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Clinical and radiological predictors of nipple-areola complex involvement in breast cancer patients
European Journal of Cancer (2012) 48, 2311– 2318
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Clinical and radiological predictors of nipple-areola complex involvement in breast cancer patients Marta D’Alonzo e, Laura Martincich b, Nicoletta Biglia e, Alberto Pisacane c, Furio Maggiorotto a, Giovanni De Rosa f, Filippo Montemurro d, Franziska Kubatzki a, Piero Sismondi e, Riccardo Ponzone a,⇑ a
Division of Gynecological Oncology, Institute for Cancer Research and Treatment (IRCC) of Candiolo, Fondazione del Piemonte per l’Oncologia, Strada Provinciale 142, Km 3.95 – 10060 Candiolo, Turin, Italy b Division of Radiology, Institute for Cancer Research and Treatment (IRCC) of Candiolo, Fondazione del Piemonte per l’Oncologia, Strada Provinciale 142, Km 3.95 – 10060 Candiolo, Turin, Italy c Division of Pathology, Institute for Cancer Research and Treatment (IRCC) of Candiolo, Fondazione del Piemonte per l’Oncologia, Strada Provinciale 142, Km 3.95 – 10060 Candiolo, Turin, Italy d Academic Division of Medical Oncology, University of Turin, Institute for Cancer Research and Treatment (IRCC) of Candiolo, Fondazione del Piemonte per l’Oncologia, Strada Provinciale 142, Km 3.95 – 10060 Candiolo, Turin, Italy e Academic Division of Gynecological Oncology, University of Turin, A.O. Ordine Mauriziano, Largo Turati 62, 110128 Turin, Italy f Division of Pathology, A.O. Ordine Mauriziano, Largo Turati 62, 110128 Turin, Italy
Available online 28 May 2012
KEYWORDS Breast cancer Nipple-areola complex sparing mastectomy Magnetic resonance Mammography
Abstract Introduction: Nipple-areola sparing mastectomy (NSM) is increasingly used in patients with non-locally advanced breast carcinoma. Literature data on the preoperative assessment of the nipple-areola complex (NAC) are inconsistent. Patients and methods: Out of 1359 patients submitted to total mastectomy between 2001 and 2010, we selected 61 patients whose pre-operative mammogram (MX) was available (MX group) and 39 patients who underwent preoperative breast magnetic resonance imaging (magnetic resonance imaging (MRI) group). The rate of NAC involvement, the value of MX and MRI to predict NAC involvement and the performance of the Schecter’s and Loewn’s algorithms for the prediction of NAC involvement were evaluated. Results: In the combined MX and MRI groups, NAC involvement was found in 14% of the cases. At univariate analysis, tumour stage (p value: 0.03), central tumour location (p value: 0.004), presence of NAC retraction (p value: 0.001) and tumour–NAC distance (p value: 0.006) were associated with NAC involvement, but only the latter parameter retained statistical significance at multivariate analysis (p value: 0.05). Tumour–NAC distance was a key predictor of NAC involvement, with a negative predictive value of 94% for MX and of 100% for MRI when the cut-off was set at 10 mm. Overall, the performance of Schecter’s
⇑ Corresponding author: Tel.: +39 011 9933036; fax: +39 011 9933440.
E-mail address: [email protected] (R. Ponzone). 0959-8049/$ - see front matter Ó 2012 Elsevier Ltd. All rights reserved. http://dx.doi.org/10.1016/j.ejca.2012.04.017
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and Loewn’s algorithms was respectively lower and similar as compared to the original series. Conclusions: Occult tumour involvement of the NAC is detected in a minority of breast cancer patients submitted to mastectomy. A tumour–NAC distance P10 mm by MRI may help select patients candidate to NSM. Ó 2012 Elsevier Ltd. All rights reserved.
1. Introduction Nipple-areola sparing mastectomy (NSM) is currently considered as a possible alternative to skin sparing mastectomy (SSM) in selected breast cancer patients undergoing immediate breast reconstruction.1,2 The oncological safety of NSM, although not formally proven, is supported by a convincing rationale and also by many retrospective3–8 and prospective clinical data.9 In the absence of randomised clinical trials, whose implementation is often difficult in surgery,10 the introduction of NSM must be regulated and carried out gradually. This is essential to minimise the possible negative effects in terms of surgical and oncological risks. A crucial issue is the possibility to predict preoperatively tumour involvement of the nipple-areola complex (NAC) in order to select which patients may be candidates to a NSM.11 The risk of NAC involvement has been assessed in several retrospective analyses of large datasets, but the issue is of considerable interest because literature data on the best clinical and radiological predictors are inconsistent.1 In the current study, we analysed a mono-institutional series of total mastectomies without NAC preservation with the following aims: (A) to estimate the actual rate of NAC involvement; (B) to assess the value of mammography (MX) and magnetic resonance imaging (MRI) in predicting NAC involvement; (C) to validate the performance of existing models for the prediction of NAC involvement. 2. Patients and methods 2.1. Patient selection All patients submitted to total mastectomy from January 2000 to July 2010 were searched in the institutional database. Out of 1359 patients retrieved, we selected those who had a scheduled appointment at the follow up clinic within the next 4 weeks. This selection was decided in order to acquire the radiograms in the shorter and most efficient way. In fact, although all patients underwent MX before surgery, we had no copy available at the Institute. Overall, 78 out of 147 patients contacted brought their original MX (MX group). The second group included all patients submitted to mastectomy from January 2009 to March 2010 who underwent preoperative MRI of the breast (54 out of 179) at the Institute (MRI group). This limited time-frame was
chosen to uniform the technique of image acquisition and processing. Indications for performing preoperative MRI were: age below 40 years of age, lobular histology, suspicion of multifocal disease, or equivocal MX findings. No overlap existed in the patients’ composition of the two groups. Patients with inflammatory breast cancer, clinically evident tumour involvement of the NAC, Paget’s disease and phylloides tumour were excluded, as well as all patients with a negative and/or low quality preoperative MX or MRI or those who underwent preoperative chemotherapy. Patients with skin and/or nipple retraction were not excluded because this does not necessarily imply tumour infiltration. All clinical and pathological information such as age, menopausal status, tumour histology, location (central versus peripheral), multifocality and/or skin involvement were obtained through a prospectively maintained institutional database. 2.2. Radiological evaluation All examinations were blindly reviewed by a radiologist (L.M.) with 15 years of experience in breast imaging. In the MX group and MRI groups, 61/78 (78.2%) and 39/54 (72.2%) cases were enrolled respectively. The remaining cases were excluded because either the quality of the images was too low (six MX and three MRI), or both (cranio-caudal and oblique) views were not available (four MX), or the lesion was not visible (six MX and one MRI), or the patient underwent preoperative chemotherapy (nine MRI) or the final diagnosis was phylloides tumour (one MX) or Paget’s disease (two MRI). MX was performed by two standard views, craniocaudal and mediolateral oblique, either with analogic or digital technique. The diameter of the lesion was defined as the maximum extension of suspicious opacity, architectural distortion and/or suspicious microcalcifications. In the case of bifocal, multifocal or multicentric lesions, these were considered as a single mass and the reference measure reflected the whole area occupied in the breast (Fig. 1). The distance between tumour and NAC (tumour–NAC distance) was defined as the minimum distance between the base of NAC and the nearest margin of the lesion. For both views, two measures were taken parallel to the nipple and to the ducts respectively and the shorter was chosen as the reference distance (Fig. 2). MRI examinations were acquired with a 1.5 T equipment (HDx Signa Excite, GE HealthCare,
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formed according to an institutional protocol with conventional haematoxylin-eosin stained sections. The NAC was routinely inspected in all mastectomies, including a single sagittal section through the nipple. The subareolar margin was dissected immediately on the fresh specimen to reproduce a surgical margin at 4–5 mm from the base of the nipple. The NAC was considered involved in case of invasive ductal/lobular carcinoma and/or ductal carcinoma in situ within the subareolar margin, but not in the case of presence of lobular carcinoma in situ/lobular intraepithelial neoplasia. The pathological report was retrieved for all patients from the MX and MRI groups to examine whether NAC involvement was explicitly mentioned or not. For 13 dubious cases, the original pathological slides were blindly reviewed by two pathologists with specific experience on breast pathology (A.P. and G.D.R.) unaware of imaging data. Fig. 1. The total diameter of a multicentric lesion was measured drawing a line (a) between the external edge of the two most periferic lesions.
