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Open Access 25.03.2016 | Clinical trial

Risk of regional recurrence in triple-negative breast cancer patients: a Dutch cohort study

verfasst von: Lori M. van Roozendaal, Leonie H. M. Smit, Gaston H. N. M. Duijsens, Bart de Vries, Sabine Siesling, Marc B. I. Lobbes, Maaike de Boer, Johannes H. W. de Wilt, Marjolein L. Smidt

Erschienen in: Breast Cancer Research and Treatment | Ausgabe 3/2016

Abstract

Triple-negative breast cancer is associated with early recurrence and low survival rates. Several trials investigate the safety of a more conservative approach of axillary treatment in clinically T1-2N0 breast cancer. Triple-negative breast cancer comprises only 15 % of newly diagnosed breast cancers, which might result in insufficient power for representative results for this subgroup. We aimed to provide a nationwide overview on the occurrence of (regional) recurrences in triple-negative breast cancer patients with a clinically T1-2N0 status. For this cohort study, 2548 women diagnosed between 2005 and 2008 with clinically T1-2N0 triple-negative breast cancer were selected from the Netherlands Cancer Registry. Follow-up data until 2014 were analyzed using Kaplan–Meier. Sentinel lymph node biopsy was performed in 2486 patients, and (completion) axillary lymph node dissection in 562 patients. Final pathologic nodal status was pN0 in 78.5 %, pN1mi in 4.5 %, pN1 in 12.3 %, pN2–3 in 3.6 %, and pNx in 1.1 %. During a follow-up of 5 years, regional recurrence occurred in 2.9 %, local recurrence in 4.2 % and distant recurrence in 12.2 %. Five-year disease-free survival was 78.7 %, distant disease-free survival 80.5 %, and 5-year overall survival 82.3 %. Triple-negative clinically T1-2N0 breast cancer patients rarely develop a regional recurrence. Their disease-free survival is more threatened by distant recurrence, affecting their overall survival. Consequently, it seems justified to include triple-negative breast cancer patients in randomized controlled trials investigating the safety of minimizing axillary staging and treatment.

Introduction

Breast cancer knows a large heterogeneity of tumors characterized by several molecular profiles with different clinical behaviors and responses to therapy. In clinical practice, breast cancer patients are generally classified by clinical and histological tumor characteristics, axillary lymph node status, hormonal receptor status, and human epidermal growth factor receptor 2 (HER2) status [1‐3]. Based on receptor status, several breast cancer subtypes are classified. One of these subtypes is triple-negative breast cancer (TNBC), which is characterized by the absence of (over)expression of estrogen receptor (ER), progesterone receptor (PR), and HER2 receptor. TNBC is found in approximately 15 % of newly diagnosed breast cancer patients [2, 4, 5] and is more prevalent in younger patients (<50 years) [2, 3, 4, 6, 7]. TNBC is associated with a more aggressive nature compared to other breast cancer subtypes, reflected by a larger tumor size, higher tumor grade, early peak of recurrence, and a worse 5-year overall survival rate [2, 5, 8, 9]. To date, the only systemic treatment option for TNBC patients is chemotherapy. Multiple-targeted drugs are at various stages of development for TNBC. However, no effective-targeted therapy has been detected so far [5, 10].

Currently, there is a trend toward a more conservative approach of axillary staging and treatment in breast cancer. The aim is to decrease the axillary morbidity rate, while maintaining excellent regional control without affecting overall survival. Randomized controlled trials revealed that completion axillary lymph node dissection (ALND) can be safely omitted in clinically T1-2N0 breast cancer in case of limited metastatic sentinel lymph nodes (SLNs) and breast conserving treatment [11, 12]. An ongoing trial investigates whether this is also applicable for SLN-positive patients undergoing a mastectomy (BOOG 2013-07). Further, the value of the SLN biopsy (SLNB) in current era is being questioned. Several trials randomize clinically T1(-2)N0 patients treated with breast conserving therapy to SLNB or ‘watchful waiting’ (BOOG 2013-08; SOUND; NCT01821768) [13].

Due to the low incidence of TNBC, only a minority of patients in these study populations represents TNBC patients, leading to insufficient power for representative results regarding this subgroup. Furthermore, clinicians are cautious on performing less axillary staging and treatment in TNBC, mainly because of its association with the aggressive nature and fewer systemic treatment options in this subtype of breast cancer patients.

