Journal of Breast Cancer

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1 Journal of Breast Cancer ORIGINAL ARTICLE J Breast Cancer 13 September; 16(3): Prognostic Value of the Nodal Ratio and Ki-67 Expression in Breast Cancer Patients Treated with Postmastectomy Radiotherapy Tae Ryool Koo, Keun Yong Eom, Eun Young Kang 1, Yu Jung Kim 1, Sung Won Kim 1, Jee Hyun Kim 1, Jae Sung Kim, In Ah Kim Department of Radiation Oncology, Seoul National University College of Medicine, Seoul; 1 Breast Care Center, Seoul National University Bundang Hospital, Seongnam, Korea Purpose: This pilot study aimed to evaluate prognostic factors of postmastectomy radiotherapy (PMRT) for breast cancer patients undergoing systemic therapy in either preoperative or postoperative setting. Methods: Between 3 and 9, 113 patients received PMRT: 61 underwent preoperative systemic therapy (PST subgroup) and 52 received postoperative systemic therapy (non- PST subgroup). Results: The median follow-up time was 72.3 months (range, months) for surviving patients. In univariate analysis of all patients, disease-free survival (DFS) was associated with age, nodal ratio (NR), and Ki-67 expression; overall survival (OS) was associated with NR and Ki-67 expression. Pathologic N stage and HER2 expression were marginally associated with DFS and OS. In the non-pst subgroup, DFS was associated with age, NR, venous invasion, and Ki-67 expression; OS was associated with age. In the PST subgroup, DFS was associated with ypn stage and NR; OS was associated with ypn, histologic grade, HER2 expression, and p53 expression. In multivariate analysis of all patients, DFS and OS were significantly associated with NR (p=.3 and p=.19, respectively) and Ki-67 expression (p=.2 and p=.15, respectively). Patients were classified into low-risk (NR.2 and Ki-67 %; n=34), intermediate-risk (NR >.2 or Ki-67 >%; n=63), and high-risk (NR >.2 and Ki-67 >%; n=16) subgroups. All low-risk patients were alive at the time of analysis. High-risk (p<.1 and p=.1, respectively) and intermediate-risk (p=.22 and p=.8, respectively) patients had significantly shorter DFS and OS than low-risk patients. This prognostic model was statistically significant for DFS when applied to the PST (p=.1) and non- PST (p=.16) subgroups separ ately. Conclusion: For breast cancer patients undergoing PMRT, NR and Ki-67 are potential prognostic factors. A model using these factors might help predict a poor prognosis. Whether NR and Ki-67 are also prognostic for different setting of systemic therapy, preoperative or postoperative, warrants further study. Key Words: Breast neoplasms, Ki-67 antigen, Lymph nodes, Mastectomy, Radiotherapy INTRODUCTION Correspondence to: In Ah Kim Department of Radiation Oncology, Seoul National University Bundang Hospital, Seoul National University College of Medicine, 182 Gumi-ro 173beon-gil, Bundang-gu, Seongnam , Korea Tel: , Fax: inah228@snu.ac.kr This work was supported by the grant (No. 81) for Cancer Control Program from Korean Ministry of Health & Welfare and for BAERI (No ) from National Research Foundation. Received: March 22, 13 Accepted: July 21, 13 For patients with locally advanced breast cancer (LABC), even after mastectomy and systemic therapy, the possibility of occult disease cannot be excluded. Postmastectomy radiotherapy (PMRT) is performed to improve locoregional control (LRC) and survival, a strategy supported by the findings of a number of randomized trials [1-3]. Axillary lymph node (ALN) status is an important prognostic factor for LRC and survival in patients with breast cancer, and the 7th American Joint Committee on Cancer (AJCC) staging system for breast cancer is based on the absolute number of pathologically positive ALNs [4]. Recently, several studies