Fig. 2. The distance between the tumour and the nipple-areola complex (NAC) was measured both as a line parallel to the ducts (a) and parallel to the nipple axis (b). The shortest measure was taken as a reference.
2.4. Prediction of NAC involvement The likelihood of NAC involvement was calculated by applying the algorithms proposed by Schecter et al.13 and Loewen et al.14 (Fig. 3). The sensitivity (Se), specificity (Sp), positive predictive value (PPV), negative predictive value (NPV) and accuracy (Acc) in predicting NAC involvement was calculated for all algorithms. Algorithms were tested using the MX and MR data separately. Receiving operating curves (ROC) were constructed to detect the best cut-off point to allow the optimal balance between Se and Sp either by MX or MRI. 2.5. Statistical analysis
Milwaukee) and dedicated phased-array 8-channel coil, using a dynamic technique (DCE-MRI) following the recommended requirements.12 Multiplanar reconstructions (MPR) from subtracted images (postcontrast series–precontrast acquisition) were used to assess the diameter of the lesion, which was defined as the maximum extent of suspicious enhancement. As for Mx, in the case of bifocal, multifocal or multicentric lesions, these were considered as a single mass and the reference measure reflected the whole area occupied in the breast. A conventional measure of the larger tumour foci was also recorded in this group. The tumour NAC-distance was measured by electronic calipers, on both axial and sagittal Maximum Intensity Projection (MIP) images. The distance between lesion and NAC was defined as the minimum distance between the base of the NAC and the nearest margin of the lesion. 2.3. Histopathological evaluation In the original pathological report, gross and histologic assessment of the mastectomy specimens were per-
Statistical significance was set at p values < 0.05 with two-tailed test. The quantitative variables were compared with the Pearson chi-square test or Fisher’s exact test. Qualitative variables were compared using the analysis of variance. The normality of variables was tested by the Kolmogorov–Smirnov procedure. Variables not normally distributed were analysed using the non-parametric Mann–Whitney U test. Multivariate analysis was performed using the logistic regression model. Statistical analysis was performed with SPSS for Windows. 3. Results 3.1. Correlation between clinical pathologic factors and NAC involvement At histopathological analysis, 14 out of 100 cases showed tumour cells in the NAC. At univariate analysis, menopausal status, tumour histology, tumour grade, immunohistochemical characteristics and multifocality did not influence NAC status. Although positive axillary
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M. D’Alonzo et al. / European Journal of Cancer 48 (2012) 2311–2318 Schecter’ algorithm NAC involvement score = (3.663 x size factor) + (2.978 x stage factor) - (.808 x distance) - 1.465
The size factor was tumor size < 1.0 cm versus tumor size ≥1.0 cm. The stage factor was stage ≤ 2B versus stage ≥ 3A. Distance was the tumor - NAC distance. NAC involvement score ≥ - 0.3665 was interpreted as NAC positive. NAC involvement score ≤ - 0.3665 was interpreted as NAC negative
Loewen’s algorithm Nipple involvement (yes/no) = -.4613 - (.3711 x distance)
Distance is the greater of cranial-caudal or medial-lateral-oblique distance. If the value for nipple involvement is less than .10, nipple involvement = no; if the value for nipple involvement is .10 or greater, nipple involvement = yes. Fig. 3. Algorithms for the prediction of occult nipple-areola complex tumour involvement.
lymph node status and larger tumour size were more common in the NAC positive group, the difference did not reach statistical significance (p value: 0.09 and 0.08, respectively). Conversely, tumour stage was positively associated with NAC involvement (p value: 0.03) (Table 1). Tumour–NAC distance showed the highest association with NAC involvement (p value: 0.006), as well as two closely related parameters such as central tumour location (p value: 0.004) and presence of NAC retraction (p value: 0.001). Since both the measurements of tumour size and tumour–NAC distance may vary with different imaging techniques, the analysis was performed separately for the MX and MRI groups. In the MX group, all significant parameters at the combined MX + MRI analysis lost their statistical significance. In contrast, in the MRI group both lesion size (p value: 0.008) and tumour–NAC distance (0.009) retained their statistical significance (Table 2). Tumour–NAC distance remained a significant predictor of NAC involvement by setting the cut off at 5 mm (p value: 0.003), 10 mm (p value: 0.002), 20 mm (p value: 0.029). We also performed a multivariate analysis which showed that a tumour– NAC distance 610 mm was the only factor independently associated with NAC involvement (relative risk: 9.55; p value 0.05) (data not shown). 3.2. Prediction of NAC involvement by tumour–NAC distance Tumour–NAC distance resulted in a key predictor of NAC involvement. Overall, the area under the curve (AUC) of the ROC curve was 0.782 (Fig. 4), and was larger for MRI than for Mx (0.888 and 0.677 respectively). The 10 mm cut-off value allowed the best balance between Se and Sp, being associated with a NPV for NAC involvement of 94% and 100% with MX and MRI respectively (Table 3).