It is questionable whether TNBC patients are at risk for higher regional recurrence rates and poorer overall survival when limiting or omitting axillary treatment. In the literature, studies on recurrence patterns in TNBC mainly focus on local and distant recurrence and overall survival. In order to gain more insight into recurrences in TNBC patients, and for regional recurrence in particular, we aimed to provide a nationwide overview on the occurrence of recurrence and overall survival in TNBC patients with a clinically T1-2N0 status.

Methods

Study population and data collection

All consecutive women of 18 years and older with primary invasive, clinically T1-2N0 unilateral TNBC diagnosed between 2005 and 2008, were identified from the Netherlands Cancer Registry, hosted by the Comprehensive Cancer Organisation the Netherlands (IKNL). Data are gathered by specially trained data managers in all hospitals in the Netherlands based on notification from the automated pathology archive (PALGA). Patients undergoing primary systemic treatment were not included in the selection. Patients diagnosed prior to 2005 or after 2008 were not included due to lack of registration of HER2 status, or lack of follow-up data, respectively. The following data were provided anonymized: age, performed surgical procedure(s), administration of adjuvant chemotherapy, adjuvant radiotherapy, histology of primary tumor and lymph nodes (i.e., tumor type, size, grade, and receptor status), time to event (local, regional, and distant event), vital status, and date of death or last day of follow-up. Five-year follow-up data on first events were available for every patient. Only first events were available, but included all events that occurred within a time frame of 3 months after diagnosis of the first event. Vital status was available up to December 31, 2014. Data were collected directly from patient records by employees of the Netherlands Cancer Registry.

Axillary lymph node staging

A clinically node negative status was defined in the 2005 Dutch breast cancer guideline as negative physical examination and axillary ultrasound [14]. Tissue sampling was recommended in case of a suspicious lymph node on axillary ultrasound. An SLNB was advised for clinically node-negative patients, followed by a completion ALND in case of a metastasis in the SLN. Isolated tumor cells were considered as pathologically node negative.

Pathological technique

The 2005 Dutch breast cancer guideline recommended to completely include SLNs of up to 0.5 cm, to half SLNs of 0.5–1.0 cm, and fully imbed SLNs greated than 1 cm in lammellas of 0.2 cm. It was furthermore recommended to section each paraffin block at three levels with 250-micrometer intervals, but this may have varied between pathology laboratories. If no metastasis was detected with hematoxylin and eosin, immunohistochemical staining was adviced.

Lymph nodes of the (completion) ALND specimen were embedded in paraffin after formalin fixation and sliced with a recommended maximum thickness of 3 mm, followed by hematoxylin and eosin staining.

Each lymph node was registered according to pathological findings: negative (pN0), or as isolated tumor cell (pN0(i+); ≤0.2 mm), micrometastasis (pN1mi; 0.2 mm ≤2.0 mm), or macrometastasis (pN1-3; >2.0 mm).

Tumors were graded according to the modified Bloom–Richardson grading system [15]. The ER and PR status was determined by immunohistochemistry and scored using <10 % of tumor staining as the negative cut off. The HER2 receptor status was determined by immunohistochemistry and recorded as negative in case of 0 or +1 staining, and positive in case of +3 staining. Fluorescence in situ hybridization analyses was performed in case of +2 staining.

Adjuvant chemotherapy recommendations

The 2005 Dutch breast cancer guideline recommended adjuvant chemotherapy for patients aged <70 years with a pathological N+ status [14]. Furthermore, adjuvant chemotherapy was recommended in patients aged <70 years with a pathological N0 status in case of a tumor size ≥3.0 cm, a tumor size of 2–3 cm and grade 2–3, or a tumor size of 1–2 cm and grade 3. For patients aged ≤35 years, adjuvant chemotherapy was also considered in case of a tumor size >1 cm or ≤1 cm and grade 2–3. As regards to patients aged ≥70 years, no standard advice was provided due to lack of evidence for benefit of chemotherapy in this patient group [14].

The adjuvant chemotherapy regimen mostly consisted of 5 cycles of fluorouracil-epirubicin-cyclophosphamide (FEC), or 6 cycles of docetaxel/paclitaxel-adriamycin-cyclophosphamide (TAC) [14].