have reported that the nodal ratio (NR), the proportion of involved ALNs amongst all excised ALNs, is of equal prognostic importance [5-1]. In addition, both gross pathologic and biomolecular parameters can be useful prognostic factors for breast cancer. In this regard, hormone receptor (HR) status and c-erbb-2/her2 status are markers of specific intrinsic subtypes of breast cancer. The Ki-67 index, a marker of cell 13 Korean Breast Cancer Society. All rights reserved. pissn This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License ( eissn licenses/by-nc/3.) which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

2 Nodal ratio and Ki-67 in postmastectomy radiotherapy 275 proliferation, is likewise a marker of a specific intrinsic subtype [11,12] and is also associated with breast cancer recurrence and death [13-16]. Conventionally, PMRT was performed following postoperative systemic therapy in LABC patients. Recently however, preoperative systemic therapy (PST) following PMRT has been widely used in order to facilitate conservation of breast tissue. Here, we report the results of a pilot study designed to identify prognostic or predictive factors for patients with LABC who undergo PMRT in either preoperative or postoperative setting of systemic therapy. METHODS With the approval of the Institutional Review Board of Table 1. Patient characteristics Variable No. (%) Age (yr)* 47 (27-77) Excised lymph nodes* 22 (1-55) Menopausal status Pre 74 (65) Post 39 (35) Clinical T ct1 3 (5) ct2 11 (18) ct3 29 (48) ct4 18 (3) Clinical N cn 4 (7) cn1 31 (51) cn2 18 (3) cn3 8 (13) Clinical stage II 11 (18) III 5 (82) Pathologic T ypt 9 (8) ypt1 32 (28) ypt2 52 (46) ypt3 16 (14) ypt4 4 (4) Pathologic N ypn 24 (21) ypn1 25 (22) ypn2 34 (3) ypn3 3 (27) Pathologic stage 7 (6) I 8 (7) II 29 (26) III 69 (61) *Median (range); The patients with preoperative systemic therapy are included only. Seoul National University Bundang Hospital (B-15/153-17), we retrospectively reviewed the medical records of 113 patients with LABC who underwent mastectomy followed by PMRT between March 3 and December 9 (Figure 1). Patients who had synchronous metastases at diagnosis, a history of malignancy, or incomplete radiotherapy (RT) were excluded from the present study. The pathologic stage was grad- PST subgroup (n=61) Non-PST subgroup (n=52) Chemo therapy Mastectomy Table 2. Tumor characteristics Maste ctomy Chemo therapy Chemotherapy Figure 1. A flow sheet on treatment of breast cancer: preoperative systemic therapy (PST) was considered in patients with advanced clinical T stage or axillary lymph node involvement. *Chemotherapy was administered before and after mastectomy; or additional chemotherapy was given in patients with adverse pathologic features. Variable No. (%) Histology IDC 94 (83) Others 19 (17) Histologic grade I 4 (4) II 51 (45) III 47 (42) Extracapsular extension Negative 28 (25) Positive 49 (43) Lymphatic invasion Negative 41 (36) Positive 72 (64) Venous invasion Negative 94 (83) Positive 19 (17) Baseline HR Negative 46 (41) Positive 67 (59) Baseline c-erbb-2-2+ (71) (29) Baseline HER2 Negative 85 (75) Positive 28 (25) Baseline p53 (%) 1 83 (73) > 1 3 (27) Baseline Ki-67 (%) 72 (64) > 41 (36) IDC=infiltrating ductal carcinoma; HR=hormone receptor. * Hormonal therapy