3.3. Validation of the algorithms The results from our series were used to validate the algorithms by Schecter et al.13 and Loewen et al.14 Measurements obtained with MRI and MX were analysed separately (Table 4). Overall, the performance of Schecter’s algorithm13 was inferior as compared to the original series due to its very low Sp (35% and 22% for MX and MRI respectively), despite its good Se (86% and 100% for MX and MRI respectively). Conversely, we were able to reproduce Loewn’s original results (Se 57%, Sp 72% for MX) and even improve their overall performance when MRI was used for measuring tumour–NAC distance (Se 100%; Sp 69%).14 4. Discussion Occult involvement of the NAC is reported in 0–58% of mastectomy specimens.1 Larger series including at least 100 patients show lower variability of occult NAC involvement (5.6–26.4%),1 and are consistent with our finding (14%). The pathological protocol for NAC evaluation, as well as pathological data collection, have a major role in determining the rate of NAC involvement. In many series, the NAC was assessed exclusively through the consultation of pathological reports. According to Schecter et al.13 this is not appropriate since only 4 cases of NAC involvement were identified by simply checking medical records in a series of 48 mastectomies, with further 9 cases identified after a pathological review of all cases. At our institution the pathological protocol requires the inspection of the NAC in all mastectomy specimens. Therefore, whenever the report contained a description of the NAC status (free of or involved with cancer), we considered the data as reliable. Only if the NAC status was not clearly stated, we asked the pathologists to review the slides. In our series, this procedure
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Table 1 Correlation between nipple–areola complex (NAC) involvement and clinical-pathological parameters (univariate analysis). N
NAC involvement
p Value
Yes (%)
No (%)
Menopausal status Premenopausal Postmenopausal
55 45
5 (35.7) 9 (64.3)
50 (58.1) 36 (41.9)
0.118
Tumor type In situ Invasive
19 81
2 (14.3) 12 (85.7)
17 (19.8) 69 (80.2)
1.000
Tumor histotype (invasive) Ductal invasive Lobular invasive Other
59 17 5
9 (75.0) 2 (16.6) 1 (8.4)
50 (72.5) 15 (21.7) 4 (5.8)
0.924
Tumor grade 1 2 3
9 33 58
0 4 (28.6) 10 (71.4)
9 (10.5) 29 (33.7) 48 (55.8)
0.356
Tumor central location Yes No
37 63
10 (71.4) 4 (28.6)
27 (31.4) 59 (68.6)
0.004
Nipple retraction Yes No
11 89
6 (42.9) 8 (57.1)
5 (5.8) 81 (94.2)
0.001
Stage I–II III–IV
90 10
10 (71.4) 4 (28.6)
80 (93.0) 6 (7.0)
0.032
Multifocality at imaging Yes No
17 83
1 (7.1) 13 (92.9)
16 (18.6) 70 (81.4)
0.453
Multifocality at pathology Yes No
41 59
5 (35.7) 9 (64.3)
36 (41.9) 50 (58.1)
0.665
53.6 52.6
41.9 41.5
0.081 0.099
Mean tumor diameter (mm) (a) (b)
100 100
Mean tumor – NAC distance (mm)
21.3
7.9
23.4
0.006
Nodal status Positive Negative
51 49
10 (71.4) 4 (28.6)
41 (47.7) 54 (52.3)
0.099
Oestrogen receptora Positive Negative
86 10
11 (84.6) 2 (15.4)
75 (90.4) 8 (9.6)
0.621
Progesterone receptor Positive Negative
82 15
10 (76.9) 3 (23.1)
72 (85.7) 12 (14.3)
0.418
Ki-67b Positive Negative
57 35
8 (72.7) 3 (27.3)
49 (60.5) 32 (39.5)
0.523
HER-2 (Herceptest) 0 1+ 2+ 3+
30 26 21 11
7 3 2 1
23 23 19 10
0.574
(53.8) (23.1) (15.4) (7.7)
(30.3) (30.3) (25.0) (13.2)
(a) In multifocal tumour the diameter of the whole area occupied in the breast was used as a reference; (b) in multifocal tumours the diameter of the largest lesion was used as a reference. a Negative: 0%, positive P1% of stained cells. b Negative: <20%, positive P20% of stained cells.
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Table 2 Correlation between nipple-areola complex (NAC) involvement and clinical parameters measured by mammography or magnetic resonance. N
NAC involvement
p Value
Yes (%)
No (%)
13 48
0 7 (100)
13 (24.1) 41 (75.9)
0.328
4 35
1 (14.3) 6 (85.7)
3 (9.4) 29 (90.6)
0.563
Mean tumor diameter (mm) MX MRIa MRIb
61 39 39
53.1 54.0 52.0
46.6 33.9 32.8
0.522 0.008 0.010
Mean tumor – NAC distance (mm) MX MRI
61 39
13.7 2.0
22.7 24.7
0.250 0.009
Multifocality at imaging MX Yes No MRI Yes No
Notes: MX: mammography; MRI: magnetic resonance. a In multifocal tumours the diameter of the whole area occupied in the breast was used as a reference. b In multifocal tumours the diameter of the largest lesion was used as a reference.
Table 3 Prediction of NAC involvement according to different cut-off values of the tumour–nipple-areolar complex (NAC) distance. Cut-off
Type of imaging
Sp%
PPV%
65 mm
MX MRI
Se% 57 86
78 78
25 46
NPV% 93 96
ACC% 75 79
610 mm
MX MRI
71 100
63 66
20 39
94 100
64 72
620 mm
MX MRI
71 100
46 50
15 30
93 100
49 59
SE: sensitivity; SP specificity; PPV: positive predictive value; NPV: negative predictive value; ACC: accuracy; MX: mammography; MRI: magnetic resonance.
Table 4 Prediction of nipple-areola complex involvement: validation of existing algorithms.
