Open Journal of Obstetrics and Gynecology
Vol.3 No.9(2013), Article ID:39151,5 pages DOI:10.4236/ojog.2013.39119

Evaluation of the BRCA1/2 mutation as a prognostic marker in primary peritoneal serous cancer

Naoto Furukawa1*, Sumire Ohno1, Takahiko Kasai2, Sachiko Morioka1, Fuminori Ito1, Yasuhito Tanase1, Shoji Haruta1, Seiji Kanayama1, Ryuji Kawaguchi1, Shozo Yoshida1, Hiroshi Kobayashi1

1Department of Obstetrics and Gynecology, Nara Medical University, Kashihara, Japan

2Diagnostic Pathology, Nara Medical University, Kashihara, Japan

Email: *furunao0813@gmail.com

Copyright © 2013 Naoto Furukawa et al. This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

Received 2 October 2013; revised 30 October 2013; accepted 6 November 2013

Keywords: BRCA1; Primary Peritoneal Serous Cancer; Prognosis

ABSTRACT

Introduction: The present study was a retrospective investigation of the relation between immunohistochemical BRCA1/2 status and prognosis in patients with primary peritoneal serous cancer (PPSC). Materials and Methods: We retrospectively evaluated 14 consecutive patients diagnosed with PPSC other than hereditary breast and ovarian cancer between 2005 and 2010. All patients had serum CA125 levels >40 U/mL prior to starting first-line chemotherapy with paclitaxel and carboplatin. Paclitaxel was administered as a 3-hour intravenous infusion at a dose of 175 mg/m2 on day 1, and carboplatin was delivered at an area under the curve of 5 based on the Calvert method. Patients received six cycles of first-line chemotherapy, except patients whose disease was determined to be progressive during the chemotherapy regimen. BRCA1/2 and p53 protein expression was determined by immunohistochemistry of patient tissue samples. The Cox proportional hazards model was used to evaluate univariate and independent multivariate associations with the effect of clinical parameters, such as age at diagnosis; tumor histology; tumor grade; and rate of change in CA125, and BRCA1/2, p53 status on overall survival. Probability values of less than 0.05 were considered to indicate statistical significance. Results: Two cases (14%) had the BRCA1 mutation, and none had the BRCA2 mutation. Eleven cases (79%) were positive for p53. In the univariate analysis, factors significantly associated with overall survival were (pre-chemotherapy CA125-pre-2nd chemotherapy CA125)/pre-chemotherapy CA125 (p = 0.0034) and (pre-chemotherapy CA125-pre-3rd chemotherapy CA125)/pre-chemo- therapy CA125 (p = 0.0245). BRCA1 and p53 status were not predictors of overall survival. Multivariate analysis performed with overall survival as an endpoint revealed that none of the factors examined was significant. Median survival rate of patients without a BRCA1 mutation was 23.5 months (2 - 82 months), and all died. By contrast, one patient with a BRCA1 mutation remains alive at 85 months, and the other patient died at 64 months. Conclusion: BRCA1 might be a predictor of overall survival in patients with PPSC receiving chemotherapy.

1. INTRODUCTION

Ovarian cancer is increasing annually in Japan [1], and the total number of ovarian cancer cases in 2006 was 7913 [2]. Standard therapy for ovarian cancer comprises primary surgical cytoreduction followed by platinumbased chemotherapy, but 25% to 90% of cases of ovarian cancer are diagnosed during progression [3]. Paclitaxel and carboplatin as first line chemotherapy are administered to patients with ovarian cancer, and overall response rates of 59% [4] and 68% [5] are reported in studies in which paclitaxel (175 - 185 mg/m2) and carboplatin (area under the curve of 5 - 6) are administered every 3 weeks. Despite a favorable initial response rate to treatment, early recurrences and platinum resistance are frequently encountered. Several reports have discussed the diverse pathogenesis of ovarian cancers. Lowgrade serous carcinomas are associated with mutations in KRAS/BRAF and evolve slowly [6]. High-grade serous carcinomas are, in contrast, associated with mutations in p53, BRCA1, or BRCA2, and evolve rapidly [6,7]. BRCA1 and BRCA2 act as tumor suppressors involved in repairing double-strand DNA breaks by homologous recombination. BRCA1/2 germline mutations occur in 11% to 15.3% and BRCA1/2 somatic mutations occur in 19% of women with unselected ovarian cancers [8]. Patients with BRCA1 and BRCA2 mutations have increased sensitivity to platinum chemotherapy and a better prognosis [9]. Primary peritoneal serous carcinoma (PPSC) is histologically and clinically similar to stage III-IV ovarian high-grade serous carcinoma, and is rare. The frequency of BRCA1/2 germline mutations in PPSC is reported to be 15.8% [10]. Another group reported that germline-BRCA1 mutations are found in 26% of PPSC patients [11]. Few reports, however, describe the frequency of somatic mutations of BRCA1/2 in patients with PPSC, or the relation between BRCA1/2 status with chemosensitivity and prognosis in patients with PPSC. BRCA immunohistochemistry identifies BRCA mutations with a sensitivity of 80% and a specificity of 93%, suggesting that BRCA immunohistochemistry is a promising screening method for BRCA mutation detection [12].