3 276 Tae Ryool Koo, et al. ed according to the seventh edition of the AJCC cancer staging system [4]. Patient and tumor characteristics are listed in Tables 1 and 2. Surgery All the patients underwent mastectomy. ALN dissection (level I and II) was performed in 11 cases (97%), with sentinel lymph node biopsy alone performed in the remaining 3 (3%). Of the patients undergoing ALN dissection, 7 underwent ALN dissection alone and underwent sentinel lymph node biopsy followed by ALN dissection (Table 3). Table 3. Treatment regimens Variable No. (%) Chemotherapy Neoadjuvant DA 3 cycles+da 3 cycles* (33) DA 6 cycles 19 (31) DA 3 cycles DAC 3 cycles 4 (7) AC 4 cycles+t 4 cycles* 1 (16) Adjuvant AC 4 cycles T 4 cycles 43 (83) Hormone therapy Tamoxifen 33 (29) Aromatase inhibitor 13 (12) Tamoxifen Aromatase inhibitor 15 (13) Targeted therapy Herceptin 24 (21) LN dissection SLNBx 3 (3) ALND 11 (97) Radiotherapy Median dose (Gy) 5.4 ( ) Regional node irradiation 16 (94) Tumor bed boost 3 (3) DA=docetaxel and doxorubicin; AC=doxorubicin and cyclophosphamide; T=paclitaxel; LN=lymph node; SLNBx=sentinel lymph node biopsy; ALND= axillary lymph node dissection. *Chemotherapy was performed before and after surgery; Median (range). Chemotherapy The most common PST regimen was DA (docetaxel and doxorubicin) followed by ACT (doxorubicin, cyclophosphamide, and paclitaxel). After completion of PST, the PST subgroup patients underwent mastectomy with ALN dissection. ACT was the most common adjuvant chemotherapy regimen. Adjuvant hormonal therapy was administered in patients with a positive HR status and consisted of 5 years of tamoxifen for premenopausal women and initial aromatase inhibitor therapy or a switch from tamoxifen to aromatase inhibitor therapy for postmenopausal women. Trastuzumab was recommended for all patients with a tumor exhibiting c-erbb-2 overexpression (3+) or HER2 gene amplification (Table 3). Radiotherapy For RT, the chest wall and supraclavicular fossa were irradiated with up to 5.4 Gy at 1.8 Gy per fraction with 5 fractions per week; for a scar boost, 9 Gy at 1.8 Gy per fraction with electrons was administered. Two opposing tangential and one anterior photon beam were used for chest wall and supraclavicular fossa RT, respectively (Table 3). PMRT was started after the completion of adjuvant chemotherapy. When capecitabine was used as the adjuvant chemotherapeutic agent, the patient received PMRT concurrently (n= 4). Biomarkers We reviewed the following histopathologic parameters: estrogen receptor (ER) status; progesterone receptor (PR) status; and the expression of c-erbb-2, p53, Ki-67, and COX-2. Baseline histopathologic parameters were evaluated by immunohistochemical (IHC) analysis using pre-pst biopsy specimens (PST subgroup) or surgical specimens (non-pst subgroup). IHC staining was performed using a BenchMark XT autostainer (Ventana Medical Systems, Tucson, USA) and an i-view detection kit (Ventana Medical Systems) as previously described [17]. The positive cut-off values were IHC staining in 1% for ER/PR [18], in > 1% for p53, and a 3+ staining score for COX-2 and c-erbb-2. The NR was defined as the number of ALNs with cancer involvement divided by the total number of excised ALNs. Lymph node (LN) status was evaluated by hematoxylin and eosin staining. Fluorescence in situ hybridization was performed for the analysis of HER2 gene amplification as reported previously [17]. Follow-up The base follow-up duration was defined from the date when the first treatment was initiated. In cases of treatment failure, we analyzed the first site of relapse. Locoregional recurrence (LRR) included recurrences in the ipsilateral chest wall or ipsilateral regional LNs (axillary, supra/infraclavicular, and internal mammary). Relapses in the contralateral chest wall, axillary LNs, supra/infraclavicular LNs, internal mammary LNs, cervical LNs, or other organs were defined as distant metastases (DM). Statistics Using the Kaplan-Meier method and the log-rank test, survival curves and differences between subgroups were estimated. For multivariate analysis, the Cox proportional hazards method was used. To compare proportions between subgroups, Pearson chi-square and Fisher exact test were used.