Fig. 4. Tumour–nipple-areola complex (NAC) distance in cm for the prediction of NAC involvement: Receiving Operating Characteristic (ROC) curve.
identified 2 additional positive NAC (from 12 to 14) out of 13 cases re-evaluated. In our study, NAC involvement was defined by the presence of invasive carcinoma and/or ductal carcinoma in situ at the subareolar margin. This boundary has clinical relevance as it represents the surgical plane of dissection of a NAC-sparing mastectomy. We used a 4–5 mm cut-off for our analysis since this is the mean
Se%
Sp%
PPV%
NPV%
ACC%
Schecter’s algorithm MX MRI Original series
86 100 92
35 22 77
15 22 –
95 100 93
41 36 83
Loewen’s algorithm MX MRI Original series
57 100 82
72 69 62
21 41 20
93 100 97
70 74 –
SE: sensitivity; SP specificity; PPV positive predictive value; NPV: negative predictive value; ACC: accuracy; MX: mammography; MRI: magnetic resonance.
thickness of the skin flaps of a mastectomy performed at the level of the superficial fascia dividing the subcutaneous fat from the breast glandular tissue.15 This was a conservative decision, since recent data1and our own
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experience16 suggest that when performing a NAC sparing mastectomy the dissection plane can be conducted even closer to the base of the nipple, including the whole duct bundle, with a reasonably low risk of necrosis. Our low rate of NAC positivity may depend by the pathological protocol which did not require serial coronal sections of the nipple and by the exclusion of lobular carcinoma in situ (LCIS) from our criteria of NAC involvement. Actually, in studies17,18 that include LCIS, the incidence of malignant NAC involvement is significantly higher than the average (30–58%). We believe LCIS should not be regarded as evidence of NAC involvement since it cannot be considered a true cancer lesion and does not mandate further surgical excision when detected at the surgical margins. Tumour size and tumour distance from the NAC show respectively a positive and negative correlation with NAC involvement in most studies.11,18,19 We showed that the risk of NAC involvement is strongly related to tumour–NAC distance and also to tumour size when measured by MRI. In order to allow external comparison, tumour size for multifocal tumours was measured either considering the separated tumour foci as single mass or as the diameter of the largest lesion, without any significant change of the results (Tables 1 and 2). Conversely, tumour size measured by Mx showed only a non-significant correlation with NAC involvement, probably because it mainly reflects the invasive component of the tumour, while MRI often includes also the surrounding non-invasive component of the disease. According to some authors,11 ductal carcinoma in situ is the most frequent type of cancer detected in the NAC and thus MRI measurement may better reflect the true risk of NAC involvement. Furthermore, in contrast with Schecter et al.,13 but in agreement with others,18,20 we found that NAC involvement was significantly related to central location of the lesion, skin and/or nipple retraction and stage of disease. We validated two dedicated algorithms in order to identify those patients whose risk is so low that a NAC sparing mastectomy may be justified. To this aim we tested separately the performance of MX and MRI in the models. In the algorithm by Schecter et al.,13 size, distance and tumour stage independently predicted NAC involvement, while Loewen et al. used only distance in their model. By entering our data in the Schecter’s algorithm, we found significantly lower Sp, PPV and Acc.13 This was not influenced by our decision to measure multifocal lesions as a single mass; in fact the ‘size factor’ of the Schecter’s algorithm is set at 1 cm and all of our multifocal tumours were larger both considering the diameter of the larger lesion or the diameter of the area occupied by the cancer foci. Conversely, we obtained values of Se, Sp, PPV and NPV comparable to that achieved by Loewen et al. (Table 3).14 By analysing the data separately according to the type of imaging used, we found
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that MRI consistently outperformed Mx as far as Se, NPV and PPV were concerned in both models,13,14 while Sp was significantly better for Mx as compared to MRI only in the Schechter’s model. In a recent comprehensive review of the literature,2 tumour size 65 cm and tumour–nipple distance P2 cm are proposed as inclusion criteria for performing a NAC sparing mastectomy, provided that retroareolar ducts do no show tumour involvement at pathological examination. Since our data suggest that tumour–NAC distance is the most important predictive factor, we tried to define the best cut-off to predict a low risk of NAC involvement. We found that the best compromise between specificity and sensitivity was obtained by setting the cut-off at 10 mm. Indeed, this cut-off at MRI was the only factor independently associated with NAC involvement at multivariate analysis and would have allowed to exclude NAC involvement in all cases of our series. Literature data on the best cut-off values of tumour–NAC distance are variable; only the study of Sacchini et al. support our 1 cm cut-off value,21 while most authors suggest that it should be set at P2 cm.3,11,22 Limitations of our study are mainly derived from its retrospective design. In order to limit selection biases, we prospectively included those patients with a scheduled appointment at the clinic, but we could not exclude image based- selection and study examination biases. Readerorder biases were avoided since the radiologist and pathologists were unaware of the pathological and radiological report respectively. Unfortunately, a proper comparison between MX and MRI was not possible in our study since only a few patients had both exams performed. In conclusion, occult tumour involvement of the NAC is detected in a minority of breast cancer patients submitted to mastectomy. Although, several parameters may predict the likelihood of NAC involvement, our data suggest that multiparametric models do not increase the overall accuracy obtained by the measurement of tumour–NAC distance. A distance of at least 10 mm, especially if measured by MRI, allows optimal discriminative power between cases at high versus low likelihood of NAC involvement and can virtually exclude NAC involvement. Caution is required in interpreting our data, since numbers are small and the study may be underpowered to detect significant differences. Furthermore, only prospective studies of NAC-sparing mastectomy in breast cancer patients will be able to assess the best parameters to predict NAC involvement and long term follow up data will be required to assess the oncological safety of the procedure. In the meantime, it appears that the decision to preserve the NAC in breast cancer patients undergoing mastectomy may be guided by MRI measurement of tumour–NAC distance in addition to the intraoperative pathological evaluation of the retroareolar ducts.
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Conflict of interest statement None declared. References 1. Rusby JE, Smith BL, Gui GP. Nipple-sparing mastectomy. Br J Surg 2010;97:305–16. 2. Garcia-Etienne CA, Cody Iii 3rd HS, Disa JJ, Cordeiro P, Sacchini V. Nipple-sparing mastectomy: initial experience at the Memorial Sloan-Kettering Cancer Center and a comprehensive review of literature. Breast J 2009;15:440–9. 3. Gerber B, Krause A, Dieterich M, Kundt G, Reimer T. The oncological safety of skin sparing mastectomy with conservation of the nipple-areola complex and autologous reconstruction: an extended follow-up study. Ann Surg 2009;249:461–8. 4. Petit JY, Veronesi U, Orecchia R, et al. Nipple sparing mastectomy with nipple areola intraoperative radiotherapy: one thousand and one cases of a five years experience at the European institute of oncology of Milan (EIO). Breast Cancer Res Treat 2009;117:333–8. 5. Lim W, Ko BS, Kim HJ, et al. Oncological safety of skin sparing mastectomy followed by immediate reconstruction for locally advanced breast cancer. J Surg Oncol 2010;102:39–42. 6. Jensen JA, Orringer JS, Giuliano AE. Nipple-sparing mastectomy in 99 patients with a mean follow-up of 5 years. Ann Surg Oncol 2011;18:1665–70. 7. Maxwell GP, Storm-Dickerson T, Whitworth P, Rubano C, Gabriel A. Advances in nipple-sparing mastectomy: oncological safety and incision selection. Aesthet Surg J 2011;31:310–9. 8. Nava MB, Ottolenghi J, Pennati A, et al. Skin/nipple sparing mastectomies and implant-based breast reconstruction in patients with large and ptotic breast: Oncological and reconstructive results. Breast 2011 [Epub ahead of print]. 9. Benediktsson KP, Perbeck L. Survival in breast cancer after nipple-sparing subcutaneous mastectomy and immediate reconstruction with implants: a prospective trial with 13 years median follow-up in 216 patients. Eur J Surg Oncol 2008;34:143–8. 10. Gurusamy KS, Gluud C, Nikolova D, Davidson BR. Assessment of risk of bias in randomized clinical trials in surgery. Br J Surg 2009;96:342–9.