Adjuvant radiation therapy indications

Breast conserving therapy consisted of breast conserving surgery followed by whole breast radiotherapy, with a fractionation scheme equivalent to 25 × 2 Gy, 5 fraction per week [14]. A boost could be considered in patients aged <60 years or in case of focal irradicality. Chest wall irradiation following mastectomy was indicated in case of irradicality, invasion of pectoralis muscle or skin, or a pathological T3-4 status. Periclavicular radiation therapy (including breast or chest wall) was indicated in case of a pathological N2-3 status or a tumor-positive axillary top, with administration of 50 Gy fractionated irradiation [14].

Statistical analysis

Primary endpoint of our study is regional recurrence rate within 5 years. A regional recurrence was registered by the Netherlands Cancer Registry as an event in lymph nodes of ipsilateral axilla, infraclavicular region, intramammary, or in the internal mammary lymph node chain. Secondary endpoints are local recurrence rate, distant recurrence rate, disease-free survival, distant disease-free survival, and overall survival. A local recurrence was registered as an event in the ipsilateral breast (or overlying skin) with similar morphologic characteristics as the primary tumor. Events located elsewhere in the body were registered as distant recurrence. Employees of the Netherlands Cancer Registry consulted the treating physician in case there was doubt about the occurrence of a recurrence.

Disease-free survival was defined as the time interval from date of diagnosis to a local, regional or distant recurrence, or death from any cause, whichever occurred first. Distant disease-free survival was defined as the time interval from date of diagnosis to a distant recurrence, or death from any cause, whichever occurred first. Overall survival was defined as the time interval between date of diagnosis and December 31, 2014 or date of death from any cause. Patients who were alive and disease-free were censored at the last day of follow-up (December 31, 2014).

Descriptive categorical data are presented as proportions and absolute numbers. Continuous variables are presented as means with standard deviations. Kaplan–Meier method was used to estimate the event rates at 5 years of follow-up. Statistical analyses were performed using Statistical Package for the Social Sciences (SPSS), version 20.0 (IBM Corporation, Armonk, NY, USA). A p value of <0.05 was considered statistically significant.

Results

Patient demographics and tumor characteristics

A total of 2548 women with clinically T1-2N0 TNBC were identified from the Netherlands Cancer Registry. In this cohort, the mean age at diagnosis was 56 years (range 20–95), with 36 % of patients aged ≤50 years. Patients demographics and tumor characteristics are presented in Table 1. The majority of patients had a clinically T1 status (63.5 %) and a grade 3 tumor (73.6 %). Breast conserving therapy was performed in 63.7 %, a mastectomy in 29.9 %, mastectomy with adjuvant radiation therapy in 4.6 %, and lumpectomy-only in 1.8 %.

Table 1

Patient demographics and tumor characteristics

Characteristic	Value
Number of Patients	2548
Age
Mean (SD)	56 (14)
Range	20–95
Clinical T-stadium, n (%)
cT1	1618 (63.5)
cT2	930 (36.5)
Local treatment breast, n (%)
Breast conserving therapy	1624 (63.7)
Mastectomy	761 (29.9)
Mastectomy and radiotherapy	118 (4.6)
Lumpectomy-only	45 (1.8)
Axillary surgery, n (%)
SLNB only	1978 (77.6)
ALND	54 (2.1)
SLNB and completion ALND	508 (19.9)
No axillary surgery	8 (0.3)
Pathological T-stadium, n (%)
pT1	1405 (55.1)
pT2	1095 (43.0)
pT3	34 (1.3)
pT4	3 (0.1)
Unknown	11 (0.4)
Pathological N-stadium, n (%)
pN0	1929 (75.7)
pN0(i+)	72 (2.8)
pN1mi	115 (4.5)
pN1	313 (12.3)
pN2	64 (2.5)
pN3	27 (1.1)
Unknown	28 (1.1)
Tumor type, n (%)
Ductal	1275 (83.4)
Lobular	47 (3.1)
Other	207 (13.5)
Grade (Bloom–Richardson), n (%)
Grade 1	106 (4.2)
Grade 2	470 (18.4)
Grade 3	1876 (73.6)
Unknown	96 (3.8)

N number of cases, SD standard deviation, SLNB sentinel lymph node biopsy, ALND axillary lymph node dissection

The SLNB was performed in 2486 patients (97.6 %) and 54 patients (2.1 %), primarily underwent an ALND (Fig. 1). The SLN was negative in 1875 patients (75.4 %), not found in 11 (0.4 %), showed isolated tumor cells in 73 (2.9 %), micrometastasis in 117 (4.7 %), and macrometastasis in 392 patients (15.8 %). A completion ALND was performed in 508 patients. Final pathological lymph node status of all 2548 patients was pN0 in 78.5 %, pN1mi in 4.5 %, pN1 in 12.3 %, pN2 in 2.5 %, pN3 in 1.1 %, and pNx in 1.1 %.