4 Nodal ratio and Ki-67 in postmastectomy radiotherapy 277 SPSS version 18. (SPSS, Chicago, USA) was used for statistical analyses. A p-value less than.5 was deemed to be statistically significant. Generally, a value above 1% to % of the Ki-67 index was defined as a high level [12-14,16]. We compared survival curves using 3 hypothetical cut-off values, 1%, 15%, and % of the baseline Ki-67 index, and found that the latter gave the most significant differences. The NR cut-off value used in previous studies varied from.15 to.25 [5,7-1]. We used 6 candidates for the cut-off value of the NR, ranging from.5 to.3 with intervals of.5. The maximal chi-square method in the R program version (R Development Core Team, Vienna, Austria; available from was used to obtain the optimal cut-off value of the NR, which was.2. RESULTS A total of 61 patients with an advanced clinical T stage tumor (T3 and T4) or ALN involvement received PST. In the PST subgroup, 7 patients received additional chemotherapy because of adverse pathologic features such as advanced stage Table 4. Univariate analysis for entire patients Variable No. 5-yr LRPFS (%) p-value 5-yr DMFS (%) p-value 5-yr DFS (%) p-value 5-yr OS (%) p-value Age (yr) > ypt T T ypn N N Nodal ratio > ECE Negative Positive HG I/II III Venous invasion Negative Positive Lymphatic invasion Negative Positive Baseline HR Negative Positive Baseline c-erbb Baseline HER2 Negative Positive Baseline p53 (%) > Baseline Ki-67 (%) > LRPFS=locoregional progression-free survival; DMFS=distant metastasis-free survival; DFS=disease-free survival; OS=overall survival; ECE=extracapsular extension; HG= histologic grade; HR= hormone receptor.

5 278 Tae Ryool Koo, et al. or negative HR status. The other 52 patients received adjuvant systemic therapy. Chest wall and supraclavicular fossa irradiation was administered in 16 patients, and chest wall irradiation only in 7 patients. A total of 3 patients received a scar boost. The median number of excised ALNs was 22 (range, 1-55) in the whole cohort and 23 (range, 1-55) and 21 (range, 5-5) in the non-pst and PST subgroups, respectively. The median NR was.19 (range, -1) in the whole cohort, including patients with pathologically noninvolved ALNs (pn), and.26 (range,.3-1.) in patients with pathologically in- Nodal ratio.2 Ki-67 % Nodal ratio >.2 Ki-67 >% p=.644 p= A B Nodal ratio.2 Ki-67 % Nodal ratio >.2 Ki-67 >% p=.6 p= Nodal ratio.2 C Ki-67 % D Nodal ratio >.2 Ki-67 >% p=.32 p= E F Figure 2. Survival curves in the patients with breast cancer having postmastectomy radiotherapy: locoregional progression-free survival according to the nodal ratio (A) and the baseline Ki-67 (B); disease-free survival according to the nodal ratio (C) and the baseline Ki-67 (D); overall survival according to the nodal ratio (E) and the baseline Ki-67 (F).

6 Nodal ratio and Ki-67 in postmastectomy radiotherapy 279 volved ALNs (pn+). We used the NR of.2 as a cut-off value to classify patients into high and low NR groups. Follow-up and failure analysis The median follow-up duration was 72.3 months (range, months) for surviving patients. In the entire cohort, the 5-year survival rates were 87.2%, 78.9%, 77.3%, and 85.3% for locoregional progression-free survival (LRPFS), distant metastasis-free survival (DMFS), disease-free survival (DFS), and overall survival (OS), respectively. With respect to the type of initial disease relapse, LRR occurred in 4 patients (PST subgroup, 4), DM in 14 patients (non-pst subgroup, 7; PST subgroup, 7), and both LRR and DM in 1 patients (non-pst subgroup, 3; PST subgroup, 7). One of the patients with initial LRR underwent resection and the other 3 underwent systemic therapy. Of those patients with initial LRR and DM, 1 patient underwent resection and systemic therapy, 1 patient underwent chemotherapy and whole brain irradiation, and 6 patients were treated using systemic therapy only. Table 5. Univariate analysis according to sequence of systemic therapy Variable Non-PST subgroup PST subgroup No. 5-yr DFS (%) p-value 5-yr OS (%) p-value No. 5-yr DFS (%) p-value 5-yr OS (%) p-value Age (yr) > ypt T T ypn N N Nodal ratio > ECE Negative Positive Histologic grade I/II <.1 III Venous invasion Negative Positive Lymphatic invasion Negative Positive Baseline HR Negative Positive Baseline c-erbb Baseline HER2 Negative Positive Baseline p53 (%) > Baseline Ki-67 (%) > PST= preoperative systemic therapy; DFS= disease-free survival; OS= overall survival; ECE=extracapsular extension; HR=hormone receptor.