11. Brachtel EF, Rusby JE, Michaelson JS, et al. Occult nipple involvement in breast cancer: clinicopathologic findings in 316 consecutive mastectomy specimens. J Clin Oncol 2009;27: 4948–54. 12. Sardanelli F, Boetes C, Borisch B, et al. Magnetic resonance imaging of the breast: recommendations from the EUSOMA working group. Eur J Cancer 2010;46:1296–316. 13. Schecter AK, Freeman MB, Giri D, Sabo E, Weinzweig J. Applicability of the nipple-areola complex-sparing mastectomy: a prediction model using mammography to estimate risk of nippleareola complex involvement in breast cancer patients. Ann Plast Surg 2006;56:498–504. 14. Loewen MJ, Jennings JA, Sherman SR, et al. Mammographic distance as a predictor of nipple-areola complex involvement in breast cancer. Am J Surg 2008;195:391–4. 15. Carlson GW. Skin sparing mastectomy: anatomic and technical considerations. Am Surg 1996;62:151–5. 16. Rivolin A, Kubatzki F, Marocco F, et al. Nipple-areola complex sparing mastectomy with periareolar pexy for breast cancer patients with moderately ptotic breasts. J Plast Reconstr Aesthet Surg 2012;65:296–303. 17. Lagios MD, Gates EA, Westdahl PR, Richards V, Alpert BS. A guide to the frequency of nipple involvement in breast cancer. A study of 149 consecutive mastectomies using a serial subgross and correlated radiographic technique. Am J Surg 1979;138: 135–42. 18. Menon RS, van Geel AN. Cancer of the breast with nipple involvement. Br J Cancer 1989;59:81–4. 19. Simmons RM, Brennan M, Christos P, King V, Osborne M. Analysis of nipple/areolar involvement with mastectomy: can the areola be preserved? Ann Surg Oncol 2002;9:165–8. 20. Morimoto T, Komaki K, Inui K, et al. Involvement of nipple and areola in early breast cancer. Cancer 1985;55:2459–63. 21. Sacchini V, Pinotti JA, Barros AC, et al. Nipple-sparing mastectomy for breast cancer and risk reduction: oncologic or technical problem? J Am Coll Surg 2006;203:704–14. 22. Vlajcic Z, Zic R, Stanec S, Lambasa S, Petrovecki M, Stanec Z. Nipple-areola complex preservation: predictive factors of neoplastic nipple-areola complex invasion. Ann Plast Surg 2005;55: 240–4.
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Clinical and radiological predictors of nipple-areola complex involvement in breast cancer patients Marta D’Alonzo e, Laura Martincich b, Nicoletta Biglia e, Alberto Pisacane c, Furio Maggiorotto a, Giovanni De Rosa f, Filippo Montemurro d, Franziska Kubatzki a, Piero Sismondi e, Riccardo Ponzone a,⇑ a
Division of Gynecological Oncology, Institute for Cancer Research and Treatment (IRCC) of Candiolo, Fondazione del Piemonte per l’Oncologia, Strada Provinciale 142, Km 3.95 – 10060 Candiolo, Turin, Italy b Division of Radiology, Institute for Cancer Research and Treatment (IRCC) of Candiolo, Fondazione del Piemonte per l’Oncologia, Strada Provinciale 142, Km 3.95 – 10060 Candiolo, Turin, Italy c Division of Pathology, Institute for Cancer Research and Treatment (IRCC) of Candiolo, Fondazione del Piemonte per l’Oncologia, Strada Provinciale 142, Km 3.95 – 10060 Candiolo, Turin, Italy d Academic Division of Medical Oncology, University of Turin, Institute for Cancer Research and Treatment (IRCC) of Candiolo, Fondazione del Piemonte per l’Oncologia, Strada Provinciale 142, Km 3.95 – 10060 Candiolo, Turin, Italy e Academic Division of Gynecological Oncology, University of Turin, A.O. Ordine Mauriziano, Largo Turati 62, 110128 Turin, Italy f Division of Pathology, A.O. Ordine Mauriziano, Largo Turati 62, 110128 Turin, Italy
Available online 28 May 2012
KEYWORDS Breast cancer Nipple-areola complex sparing mastectomy Magnetic resonance Mammography
Abstract Introduction: Nipple-areola sparing mastectomy (NSM) is increasingly used in patients with non-locally advanced breast carcinoma. Literature data on the preoperative assessment of the nipple-areola complex (NAC) are inconsistent. Patients and methods: Out of 1359 patients submitted to total mastectomy between 2001 and 2010, we selected 61 patients whose pre-operative mammogram (MX) was available (MX group) and 39 patients who underwent preoperative breast magnetic resonance imaging (magnetic resonance imaging (MRI) group). The rate of NAC involvement, the value of MX and MRI to predict NAC involvement and the performance of the Schecter’s and Loewn’s algorithms for the prediction of NAC involvement were evaluated. Results: In the combined MX and MRI groups, NAC involvement was found in 14% of the cases. At univariate analysis, tumour stage (p value: 0.03), central tumour location (p value: 0.004), presence of NAC retraction (p value: 0.001) and tumour–NAC distance (p value: 0.006) were associated with NAC involvement, but only the latter parameter retained statistical significance at multivariate analysis (p value: 0.05). Tumour–NAC distance was a key predictor of NAC involvement, with a negative predictive value of 94% for MX and of 100% for MRI when the cut-off was set at 10 mm. Overall, the performance of Schecter’s
⇑ Corresponding author: Tel.: +39 011 9933036; fax: +39 011 9933440.
E-mail address: [email protected] (R. Ponzone). 0959-8049/$ - see front matter Ó 2012 Elsevier Ltd. All rights reserved. http://dx.doi.org/10.1016/j.ejca.2012.04.017
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and Loewn’s algorithms was respectively lower and similar as compared to the original series. Conclusions: Occult tumour involvement of the NAC is detected in a minority of breast cancer patients submitted to mastectomy. A tumour–NAC distance P10 mm by MRI may help select patients candidate to NSM. Ó 2012 Elsevier Ltd. All rights reserved.