In the present study, we retrospectively investigated the relation between immunohistochemical BRCA1/2 status and prognosis in patients with PPSC.

2. MATERIALS AND METHODS

2.1. Patient Selection

The present study was conducted in accordance with the principles of the Declaration of Helsinki. We retrospectively evaluated 14 consecutive patients diagnosed with PPSC (all stage IIIC) other than hereditary breast and ovarian cancer between 2005 and 2010. Genetic testing was not available during this period, however, so hereditary breast and ovarian cancer were diagnosed by asking patients detailed questions regarding family history. All patients underwent a laparotomy or laparoscopy to obtain a small tissue sample for examination under a microscope, but none of them underwent debulking surgery. Diagnostic criteria include normal sized ovaries; extraovarian site involvement greater than surface involvement of the ovary; an ovarian component of less than 5 × 5 mm within the ovary and otherwise confined to the surface of the ovary; and histologic characteristics predominantly of the serous type [13]. All patients had serum CA125 levels >40 U/mL prior to starting first-line chemotherapy with paclitaxel and carboplatin. Paclitaxel was administered as a 3-hour intravenous infusion at a dose of 175 mg/m2 on day 1, and carboplatin was delivered at an area under the curve of 5 based on the Calvert method. Patients received 6 cycles of first-line chemotherapy, except patients whose disease was determined to be progressing during the chemotherapy regimen. The retrieved clinical data included patient age at diagnosis, tumor histology, tumor grade, CA125, and overall survival from the medical records. Rates of change in CA125 were calculated as follows: (pre-chemotherapy CA125—pre-2nd chemotherapy CA125)/pre-chemotherapy CA125; and (pre-chemotherapy CA125—pre-3rd chemotherapy CA125)/pre-chemotherapy CA125. Prechemotherapy CA125 represents the CA125 level before administering the first dose of chemotherapy, Pre-2nd chemotherapy CA125 represents the CA125 level before administering the second dose of chemotherapy; and Pre- 3rd chemotherapy CA125 represents the CA125 level before administering the third dose of chemotherapy.

2.2. Immunohistochemistry

BRCA1/2 and p53 protein expression was determined by immunohistochemistry of patient tissue samples. Immunohistochemistry staining was performed according to standard techniques. Staining was carried out with a mouse monoclonal IgG antibody, anti-BRCA1 (OP92- 100UGCN, Merck Chemicals Ltd, Nottingham, UK), and anti-BRCA2 (MAB2476, R & D Systems, Minnesota, US). Two independent pathologists blinded to the clinical data and each other’s opinion scored the expression based on the staining intensity. Scoring was as follows: 0, 0%; 1, 1 to <10%; 2, 10 to <50%; 3, 50 to <90%; 4, if >90% of the cells were positive. The tumor was considered BRCA1/2 mutation-positive when less than 10% of the tumor cells had a positive reaction. The tumor was considered p53-positive when 50% or more of the tumor cells had a positive reaction.

2.3. Statistical Analysis

All statistical analyses were conducted using SPSS software Version 17 (SPSS Inc., Chicago, IL, USA).The Cox proportional hazards model was used to evaluate univariate and independent multivariate associations with the effect of clinical parameters, and BRCA1/2 and p53 status on overall survival. Probability values of less than 0.05 were considered to indicate statistical significance.