7 2 Tae Ryool Koo, et al. Univariate analysis Univariate analysis revealed that patients with a NR of >.2 had a significantly lower DMFS (p=.3), DFS (p=.6), and OS (p=.32) than those with a NR of.2. Patients with a baseline Ki-67 index of > % had a significantly lower LRPFS (p=.32), DMFS (p=.13), DFS (p=.7), and OS (p =.3) than those with a baseline Ki-67 index of p= p= Figure 3. Survival curves in the patients with breast cancer having postmastectomy radiotherapy according to pathologic nodal stage: (A) disease-free survival and (B) overall survival. Table 6. Multivariate analysis ypno-1 ypn2-3 ypno-1 ypn2-3 A B %. The baseline HR level was associated with LRPFS (p=.25) but not with DMFS (p=.379), DFS (p=.236), and OS (p=.253). The pathologic nodal stage was marginally associated with DMFS (p=.64), DFS (p=.87), and OS (p=.84). These results are detailed in Table 4, Figures 2 and 3. We also performed subgroup analysis for the non-pst and PST subgroups. In the former, age (p=.1), NR (p=.3), venous invasion (p=.35), and the baseline Ki-67 index (p=.37) were associated with DFS, although only age (p=.48) was associated with OS. In the PST subgroup, ypn stage (p=.48) and NR (p=.28) were associated with DFS and ypn (p=.3), histologic grade (p<.1), baseline HER2 expression (p=.48), and baseline p53 expression (p=.26) were associated with OS (Table 5). Multivariate analysis We performed multivariate analysis incorporating the NR, baseline Ki-67 index, age, histologic grade, and baseline p53 expression, all of which were found to be significantly associated with DFS or OS in univariate analysis of the entire cohort. A high NR was associated with poor DMFS (relative risk [RR], 4.63; 95% confidence interval [CI], ; p=.2), DFS (RR, 3.589; 95% CI, ; p=.3), and OS (RR, 3.444; 95% CI, ; p=.19). A high baseline Ki-67 index was associated with poor DMFS (RR, 3.125; 95% CI, ; p=.4), DFS (RR, 3.274; 95% CI, ; p=.2), and OS (RR, 3.133; 95% CI, ; p=.15). Results of the multivariate analysis are detailed in Table 6. Prognostic model We devised a prognostic model using the NR and baseline Ki-67 index, with a score of zero points for a NR of.2 or a baseline Ki-67 index of % and 1 point for a NR of >.2 or a baseline Ki-67 index of > %. Patients were classified into 3 subgroups according to their total score: low risk ( point, n = 34), intermediate risk (1 point, n = 63), and high risk (2 points, n = 16). No deaths occurred in the low-risk group, whereas 13 patients in the intermediate-risk group and Variable LRPFS DMFS DFS OS p-value RR (95% CI) p-value RR (95% CI) p-value RR (95% CI) p-value RR (95% CI) Young age ( 35 yr) Histologic grade (III) ( ) High nodal ratio (>.2) ( ) ( ) ( ) Baseline Ki-67 (> %) ( ) ( ) ( ) Baseline HR (+) Baseline p53 (> 1%) LRPFS=locoregional progression-free survival; DMFS=distant metastasis-free survival; DFS=disease-free survival; OS=overall survival; RR=relative risk; CI= confidence interval; HR= hormone receptor.

