Pathologic complete response and overall survival in breast cancer subtypes in stage III inflammatory breast cancer

The NCR is a nationwide population-based cancer registry. All newly diagnosed malignancies in the Netherlands are recorded and notified through the nationwide Pathology Archive (PALGA), which collects all pathology reports of Dutch hospitals (N = 92). Trained NCR registrars directly collect patient-, tumor- and treatment-related characteristics from the patient’s medical records. The NCR collects cancer incidence data covering more than 95% of all cancer patients in the Netherlands [16]. Morphology and differentiation are graded according to the International Classification of Diseases for Oncology [17]. Staging is performed according to the TNM classification [18, 19]. With respect to IBC, the TNM criteria have not changed over time. The municipal administration was used to verify the patient’s vital status and, if applicable, date of death through a yearly linkage. Follow-up has been completed until February 29, 2016. The privacy committee of the NCR has approved this study.

Patients, diagnosed from 2006 to 2015, with clinical T4dN0–3M0 breast cancer were identified, excluding patients with only a pathological T4d status without clinical T4d status.

The year 2006 was selected as the start of the analysis since HER2 was not routinely collected prior to 2006. Histological type and HR/HER2 status were assessed in the primary tumor from a needle biopsy prior to any therapy. Patients were classified into four breast cancer subtypes, based on HR status and HER2 status: HR+ (ER+ and/or PR+)/HER2− , HR+ (ER+ and/or PR+)/HER2+, HR− (ER− and PR−)/HER2+ (HER2-enriched), and HR− (ER− and PR−)/HER2− (triple negative). Patients were excluded when data on HR and/or HER2 receptor status were missing.

According to Dutch guidelines, ER/PR status had been determined with immunohistochemistry (IHC). At least 10% positive tumor nuclei were considered as a positive result. In the Netherlands, HER2 status was considered positive with an immunohistochemical score of 3 + (at least 10% of tumor cells with strong complete membrane staining) or amplification of the HER2 gene diagnosed with in situ hybridization (ISH) (in at least 10% of tumor cells showing a ratio of HER2 probe to centromere chromosome 17 probe of > 2.2 or with single probe HER2 test when mean > 6 HER2 genes per tumor nucleus were detected) or with other amplification-based techniques, such as multiplex ligation-dependent probe amplification (MLPA). In case of an immunohistochemical score of 2 + (at least 10% of tumor cells with slight to moderate complete membrane staining, considered as an equivocal result), ISH or MLPA was performed. If in this case HER2 was found to be amplified, HER2 was considered positive. HER2 status was considered negative with an immunohistochemical score of 0 or 1 + or if ISH or MLPA showed no amplification of the HER2 gene. In the Netherlands, some variation in determining the HER2 status existed in the period 2006–2016 (especially the cutoff for amplification (> 2,2 or ≥ 2) in the double probe ISH test). For this study the HER2 status as was registered in the NCR was used.

Compared to other authors, we did not incorporate tumor grade in the subtype classification [9].

If data were missing for pretreatment biopsies, this was substituted with data of the postoperative specimen. In all cases, the highest known grade was registered. Grade could be determined in 99% of patients who underwent a surgical procedure without NACT. If available, clinical lymph node involvement was determined on clinical and radiological findings and pretreatment pathological information. Pathological lymph node involvement was determined after surgery without NACT (pN status) or with NACT (ypN status). Trimodality treatment (NACT, surgery, and adjuvant locoregional radiation therapy) was analyzed. Chemotherapy, endocrine therapy, and targeted therapy (trastuzumab) were reported as administered or not administered. If available, specific types of chemotherapy were assessed. Pathological response to NACT was analyzed and pCR was defined as the absence of microscopic residual invasive cancer in the surgically removed specimen (ypT0 and ypTis) after NACT, whereas the absence of invasive residual disease in axillary lymph nodes was considered as lymph node pCR (ypN0). With respect to tumor stage, ypT1-3 tumors were considered to have achieved a partial response to NACT. Resection margin status was reported (from 2011 onwards) as free, focal incomplete, or more than focal incomplete, according to the Dutch Guideline for Breast Cancer Treatment. A free resection margin is defined as no tumor, either invasive and/or ductal carcinoma in situ (DCIS), reaching the inked margin. No information was available concerning re-operations.

Tumor characteristics were compared between the different subtypes using Chi-squared tests for categorical variables and non-parametric approaches (Mann–Whitney U tests) for continuous variables. Fisher’s exact test was used to determine if there were non-random associations between two categorical variables in case of less than five patients per stratum. In case of too little events to calculate the p value accurately, the p value was not calculated. The OS was calculated from the date of diagnosis to the date of death from any cause, or the last date of observation. Follow-up was calculated until time of death or end of observation. OS was determined using Kaplan–Meier curves and breast cancer subtypes were compared using the log-rank test. To adjust for patient-, tumor-, and treatment-related characteristics, a multivariable Cox proportional hazard analysis was performed. Variables included were age, breast cancer subtype, nodal stage, histological tumor type, and grade, and trimodality therapy, as these variables were significantly different between breast cancer subtypes and significantly influenced the outcome (p < 0.1). For all other analyses, a p value < 0.05 was considered as statistically significant. All statistical analyses were performed in the software package STATA version 14.1.