Adjuvant chemotherapy was administered to 1534 patients (60 %). Administration of adjuvant chemotherapy per age category is presented in Table 2. In patients aged ≤70 years, 73 % received adjuvant chemotherapy.

Table 2

Administered adjuvant chemotherapy per age category

Age category	No chemotherapy	Chemotherapy	Total
20–30 year, n (%)	2 (3.3)	58 (96.7)	60 (2.4)
31–40 year, n (%)	23 (7.4)	286 (92.6)	309 (12.1)
41–50 year, n (%)	96 (17.2)	462 (82.8)	558 (21.9)
51–60 year, n (%)	191 (29.1)	465 (70.9)	656 (25.7)
61–70 year, n (%)	261 (50.5)	256 (49.5)	517 (20.3)
≥70 year, n (%)	441 (98.4)	7 (1.6)	448 (17.6)
Total	1014 (39.8)	1534 (60.2)	2548

Outcome

During a follow-up of 5 years, 328 patients experienced a solitary recurrence: 25 patients (1.0 %) a regional recurrence, 60 patients (2.4 %) a local recurrence, and 243 patients (9.5 %) a distant recurrence. Concomitant disease occurred in another 75 patients: a local and regional recurrence in 10 patients (0.4 %), a local and distant recurrence in 25 patients (1.0 %), a regional and distant recurrence in 28 patients (1.1 %), and a local, regional, and distant recurrence in 12 patients (0.5 %).

Median time to the detection of any recurrence was 1.7 years (range 0.1–5.0 years), and in 75 % of the patients the recurrence was detected within 3 years after breast cancer diagnosis (interquartile range (IQR) 1.0–2.8 years). Five-year disease-free survival, and distant disease-free survival was 78.7 and 80.5 %, respectively. Median follow-up for overall survival was 7.7 years (IQR 6.2-8.8), with a 5-year overall survival of 82.3 %, and 10-year overall survival of 72.2 %.

Regional recurrences

A total of 75 patients (2.9 %) experienced a regional recurrence in our cohort, of whom 25 (1.0 %) a solitary regional recurrence, and 50 (1.9 %) concomitant local and/or distant disease. Patient demographics and tumor characteristics at initial diagnosis of the 75 patients are presented in Table 3. An SLNB was performed for axillary staging after diagnosis in 74 patients, revealing no metastases in 37 patients (50 %), isolated tumor cells in two patients (3 %), micrometastasis in 5 patients (7 %), and macrometastasis in 24 patients (32 %). In two patients, the SLN was not found; in four patients, results were unknown; and in one patient, no SLNB was performed. A (completion) ALND was performed in 30 patients. Final pathological lymph node status was pN0 in 39 patients (52.0 %), pN0i+ in two patients (2.7 %), pN1mi in 5 patients (6.7 %), pN1 in 19 patients (25.3 %), pN2 in three patients (4.0 %), pN3 in two patients (2.7 %), and unknown in five patients. Adjuvant chemotherapy was administered to 45 patients.