1. Introduction Nipple-areola sparing mastectomy (NSM) is currently considered as a possible alternative to skin sparing mastectomy (SSM) in selected breast cancer patients undergoing immediate breast reconstruction.1,2 The oncological safety of NSM, although not formally proven, is supported by a convincing rationale and also by many retrospective3–8 and prospective clinical data.9 In the absence of randomised clinical trials, whose implementation is often difficult in surgery,10 the introduction of NSM must be regulated and carried out gradually. This is essential to minimise the possible negative effects in terms of surgical and oncological risks. A crucial issue is the possibility to predict preoperatively tumour involvement of the nipple-areola complex (NAC) in order to select which patients may be candidates to a NSM.11 The risk of NAC involvement has been assessed in several retrospective analyses of large datasets, but the issue is of considerable interest because literature data on the best clinical and radiological predictors are inconsistent.1 In the current study, we analysed a mono-institutional series of total mastectomies without NAC preservation with the following aims: (A) to estimate the actual rate of NAC involvement; (B) to assess the value of mammography (MX) and magnetic resonance imaging (MRI) in predicting NAC involvement; (C) to validate the performance of existing models for the prediction of NAC involvement. 2. Patients and methods 2.1. Patient selection All patients submitted to total mastectomy from January 2000 to July 2010 were searched in the institutional database. Out of 1359 patients retrieved, we selected those who had a scheduled appointment at the follow up clinic within the next 4 weeks. This selection was decided in order to acquire the radiograms in the shorter and most efficient way. In fact, although all patients underwent MX before surgery, we had no copy available at the Institute. Overall, 78 out of 147 patients contacted brought their original MX (MX group). The second group included all patients submitted to mastectomy from January 2009 to March 2010 who underwent preoperative MRI of the breast (54 out of 179) at the Institute (MRI group). This limited time-frame was
chosen to uniform the technique of image acquisition and processing. Indications for performing preoperative MRI were: age below 40 years of age, lobular histology, suspicion of multifocal disease, or equivocal MX findings. No overlap existed in the patients’ composition of the two groups. Patients with inflammatory breast cancer, clinically evident tumour involvement of the NAC, Paget’s disease and phylloides tumour were excluded, as well as all patients with a negative and/or low quality preoperative MX or MRI or those who underwent preoperative chemotherapy. Patients with skin and/or nipple retraction were not excluded because this does not necessarily imply tumour infiltration. All clinical and pathological information such as age, menopausal status, tumour histology, location (central versus peripheral), multifocality and/or skin involvement were obtained through a prospectively maintained institutional database. 2.2. Radiological evaluation All examinations were blindly reviewed by a radiologist (L.M.) with 15 years of experience in breast imaging. In the MX group and MRI groups, 61/78 (78.2%) and 39/54 (72.2%) cases were enrolled respectively. The remaining cases were excluded because either the quality of the images was too low (six MX and three MRI), or both (cranio-caudal and oblique) views were not available (four MX), or the lesion was not visible (six MX and one MRI), or the patient underwent preoperative chemotherapy (nine MRI) or the final diagnosis was phylloides tumour (one MX) or Paget’s disease (two MRI). MX was performed by two standard views, craniocaudal and mediolateral oblique, either with analogic or digital technique. The diameter of the lesion was defined as the maximum extension of suspicious opacity, architectural distortion and/or suspicious microcalcifications. In the case of bifocal, multifocal or multicentric lesions, these were considered as a single mass and the reference measure reflected the whole area occupied in the breast (Fig. 1). The distance between tumour and NAC (tumour–NAC distance) was defined as the minimum distance between the base of NAC and the nearest margin of the lesion. For both views, two measures were taken parallel to the nipple and to the ducts respectively and the shorter was chosen as the reference distance (Fig. 2). MRI examinations were acquired with a 1.5 T equipment (HDx Signa Excite, GE HealthCare,
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formed according to an institutional protocol with conventional haematoxylin-eosin stained sections. The NAC was routinely inspected in all mastectomies, including a single sagittal section through the nipple. The subareolar margin was dissected immediately on the fresh specimen to reproduce a surgical margin at 4–5 mm from the base of the nipple. The NAC was considered involved in case of invasive ductal/lobular carcinoma and/or ductal carcinoma in situ within the subareolar margin, but not in the case of presence of lobular carcinoma in situ/lobular intraepithelial neoplasia. The pathological report was retrieved for all patients from the MX and MRI groups to examine whether NAC involvement was explicitly mentioned or not. For 13 dubious cases, the original pathological slides were blindly reviewed by two pathologists with specific experience on breast pathology (A.P. and G.D.R.) unaware of imaging data. Fig. 1. The total diameter of a multicentric lesion was measured drawing a line (a) between the external edge of the two most periferic lesions.
Fig. 2. The distance between the tumour and the nipple-areola complex (NAC) was measured both as a line parallel to the ducts (a) and parallel to the nipple axis (b). The shortest measure was taken as a reference.
2.4. Prediction of NAC involvement The likelihood of NAC involvement was calculated by applying the algorithms proposed by Schecter et al.13 and Loewen et al.14 (Fig. 3). The sensitivity (Se), specificity (Sp), positive predictive value (PPV), negative predictive value (NPV) and accuracy (Acc) in predicting NAC involvement was calculated for all algorithms. Algorithms were tested using the MX and MR data separately. Receiving operating curves (ROC) were constructed to detect the best cut-off point to allow the optimal balance between Se and Sp either by MX or MRI. 2.5. Statistical analysis
Milwaukee) and dedicated phased-array 8-channel coil, using a dynamic technique (DCE-MRI) following the recommended requirements.12 Multiplanar reconstructions (MPR) from subtracted images (postcontrast series–precontrast acquisition) were used to assess the diameter of the lesion, which was defined as the maximum extent of suspicious enhancement. As for Mx, in the case of bifocal, multifocal or multicentric lesions, these were considered as a single mass and the reference measure reflected the whole area occupied in the breast. A conventional measure of the larger tumour foci was also recorded in this group. The tumour NAC-distance was measured by electronic calipers, on both axial and sagittal Maximum Intensity Projection (MIP) images. The distance between lesion and NAC was defined as the minimum distance between the base of the NAC and the nearest margin of the lesion. 2.3. Histopathological evaluation In the original pathological report, gross and histologic assessment of the mastectomy specimens were per-
Statistical significance was set at p values < 0.05 with two-tailed test. The quantitative variables were compared with the Pearson chi-square test or Fisher’s exact test. Qualitative variables were compared using the analysis of variance. The normality of variables was tested by the Kolmogorov–Smirnov procedure. Variables not normally distributed were analysed using the non-parametric Mann–Whitney U test. Multivariate analysis was performed using the logistic regression model. Statistical analysis was performed with SPSS for Windows. 3. Results 3.1. Correlation between clinical pathologic factors and NAC involvement At histopathological analysis, 14 out of 100 cases showed tumour cells in the NAC. At univariate analysis, menopausal status, tumour histology, tumour grade, immunohistochemical characteristics and multifocality did not influence NAC status. Although positive axillary
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M. D’Alonzo et al. / European Journal of Cancer 48 (2012) 2311–2318 Schecter’ algorithm NAC involvement score = (3.663 x size factor) + (2.978 x stage factor) - (.808 x distance) - 1.465
The size factor was tumor size < 1.0 cm versus tumor size ≥1.0 cm. The stage factor was stage ≤ 2B versus stage ≥ 3A. Distance was the tumor - NAC distance. NAC involvement score ≥ - 0.3665 was interpreted as NAC positive. NAC involvement score ≤ - 0.3665 was interpreted as NAC negative
Loewen’s algorithm Nipple involvement (yes/no) = -.4613 - (.3711 x distance)
Distance is the greater of cranial-caudal or medial-lateral-oblique distance. If the value for nipple involvement is less than .10, nipple involvement = no; if the value for nipple involvement is .10 or greater, nipple involvement = yes. Fig. 3. Algorithms for the prediction of occult nipple-areola complex tumour involvement.