3. RESULTS

The baseline patient characteristics are shown in Table 1. Two cases (14%) had a BRCA1 mutation, and none had a BRCA2 mutation. Eleven cases (79%) were positive for p53. In the univariate analysis, the factors significantly associated with overall survival were (pre-chemotherapy CA125—pre-2nd chemotherapy CA125)/pre-chemotherapy CA125 (p = 0.0034) and (pre-chemotherapy CA125—pre-3rd chemotherapy CA125)/pre-chemotherapy CA125 (p = 0.0287). Neither BRCA1 nor p53 status were detected as predictors of overall survival (Table 2).

Table 1. Patient characteristics.

Table 2. Univariate analysis of risk factors associated with overall survival.

Multivariate analysis performed with overall survival as an endpoint revealed that neither was a significant factor (Table 3). Median survival rate was 23.5 months (2 - 82 months) in patients with no BRCA1 mutation, and all had died. By contrast, one patient with a BRCA1 mutation remains alive (85 months), and the other patient died at 64 months. Median survival rate was 23 months (2 - 85 months) in patients that were p53-positive, and 27 months (22 - 36 months) in patients that were p53-negative.

4. DISCUSSION

PPSC is reported to arise from the extra-ovarian peritoneum [14]. A recent study, however, demonstrated an association with tubal intraepithelial carcinoma in 47% of patients with PPSC [15], suggesting the potential role of the distal fallopian tube as an organ of serous carcinogenesis. Symptoms include abdominal distension and pain with ascites caused by peritonitis carcinomatosa. Most patients do not consult a gynecologist until the disease is in an advanced stage, and patients with PPSC have a worse prognosis than those with ovarian cancer.

Table 3. Multivariate analysis of risk factors associated with overall survival.

Median survival is 12 to 18 months [16]. PPSC is an ovarian cancer subtype, and therefore the chemotherapy regimen is the same as that for ovarian cancer. Patients with ovarian cancer with a BRCA mutation are considered to be platinum-sensitive, and thus have better prognosis than those with no BRCA mutation. Overall survival is 52.7 months in patients with low/intermediate BRCA1 mRNA expression, which is significantly better than the overall survival of 18.2 months in patients with high BRCA expression [9]. In the present study, median survival was 22 months in patients with positive BRCA1 expression and 64 months in the 2 patients with negative BRCA1 expression. Based on the present study, BRCA1 may be also a predictor of the prognosis of PPSC, although the sample size was small. By contrast, no BRCA2 mutation was detected in the present study. Some reports documented an overall survival advantage conferred by BRCA2 mutations compared with either having no BRCA mutation or having a BRCA1 mutation in ovarian cancer [17,18]. In these reports, the frequency of the BRCA2 mutation was half that of the BRCA1 mutation. In the present study, it is therefore not surprising that no cases of BRCA2 mutation were detected because the BRCA1 mutation was detected in only two cases. No relation between p53 status and overall survival was detected in the present study. Over half the PPSC patients were p53-positive, and BRCA1 mutation carriers had a higher overall incidence of p53 mutations than those with wild-type BRCA1 [11]. The p53 signature, which is defined as a morphologically normal, strongly p53-immunopositive segment of tubal secretory (non-ciliated) cells spanning at least 12 consecutive nuclei [19], has been found in patients with BRCA germline mutations, with an incidence ranging from 11% to 71% of cases, and also in normal controls (19% - 50%) [20-22]. To our knowledge, however, no reports have described a relation between p53 status and overall survival in patients with PPSC.

CA125 is a useful marker for estimating treatment efficacy in patients with ovarian cancer and PPSC. The CA125 regression rate is a predictor of optimal debulking surgery in patients receiving neoajduvant chemotherapy with advanced ovarian cancer [23,24], suggesting that the CA125 regression rate may be predictor of overall survival in patients with PPSC without surgery. In the present study, however, the CA125 regression rate was detected as a factor in univariate analysis but not in multivariate analysis. Possible explanations for CA125 regression rate not being detected as a predictor of overall survival in the present study might be the more aggressive behaviour of PPSC compared with ovarian cancer and the small sample size. Limitations of the present study include the small sample size, the fact that it is a retrospective study, hereditary breast and ovarian cancer might be included because genetic testing was not available.

5. CONCLUSION

In conclusion, the BRCA1 mutation was detected in 14% in patients with PPSC and these patients had a better prognosis than patients not having the BRCA1 mutation. BRCA1 might be a predictor of overall survival in patients with PPSC receiving chemotherapy. There is a need for new biomarkers, however, because most patients with PPSC have a poor prognosis and have no BRCA1 mutation.

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NOTES

*Corresponding author.