8 Nodal ratio and Ki-67 in postmastectomy radiotherapy 281 Low vs. Intermediate Low vs. High Low risk Intermdiate risk High risk p=.4 p= Low vs. Intermediate Low vs. High Low risk Intermdiate risk High risk p=.22 p< Low vs. Intermediate Low vs. High Intermdiate risk High risk Low risk p=.8 p< Figure 4. Survival curves in the patients with breast cancer having postmastectomy radiotherapy according to the risk group: (A) locoregional progression-free survival, (B) disease-free survival, and (C) overall survival. A B C 6 patients in the high-risk group had died at the time of the last follow-up. When comparing the high- and low-risk patients, a significant difference was found in LRPFS (p=.), DMFS (p<.1), DFS (p<.1), and OS (p<.1). A significant difference was also observed between the intermediate- and low-risk groups with respect to DMFS (p=.31), DFS (p=.22), and OS (p=.8), but not LRPFS (p=.4) (Figure 4). We used the Cox proportional hazards method in order to evaluate the RR among the different risk groups. For LRPFS, the high- and intermediate-risk groups demonstrated RRs of (95% CI, ; p=.67) and (95% CI, ; p=.222), respectively, and for DMFS, the RRs of the high- and intermediate-risk groups were (95% CI, ; p=.1) and 4. (95% CI, ; p=.49), respectively. With respect to DFS, the high- and intermediate-risk patients showed RRs of (95% CI, ; p=.1) and (95% CI, ; p=.37), respectively. We applied this prognostic model to the non-pst and PST subgroups. There was a significant difference in DMFS (p=.16 and p<.1) and DFS (p=.16 and p<.1) in the non-pst and PST subgroups, respectively. There was no significant difference in the LRPFS in the non-pst (p=.364) and PST (p=.224) subgroups, although there was a significant difference with respect to OS in the PST subgroup (p=.45) but not in the non-pst subgroup (p=.74). DISCUSSION Several large, randomized studies have shown that PMRT improves LRC and survival in breast cancer patients, particularly those with more than 3 involved ALNs [1-3]. To date though, the role of PMRT in breast cancer patients with fewer than 4 metastatic ALNs has not been evaluated. Overgaard et al. [19] conducted a reanalysis of Danish trials and found that PMRT benefited patients with 1 to 3 positive ALNs. Recently, the number of excised ALNs was shown to be as important as the number of involved ALNs, suggesting that the NR is an important prognostic factor [5-1]. In a study by the Surveillance, Epidemiology and End Results program, the NR was found to be better at predicting disease-specific survival than the number of involved ALNs [7]. Truong et al. [8] reported that an NR of.25 was associated with a poor prognosis with respect to LRR, DM, and OS in patients with 1 to 3 involved ALNs. Ahn et al. [1] analyzed a nationwide registry of pn+ patients and concluded that the NR was a better prognostic factor than pn stage, particularly in patients with high-risk factors such as young age, a HER2/neu-enriched tumor, or a triple-negative tumor. In the study we report here, the pn stage showed only a borderline association with recurrence or survival in univariate analysis. A possible reason for this finding may be the heterogeneity in the sequence of systemic therapy. After PST,

9 282 Tae Ryool Koo, et al. more patients could have a lower N stage as a result of chemotherapy. This finding might also be explained by the relatively small size and short follow-up period of our study. As shown in Figure 2, the DFS and OS curves differed between patients with pn-1 and pn2-3, and it is possible that with a greater number of patients and a longer follow-up period, a statistically significant relationship might be found between survival and pn stage. Although this pilot study included patients with different pn stages, the NR (cut-off value of.2) was associated with a high risk of metastasis and short survival in LABC patients. Because the NR reflects the absolute number of excised ALNs, it might have a higher prognostic value than pn stage []. In the current cancer staging system [4], the usefulness of the absolute number of involved nodes for predicting disease burden in the axilla is confounded by the number of nodes removed [21]. When additional ALNs are excised, less residual occult disease may be expected. In Canada, ALN dissection, including all level I and II ALNs, is recommended for accurate staging and reducing the risk of recurrence in the axilla [22]. Although several studies have