lymph node status and larger tumour size were more common in the NAC positive group, the difference did not reach statistical significance (p value: 0.09 and 0.08, respectively). Conversely, tumour stage was positively associated with NAC involvement (p value: 0.03) (Table 1). Tumour–NAC distance showed the highest association with NAC involvement (p value: 0.006), as well as two closely related parameters such as central tumour location (p value: 0.004) and presence of NAC retraction (p value: 0.001). Since both the measurements of tumour size and tumour–NAC distance may vary with different imaging techniques, the analysis was performed separately for the MX and MRI groups. In the MX group, all significant parameters at the combined MX + MRI analysis lost their statistical significance. In contrast, in the MRI group both lesion size (p value: 0.008) and tumour–NAC distance (0.009) retained their statistical significance (Table 2). Tumour–NAC distance remained a significant predictor of NAC involvement by setting the cut off at 5 mm (p value: 0.003), 10 mm (p value: 0.002), 20 mm (p value: 0.029). We also performed a multivariate analysis which showed that a tumour– NAC distance 610 mm was the only factor independently associated with NAC involvement (relative risk: 9.55; p value 0.05) (data not shown). 3.2. Prediction of NAC involvement by tumour–NAC distance Tumour–NAC distance resulted in a key predictor of NAC involvement. Overall, the area under the curve (AUC) of the ROC curve was 0.782 (Fig. 4), and was larger for MRI than for Mx (0.888 and 0.677 respectively). The 10 mm cut-off value allowed the best balance between Se and Sp, being associated with a NPV for NAC involvement of 94% and 100% with MX and MRI respectively (Table 3).
3.3. Validation of the algorithms The results from our series were used to validate the algorithms by Schecter et al.13 and Loewen et al.14 Measurements obtained with MRI and MX were analysed separately (Table 4). Overall, the performance of Schecter’s algorithm13 was inferior as compared to the original series due to its very low Sp (35% and 22% for MX and MRI respectively), despite its good Se (86% and 100% for MX and MRI respectively). Conversely, we were able to reproduce Loewn’s original results (Se 57%, Sp 72% for MX) and even improve their overall performance when MRI was used for measuring tumour–NAC distance (Se 100%; Sp 69%).14 4. Discussion Occult involvement of the NAC is reported in 0–58% of mastectomy specimens.1 Larger series including at least 100 patients show lower variability of occult NAC involvement (5.6–26.4%),1 and are consistent with our finding (14%). The pathological protocol for NAC evaluation, as well as pathological data collection, have a major role in determining the rate of NAC involvement. In many series, the NAC was assessed exclusively through the consultation of pathological reports. According to Schecter et al.13 this is not appropriate since only 4 cases of NAC involvement were identified by simply checking medical records in a series of 48 mastectomies, with further 9 cases identified after a pathological review of all cases. At our institution the pathological protocol requires the inspection of the NAC in all mastectomy specimens. Therefore, whenever the report contained a description of the NAC status (free of or involved with cancer), we considered the data as reliable. Only if the NAC status was not clearly stated, we asked the pathologists to review the slides. In our series, this procedure
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Table 1 Correlation between nipple–areola complex (NAC) involvement and clinical-pathological parameters (univariate analysis). N
NAC involvement
p Value
Yes (%)
No (%)
Menopausal status Premenopausal Postmenopausal
55 45
5 (35.7) 9 (64.3)
50 (58.1) 36 (41.9)
0.118
Tumor type In situ Invasive
19 81
2 (14.3) 12 (85.7)
17 (19.8) 69 (80.2)
1.000
Tumor histotype (invasive) Ductal invasive Lobular invasive Other
59 17 5
9 (75.0) 2 (16.6) 1 (8.4)
50 (72.5) 15 (21.7) 4 (5.8)
0.924
Tumor grade 1 2 3
9 33 58
0 4 (28.6) 10 (71.4)
9 (10.5) 29 (33.7) 48 (55.8)
0.356
Tumor central location Yes No
37 63
10 (71.4) 4 (28.6)
27 (31.4) 59 (68.6)
0.004
Nipple retraction Yes No
11 89
6 (42.9) 8 (57.1)
5 (5.8) 81 (94.2)
0.001
Stage I–II III–IV
90 10
10 (71.4) 4 (28.6)
80 (93.0) 6 (7.0)
0.032
Multifocality at imaging Yes No
17 83
1 (7.1) 13 (92.9)
16 (18.6) 70 (81.4)
0.453
Multifocality at pathology Yes No
41 59
5 (35.7) 9 (64.3)
36 (41.9) 50 (58.1)
0.665
53.6 52.6
41.9 41.5
0.081 0.099
Mean tumor diameter (mm) (a) (b)
100 100
Mean tumor – NAC distance (mm)
21.3
7.9
23.4
0.006
Nodal status Positive Negative
51 49
10 (71.4) 4 (28.6)
41 (47.7) 54 (52.3)
0.099
Oestrogen receptora Positive Negative
86 10
11 (84.6) 2 (15.4)
75 (90.4) 8 (9.6)
0.621
Progesterone receptor Positive Negative
82 15
10 (76.9) 3 (23.1)
72 (85.7) 12 (14.3)
0.418
Ki-67b Positive Negative
57 35
8 (72.7) 3 (27.3)
49 (60.5) 32 (39.5)
0.523
HER-2 (Herceptest) 0 1+ 2+ 3+
30 26 21 11
7 3 2 1
23 23 19 10
0.574
(53.8) (23.1) (15.4) (7.7)
(30.3) (30.3) (25.0) (13.2)
(a) In multifocal tumour the diameter of the whole area occupied in the breast was used as a reference; (b) in multifocal tumours the diameter of the largest lesion was used as a reference. a Negative: 0%, positive P1% of stained cells. b Negative: <20%, positive P20% of stained cells.