From 2006 to 2015, 1216 patients with stage III IBC were identified. After exclusion of 114 patients due to unknown HR/HER2 status and 41 patients with a pathological T4d status without clinical T4d status, 1061 patients remained for analysis. Clinicopathological characteristics for each subtype are shown in Table 1.

The distribution of breast cancer subtypes was as follows: HR+/HER2− (N = 453, 42.7%), HR−/HER2− (triple negative) (N = 258, 24.3%), HR−/HER2+ (HER2-enriched) (N = 180, 17.0%), HR+/HER2+ (N = 170, 16.0%). In the HR+/HER2− and HR+/HER2+ groups, 14 and 12 tumors, respectively, were ER− and PR+ .

In 670 patients (63.1%), NACT was administered and least often in HR+/HER2− IBC. Adjuvant radiotherapy was given in 679 patients (66.4–78.3%; 85.0% of all operated patients). Adjuvant radiotherapy was administered less often in HR+/HER2− IBC (60.9%), compared to HER2-enriched (66.7%), HR−/HER2− (66.3%), and HR+/HER2+ (65.9%) IBC (Table 2).

Of the 623 patients with HR-positive (HR+/HER2– and HR+/HER2+) IBC, 559 patients (89.7%) received antihormonal treatment. In patients with HR+/HER2+ and HR−/HER2+ disease (350 patients), trastuzumab was perioperatively administered in 248 patients (70.9%).

Surgery was performed in 799 patients (75.3%), of which mastectomy with axillary lymph node dissection was performed most often in all subgroups (56.7–74.4%). Twenty-eight patients underwent breast-conserving therapy and in 24 of these patients information concerning surgical margins was available: 21 patients had a complete and 3 patients underwent an incomplete resection.

In 560 (52.8%) of all IBC patients (and in 78.0% of patients who were surgically treated), trimodality therapy was applied, regardless of subgroups.

Patients receiving NACT were younger (54.0 years ± 11.8 years) compared to patients not receiving it (73.7 years ± 14.6 years). The median age for HER2+ patients receiving trastuzumab was 54.6 years ± 13.7 years, compared with 63.7 years ± 16.1 years for patients not receiving it.

pCR of the breast tumor was achieved in 156 patients (23.2%), out of 670 patients who received NACT. pCR of the breast and lymph nodes was reported in 10 of 250 patients with HR+/HER2− (4.0%), 24 of 116 patients with HR+/HER2+ (20.7%), 47 of 128 patients with HR−/HER2+ (36.7%), and 28 of 176 patients with HR−/HER2− (15.9%) (Table 3).

In patients receiving trimodality therapy, achieved pCR rates (after NACT and surgery and prior to adjuvant radiation therapy) were HR+/HER2− 14 (6.4%), HR+/HER2+ 22 (23.9%), HR−/HER2+ 47 (44.3%), HR−/HER2− 28 (19.6%).

Figure 1 shows crude OS of all included patients, subdivided by subtype. The study cohort had a median survival of 4.2 years with a median follow-up of 2.4 years (interquartile range 1.1–4.5) and a 5-year OS rate of 55.6%. OS differed significantly between the subtypes (p < 0.001), with the worst OS for triple-negative IBC: HR+/HER2− (60.0%), HR+/HER2+ (67.7%), HR−/HER2+ (57.2%), HR−/HER2− (38.8%). After correction for confounding variables, HR−/HER2− disease still was associated with a significantly lower 5-year OS, compared to HR+/HER2− disease [HR 2.40 (95% CI 1.29–4.45)] (Table 4).

Figure 2 displays OS of the different subtypes in case of pCR.

In case of a combined pCR (ypT0/TisN0), an improved survival was observed for all subtypes, but especially for HER2+ tumor subtypes: HR+/HER2− (80.0 vs. 70.6%), HR+/HER2+ (91.7 vs. 72.4%), HR−/HER2+ (83.0 vs. 50.0%), HR−/HER2− (57.1 vs. 42.5%) (Table 4).

A total of 68 patients underwent NACT and (any type of) surgery without subsequent radiotherapy.

Patients who received trimodality therapy had better OS as opposed to those who did not have it (Fig. 3a, b, respectively): HR+/HER2− (74.9 vs. 46.1%), HR+/HER2+ (80.4 vs. 52.6%), HR−/HER2+ (76.4 vs. 29.7%), HR−/HER2− (47.6 vs. 27.8%). After correction for age, breast cancer subtype, morphology, tumor grade, and clinical nodal status, trimodality therapy was still associated with improved survival [HR 0.42 (95% CI 0.29–0.59)].