Table 3

Characteristics of patients with a regional event diagnosed during follow-up

	Regional event
Number of events, %	75 (2.9)
Median time to event in years, range	1.6 (0.1–4.9)
Interquartile range time to event, years
25 %	0.8
75 %	2.5
Mean age at initial diagnosis, SD	54 (14.7)
Clinical T-status, n (%)
cT1	40 (53.3)
cT2	35 (46.7)
Local treatment breast, n (%)
BCT	37 (49.3)
Mastectomy	31 (41.3)
Mastectomy + RT	2 (2.7)
Lumpectomy	5 (6.7)
Axillary surgery, n (%)
SLNB only	45 (60.0)
ALND	1 (1.3)
SLNB and cALND	29 (38.7)
No axillary surgery	–
Chemotherapy, n (%)
Yes	45 (60.0)
No	30 (40.0)
Pathological T-stadium, n (%)
pT1	31 (41.3)
pT2	42 (56.0)
pT3	1 (1.3)
Unknown	1 (1.3)
Pathological N-stadium, n (%)
pN0	39 (52.0)
pN0(i+)	2 (2.7)
pN1mi	5 (6.7)
pN1	19 (25.3)
pN2	3 (4.0)
pN3	2 (2.7)
Unknown	5 (6.7)
Grade, n (%)
Grade 1	1 (1.3)
Grade 2	11 (14.7)
Grade 3	61 (81.3)
Unknown	1 (2.7)
Recurrences, n (%)
Regional	25 (33.3)
Regional and local	10 (13.3)
Regional and distant	28 (37.3)
Regional, local and distant	12 (16.0)

N number of cases, SD standard deviation, BCT breast conserving therapy, RT radiotherapy, SLNB sentinel lymph node biopsy, ALND axillary lymph node dissection, Grade according to modified Bloom–Richardson

The median time to the detection of the regional recurrence was 1.6 years (range 0.1–4.9). In 25 % of the patients, the regional recurrence was already detected within the first year after breast cancer diagnosis, and in 75 % within 2.5 years (IQR 0.8–2.5 years).

There were 16 deaths among the 25 patients with a solitary regional recurrence and 45 deaths in case of concomitant local and/or distant recurrence, resulting in a 5-year overall survival of 28.4 %. The median time to death was 3.6 years (range 0.3–9.8). No additional statistical analyses were performed given the small number of events.

Discussion

The aim of this study was to provide a nationwide overview on the occurrence of regional recurrences in patients with TNBC and a clinically T1-2N0 status, in the context of the randomized controlled trials investigating the safety of minimizing axillary staging and treatment. In this Dutch nationwide registry TNBC population, 2.9 % of the patients developed a regional recurrence during 5 years of follow-up. Most were detected within 3 years after diagnosis. Distant recurrences occurred more frequently, in 12 %. Regional recurrences represent only a minor part of the events that occur in TNBC.

In the present cohort of 2548 TNBC patients, all patients were staged as clinically T1-2N0. Preoperative staging included a negative axillary ultrasound, which is known to decrease the rate of extensive lymph node disease in particular [16, 17]. This resulted in a relatively favorable pathological N-status in our cohort, with pN0 in 78.5 %, pN1mi in 4.5 %, pN1 in 12.3 %, and pN2–3 in 3.6 %. The rate of lymph node positive disease in these TNBC patients seems to correspond to other breast cancer subtypes. Regardless of the receptor status, a cohort study of 12,113 patients with clinically T1-2N0 breast cancer, who were treated with breast conserving therapy, revealed pN0 in 79.8 %, pN1mi in 7.3 %, pN1 in 11.1 %, and pN2-3 in 1.7 % [17].

Several studies investigated the association between tumor subtype and nodal status, and showed that the incidence of lymph node metastases in TNBC is equal or even lower compared to ER-positive or HER2-positive tumors [18‐22]. TNBC is associated with similar characteristics that are related to lymph node involvement, such as younger age and higher tumor grade; though, there is no association between TNBC and lymphovascular invasion [2, 8, 19]. The study of Ugras et al. revealed that all breast cancer subtypes were independently associated with lymphovascular invasion (p < 0.0001), with TNBC having the lowest incidence of lymphovascular invasion, which might explain a lower incidence of node positivity in some cohorts [18, 22].

Main focus of our study was the occurrence of regional recurrences in TNBC. Only 25 patients (1.0 %) in our cohort experienced a solitary regional recurrence and 50 patients (1.9 %) experienced regional recurrence together with a local and/or distant event. In literature, one other study reported specifically on regional recurrence in TNBC. It concerned a prospective database review questioning the safety of breast conserving therapy in TNBC. This study included 1851 patients with stage I to III breast cancer who were treated with breast conserving therapy, of whom 234 patients had TNBC. They revealed a regional recurrence rate of 1.3 % at a median follow-up of 5 years in the TNBC group and 4.7 % local recurrences, which were comparable to the total patient group (1.1 % regional recurrences and 2.5 % local recurrences) [9]. Distant recurrence occurred in 9.0 % of patients with TNBC, compared to 3.6 % for all patients together. A significant difference for distant recurrence was found between TNBC and patients with a luminal A subtype (positive for ER or PR and negative for HER2) (p = 0.001).