reported a possible prognostic role for the NR in LRC [8,23,24], we could not establish a relationship between the NR and LRC in this study. This may have been because of the relatively short follow-up duration (approximately 6 years). Improved LRC as a result of regional RT [25,26] might also account for the lack of any significant difference in LRPFS between the high NR and low NR patient groups. We suggest therefore that a randomized controlled study focusing specifically on the prognostic role of NR be conducted. In addition to the NR, biomolecular markers might also have prognostic value for LABC patients. It is generally accepted that biomolecular markers of cell proliferation, such as the baseline Ki-67 index used in our study, are associated with the response to systemic therapy [27]. Our study showed that a high baseline Ki-67 index was associated with a high risk of mortality. Furthermore, a relationship between a high Ki-67 index and other indicators of a poor prognosis has been previously reported [28]. This negative relationship would explain the prognostic value of Ki-67 index. In the present study, a Ki-67 index in excess of % was associated with baseline negative HR expression (p<.1). Consistent with our findings, the Ki-67 index has been shown to be a possible prognostic marker in several other studies. Cheang et al. [12] classified invasive breast cancer into luminal A, luminal B, and HER2-positive intrinsic subtypes on the basis of hormone receptor status, HER2 status, and the Ki-67 index, as determined using IHC. The Ki-67 index was used to distinguish luminal B from luminal A, using a cut-off value of 14%. The luminal B and luminal HER2 subtypes were found to have a poor prognosis with respect to breast cancer recurrence-free and disease-specific survival. The 1-year breast cancer-specific survival rates were 92%, 79%, and 78% in luminal A, luminal B, and HER2 positive cancer, respectively (p<.1). In a meta-analysis study of early breast cancer, Ki-67 positivity (cut-off points were defined by the authors of the studies being included) was associated with increased relapse (RR, 1.93; 95% CI, ; p<.1) and shorter survival (RR, 1.95; 95% CI, ; p<.1) in all patients. The authors of that study suggested that Ki-67 positivity was a prognostic marker in patients with early breast cancer [14]. Despite these studies, in general, the association between specific biomolecular markers and LRC remains unclear. Two previous studies found that the Ki-67 index was a possible prognostic factor of LRC [13,16]. Voduc et al. [13] defined the luminal B subtype as being ER(+) or PR(+) and HER2(-) and having a Ki-67 index of 14% in patients who had undergone mastectomy. The luminal B subgroup was associated with a high risk of local and regional recurrences. Selz et al. [16] reported that a Ki-67 index of > % was prognostic for LRFPS (RR, 4.18; 95% CI, ; p=.215) in breast cancer patients with pn after modified radical mastectomy. In addition to HER2 status, the Ki-67 index, representing tumor aggressiveness, may also be a means of identifying high-risk groups among breast cancer patients. However, controversy still exists regarding the optimal cut-off point for Ki- 67; a level of Ki-67 above 1% to % has been suggested to define a high-risk group in several studies [12-14,16]. In our study, the baseline Ki-67 index was used to determine the risk groups, using a cut-off point of %. The 11 St. Gallen Consensus [11] recommended a Ki-67 labeling index of 14% as the cut-off point to classify the intrinsic subtype of breast cancer; however, these guidelines have not been clarified. It therefore remains necessary to develop a standardized approach to using the Ki-67 index, including a single cut-off value and a reproducible way of determining the index. Here, we propose a prognostic model using 2 parameters, the NR and baseline Ki-67 index, both of which are significantly associated with disease relapse, reflecting the probability of residual tumor on a macroscopic scale and the possibility of disease relapse on a microscopic scale, respectively. Our prognostic model is simple to apply and can identify the poor prognostic group amongst a heterogeneous population with disparate pn stages or sequences of systemic therapy. Using our prognostic model, patients with a high risk of disease relapse can be identified, and intensified adjuvant treatment can be considered to improve their survival. With respect to LRC,

