4 in modulating responses to hormones and hormonal therapy has not been characterized in ovarian cancer. Here we demonstrate that 17β-estradiol, tamoxifen, and fulvestrant induce nuclear and nucleolar translocation of HE4 and that HE4 overexpression induces resistance to antiestrogens. HE4 was found to interact with estrogen receptor-α (ER-α), and HE4 overexpression resulted in ER-α downregulation in vitro and in human ovarian cancers. We identified a novel role for importin-4 in governing the nuclear transport of HE4. Treatment with ivermectin, an importin inhibitor, blocked HE4/importin-4 nuclear accumulation and sensitized HE4-overexpressing ovarian cancer cells to fulvestrant and tamoxifen.


Gynecologic Oncology | 2015

Assessing the risk of ovarian malignancy algorithm for the conservative management of women with a pelvic mass.

Elizabeth Lokich; M. Palisoul; Nicole Romano; M. Craig Miller; Katina Robison; Ashley Stuckey; Paul DiSilvestro; Cara Mathews; C.O. Granai; Geralyn Lambert-Messerlian; Richard G. Moore

OBJECTIVE To evaluate the use of as an aid in the identification of women who can safely undergo conservative, non-surgical management. METHODS All patients referred to the Program in Womens Oncology for surgery with a pelvic mass are evaluated at a prospective multidisciplinary tumor board (TB) where ROMA and imaging are used for management recommendations. This study evaluated women presented to TB with a pelvic mass between 2009 and 2013 who had either surgical or conservative management. RESULTS Of the 498 patients assessed, 392 (79%) had benign disease, 22 (4%) had LMP tumors, 28 (6%) had stage I-II epithelial ovarian cancer (EOC), 36 (7%) had stage III-IV EOC and 20 (4%) had non-EOC. Using clinical assessment in conjunction with ROMA, the TB recommended observation in 188 (37.8%) women. All patients diagnosed with an invasive malignancy were recommended for surgery by the TB. In the 315 patients managed surgically, 212 were found to have benign disease and 84 women were diagnosed with an invasive malignancy. The sensitivity for the initial TB recommendations using ROMA in conjunction with clinical judgment for detecting malignancy was 100% with a specificity of 47.7% and a NPV of 100%. When including low malignant potential tumors the sensitivity was 99.1%. For stage I-IV EOC ROMA alone had a sensitivity of 95.3%. CONCLUSIONS ROMA in conjunction with clinical assessment can safely identify women for conservative management.


Scientific Reports | 2015

Tetrathiomolybdate mediates cisplatin-induced p38 signaling and EGFR degradation and enhances response to cisplatin therapy in gynecologic cancers

Kyu Kwang Kim; Alex Han; Naohiro Yano; Jennifer R. Ribeiro; Elizabeth Lokich; Rakesh K. Singh; Richard G. Moore

Cisplatin and its analogs are among the most widely used chemotherapeutic agents against various types of cancer. It is known that cisplatin can activate epidermal growth factor receptor (EGFR), which may provide a survival benefit in cancers. Tetrathiomolybdate (TM) is a potent anti-cancer and anti-angiogenic agent and has been investigated in a number of clinical trials for cancer. In this study, we explore the therapeutic potential of TM on cisplatin-mediated EGFR regulation. Our study shows that TM is not cytotoxic, but exerts an anti-proliferative effect in ECC-1 cells. However, TM treatment prior to cisplatin markedly improves cisplatin-induced cytotoxicity. TM suppressed cisplatin-induced activation of EGFR while potentiating activation of p38; the activation of p38 signaling appeared to promote cisplatin-induced EGFR degradation. These results are in contrast to what we saw when cells were co-treated with cisplatin plus an EGFR tyrosine kinase inhibitor, where receptor activation was inhibited but receptor degradation was also blocked. Our current study is in agreement with previous findings that TM may have a therapeutic benefit by inhibiting EGFR activation. We furthermore provide evidence that TM may provide an additional benefit by potentiating p38 activation following cisplatin treatment, which may in turn promote receptor degradation by cisplatin.


Gynecologic Oncology | 2015

Isolated Inguinal Node Recurrences of Ovarian Cancer: A Case Series Study

Jenna Emerson; Kristin Rojas; Elizabeth Lokich; C.O. Granai; Katina Robison


American Journal of Obstetrics and Gynecology | 2018

While women await surgery for type I endometrial cancer, depot medroxyprogesterone acetate reduces tumor glandular cellularity

Stephen Fiascone; Valery A. Danilack; Mary J. Kao; Michael Cohen; Kamaljeet Singh; Elizabeth T. Kalife; Christine Luis; Elizabeth Lokich; Paul DiSilvestro; Katina Robison


American Journal of Obstetrics and Gynecology | 2016

Cancer of the uterus and treatment of stress incontinence: a pilot study

Katina Robison; Elizabeth Lokich; Sonali Raman; Christine Luis; Christina Raker; Melissa A. Clark; Kyle Wohlrab


Gynecologic Oncology | 2015

HE4-targeted antisense phosphorothioligos mitigate cisplatin resistance in epithelial ovarian cancer

Elizabeth Lokich; Emily K. Hill; Alex Han; Nicole Romano; Naohiro Yano; Kyu Kwang Kim; Ginny Hovanessian; Rakesh K. Singh; Richard G. Moore


Gynecologic Oncology | 2015

47 — Focused PlenaryROMA guided conservative management for women diagnosed with an ovarian cyst or pelvic mass

Elizabeth Lokich; M. Palisoul; Nicole Romano; Ashley Stuckey; Katina Robison; Paul DiSilvestro; Cara Mathews; M.C. Miller; C.O. Granai; Richard G. Moore


Gynecologic Oncology | 2015

ROMA guided conservative management for women diagnosed with an ovarian cyst or pelvic mass

Elizabeth Lokich; M. Palisoul; Nicole Romano; Christina Raker; C. Miller; Katina Robison; Ashley Stuckey; Carolyn K. McCourt; Paul DiSilvestro; Cara Mathews; C.O. Granai; Richard G. Moore

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