No further studies have been published on regional recurrence in TNBC, although there have been several studies on local recurrence, more specifically comparing breast conserving therapy and mastectomy. These studies showed that there is a higher rate of local recurrence in TNBC, compared to other subtypes, without significant differences for type of local breast treatment [1, 9, 23, 24, 25]. However, in one study, the increased local recurrence rate for TNBC lost significance after adjustments for factors such as age, tumor size, and grade [9]. Local recurrence rates of 4.2–10 % are reported, which is slightly higher than in current study, presumably due to the fact that we included only clinically T1-2N0 patients [1, 9, 24, 25].

The median time to any recurrence in TNBC is short compared to other subtypes, and almost all events occur within 5 years after diagnosis [26, 27]. This is also the case in our cohort, where the median time to any recurrence was 1.7 years, with even 75 % of all events within 3 years after diagnosis.

The systemic treatment option for TNBC is, until now, limited to chemotherapy. In neoadjuvant chemotherapy trials, pathological complete response (PCR) rates of primary tumor and lymph nodes are reported in up to 40 % in the TNBC subtype [28‐32]. PCR provides prognostic information for TNBC as well as for HER2-positive (ER/PR negative) patients. A meta-analysis of Cortazar et al. evaluated 11,955 patients from neoadjuvant chemotherapy trials and showed a PCR in 34 % of TNBC patients [32]. Event-free survival and overall survival were improved in patients achieving PCR, with a hazard ratio of 0.24 (95 % CI 0.18–0.33) and 0.16 (95 % CI 0.11–0.25), respectively.

Adjuvant chemotherapy was administered to 60 % of patients in our cohort. Patients treated with neoadjuvant chemotherapy were not included. The indications for adjuvant chemotherapy have been expanded over the years. Comparison of the 2005 and current 2012 Dutch breast cancer guideline shows some changes in indications [14, 33]. Chemotherapy is now indicated in case of a primary tumor size >2 cm (vs. ≥3 cm), and 1–2 cm and tumor grade 2–3 (vs. 1–2 cm and tumor grade 3). Considering elderly, current Dutch guideline now considers chemotherapy for fit patients aged 70 years or older who are pathological lymph node positive. There further have been some changes in the regimen of adjuvant chemotherapy. Six cycles of TAC is still commonly administered in current practice, but FEC is nowadays combined with a taxane, and antracycline-based chemotherapy can be administered in combination with a taxane [33]. Preliminary research has shown that the addition of carboplatin to a taxane increases the PCR rate in TNBC, though no survival data are available yet [34]. Changements in indications and regimen of chemotherapy are likely to positively influence patients outcome.

Conclusion

Triple-negative clinically T1-2N0 breast cancer patients rarely develop a regional recurrence. Their disease-free survival is more threatened by distant recurrence, which affects their overall survival. Consequently, it seems justified to include triple-negative breast cancer patients in randomized controlled trials investigating the safety of minimizing axillary treatment.

Compliance with ethical standards

Conflict of interest

The authors declare that they have no conflict of interest.

Open AccessThis article is distributed under the terms of the Creative Commons Attribution-NonCommercial 4.0 International License (http://creativecommons.org/licenses/by-nc/4.0/), which permits any noncommercial use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made.

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Titel: Risk of regional recurrence in triple-negative breast cancer patients: a Dutch cohort study
verfasst von: Lori M. van Roozendaal
Leonie H. M. Smit
Gaston H. N. M. Duijsens
Bart de Vries
Sabine Siesling
Marc B. I. Lobbes
Maaike de Boer
Johannes H. W. de Wilt
Marjolein L. Smidt
Publikationsdatum: 25.03.2016
Verlag: Springer US
Erschienen in: Breast Cancer Research and Treatment / Ausgabe 3/2016
Print ISSN: 0167-6806
Elektronische ISSN: 1573-7217
DOI: https://doi.org/10.1007/s10549-016-3757-4

Springer Medizin

Risk of regional recurrence in triple-negative breast cancer patients: a Dutch cohort study

Abstract

Introduction