10 Nodal ratio and Ki-67 in postmastectomy radiotherapy 283 however, the high-risk group tended to have a worse prognosis than the low-risk group (p=.67), and the intermediaterisk group showed no association. We expect that this prognostic model would be more useful to identify the high-risk group among LABC patients with an increased long-term follow-up period. Our study has several limitations. The patients needed to be analyzed independently according to the use of PST because the NR has a prognostic value in patients with PST [6]. However, subgroup multivariate analysis was not performed because of an insufficient number of patients. In addition, the relatively short follow-up duration was a hindrance to comparing OS. These limitations may have made it more difficult to identify a relationship between treatment outcomes and well-known prognostic factors, such as T/N stage and HR status. Furthermore, the study included patients with a range of different N stages and 21% of patients had pn tumors (21%), whereas the other studies on the prognostic value of NR discussed here only involved node-positive patients. Therefore, a further study is needed with a more homogenous patient group with respect to the sequence of systemic therapy and pn stage. Additionally, for a more precise prognostic model, the change in biomarker status before and after PST [15,29] should be considered. In conclusion, we found that the NR and baseline Ki-67 index were potential prognostic markers in LABC patients who underwent PMRT. Our prognostic model, using these 2 factors, might be able to identify patients at high risk of disease relapse. Improved prognostic models will help to individualize treatment regimens for breast cancer patients. CONFLICT OF INTEREST The authors declare that they have no competing interests. REFERENCES 1. 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11 284 Tae Ryool Koo, et al. my irradiation limited to patients with four or more positive nodes, as recommended in international consensus reports? A subgroup analysis of the DBCG 82 b&c randomized trials. Radiother Oncol 7;82: Schmoor C, Sauerbrei W, Bastert G, Bojar H, Schumacher M; German Breast Cancer Study Group. Long-term prognosis of breast cancer patients with 1 or more positive lymph nodes treated with CMF. Eur J Cancer 1;37: Woodward WA, Vinh-Hung V, Ueno NT, Cheng YC, Royce M, Tai P, et al. Prognostic value of nodal ratios in node-positive breast cancer. J Clin Oncol 6;24: Canadian Association of Radiation Oncologists; The Steering Committee on Clinical Practice Guidelines for the Care and Treatment of Breast Cancer. Axillary dissection. CMAJ 1998;158(Suppl 3):S Katz A, Buchholz TA, Thames H, Smith CD, McNeese MD, Theriault R, et al. Recursive partitioning analysis of locoregional recurrence patterns following mastectomy: implications for adjuvant irradiation. Int J Radiat Oncol Biol Phys 1;5: Grills IS, Kestin LL, Goldstein N, Mitchell C, Martinez A, Ingold J, et al. Risk factors for regional nodal failure after breast-conserving therapy: regional nodal irradiation reduces rate of axillary failure in patients with four or more positive lymph nodes. Int J Radiat Oncol Biol Phys 3; 56: Wai ES, Lesperance M, Speers CH, Truong PT, Jones S, Tyldesley S, et al. Increased use of regional radiotherapy is associated with improved outcome in a population-based cohort of women with breast cancer with 1-3 positive nodes. Radiother Oncol 1;97: Truong PT, Jones SO, Kader HA, Wai ES, Speers CH, Alexander AS, et al. Patients with t1 to t2 breast cancer with one to three positive nodes have higher local and regional recurrence risks compared with nodenegative patients after breast-conserving surgery and whole-breast radiotherapy. Int J Radiat Oncol Biol Phys 9;73: Paik S, Shak S, Tang G, Kim C, Baker J, Cronin M, et al. A multigene assay to predict recurrence of tamoxifen-treated, node-negative breast cancer. N Engl J Med 4;351: Viale G, Giobbie-Hurder A, Regan MM, Coates AS, Mastropasqua MG, Dell Orto P, et al. Prognostic and predictive value of centrally reviewed Ki-67 labeling index in postmenopausal women with endocrine-responsive breast cancer: results from Breast International Group Trial 1-98 comparing adjuvant tamoxifen with letrozole. J Clin Oncol 8;26: Yerushalmi R, Woods R, Ravdin PM, Hayes MM, Gelmon KA. Ki67 in breast cancer: prognostic and predictive potential. Lancet Oncol 1; 11:

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