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Table 2 Correlation between nipple-areola complex (NAC) involvement and clinical parameters measured by mammography or magnetic resonance. N
NAC involvement
p Value
Yes (%)
No (%)
13 48
0 7 (100)
13 (24.1) 41 (75.9)
0.328
4 35
1 (14.3) 6 (85.7)
3 (9.4) 29 (90.6)
0.563
Mean tumor diameter (mm) MX MRIa MRIb
61 39 39
53.1 54.0 52.0
46.6 33.9 32.8
0.522 0.008 0.010
Mean tumor – NAC distance (mm) MX MRI
61 39
13.7 2.0
22.7 24.7
0.250 0.009
Multifocality at imaging MX Yes No MRI Yes No
Notes: MX: mammography; MRI: magnetic resonance. a In multifocal tumours the diameter of the whole area occupied in the breast was used as a reference. b In multifocal tumours the diameter of the largest lesion was used as a reference.
Table 3 Prediction of NAC involvement according to different cut-off values of the tumour–nipple-areolar complex (NAC) distance. Cut-off
Type of imaging
Sp%
PPV%
65 mm
MX MRI
Se% 57 86
78 78
25 46
NPV% 93 96
ACC% 75 79
610 mm
MX MRI
71 100
63 66
20 39
94 100
64 72
620 mm
MX MRI
71 100
46 50
15 30
93 100
49 59
SE: sensitivity; SP specificity; PPV: positive predictive value; NPV: negative predictive value; ACC: accuracy; MX: mammography; MRI: magnetic resonance.
Table 4 Prediction of nipple-areola complex involvement: validation of existing algorithms.
Fig. 4. Tumour–nipple-areola complex (NAC) distance in cm for the prediction of NAC involvement: Receiving Operating Characteristic (ROC) curve.
identified 2 additional positive NAC (from 12 to 14) out of 13 cases re-evaluated. In our study, NAC involvement was defined by the presence of invasive carcinoma and/or ductal carcinoma in situ at the subareolar margin. This boundary has clinical relevance as it represents the surgical plane of dissection of a NAC-sparing mastectomy. We used a 4–5 mm cut-off for our analysis since this is the mean
Se%
Sp%
PPV%
NPV%
ACC%
Schecter’s algorithm MX MRI Original series
86 100 92
35 22 77
15 22 –
95 100 93
41 36 83
Loewen’s algorithm MX MRI Original series
57 100 82
72 69 62
21 41 20
93 100 97
70 74 –
SE: sensitivity; SP specificity; PPV positive predictive value; NPV: negative predictive value; ACC: accuracy; MX: mammography; MRI: magnetic resonance.
thickness of the skin flaps of a mastectomy performed at the level of the superficial fascia dividing the subcutaneous fat from the breast glandular tissue.15 This was a conservative decision, since recent data1and our own
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experience16 suggest that when performing a NAC sparing mastectomy the dissection plane can be conducted even closer to the base of the nipple, including the whole duct bundle, with a reasonably low risk of necrosis. Our low rate of NAC positivity may depend by the pathological protocol which did not require serial coronal sections of the nipple and by the exclusion of lobular carcinoma in situ (LCIS) from our criteria of NAC involvement. Actually, in studies17,18 that include LCIS, the incidence of malignant NAC involvement is significantly higher than the average (30–58%). We believe LCIS should not be regarded as evidence of NAC involvement since it cannot be considered a true cancer lesion and does not mandate further surgical excision when detected at the surgical margins. Tumour size and tumour distance from the NAC show respectively a positive and negative correlation with NAC involvement in most studies.11,18,19 We showed that the risk of NAC involvement is strongly related to tumour–NAC distance and also to tumour size when measured by MRI. In order to allow external comparison, tumour size for multifocal tumours was measured either considering the separated tumour foci as single mass or as the diameter of the largest lesion, without any significant change of the results (Tables 1 and 2). Conversely, tumour size measured by Mx showed only a non-significant correlation with NAC involvement, probably because it mainly reflects the invasive component of the tumour, while MRI often includes also the surrounding non-invasive component of the disease. According to some authors,11 ductal carcinoma in situ is the most frequent type of cancer detected in the NAC and thus MRI measurement may better reflect the true risk of NAC involvement. Furthermore, in contrast with Schecter et al.,13 but in agreement with others,18,20 we found that NAC involvement was significantly related to central location of the lesion, skin and/or nipple retraction and stage of disease. We validated two dedicated algorithms in order to identify those patients whose risk is so low that a NAC sparing mastectomy may be justified. To this aim we tested separately the performance of MX and MRI in the models. In the algorithm by Schecter et al.,13 size, distance and tumour stage independently predicted NAC involvement, while Loewen et al. used only distance in their model. By entering our data in the Schecter’s algorithm, we found significantly lower Sp, PPV and Acc.13 This was not influenced by our decision to measure multifocal lesions as a single mass; in fact the ‘size factor’ of the Schecter’s algorithm is set at 1 cm and all of our multifocal tumours were larger both considering the diameter of the larger lesion or the diameter of the area occupied by the cancer foci. Conversely, we obtained values of Se, Sp, PPV and NPV comparable to that achieved by Loewen et al. (Table 3).14 By analysing the data separately according to the type of imaging used, we found
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that MRI consistently outperformed Mx as far as Se, NPV and PPV were concerned in both models,13,14 while Sp was significantly better for Mx as compared to MRI only in the Schechter’s model. In a recent comprehensive review of the literature,2 tumour size 65 cm and tumour–nipple distance P2 cm are proposed as inclusion criteria for performing a NAC sparing mastectomy, provided that retroareolar ducts do no show tumour involvement at pathological examination. Since our data suggest that tumour–NAC distance is the most important predictive factor, we tried to define the best cut-off to predict a low risk of NAC involvement. We found that the best compromise between specificity and sensitivity was obtained by setting the cut-off at 10 mm. Indeed, this cut-off at MRI was the only factor independently associated with NAC involvement at multivariate analysis and would have allowed to exclude NAC involvement in all cases of our series. Literature data on the best cut-off values of tumour–NAC distance are variable; only the study of Sacchini et al. support our 1 cm cut-off value,21 while most authors suggest that it should be set at P2 cm.3,11,22 Limitations of our study are mainly derived from its retrospective design. In order to limit selection biases, we prospectively included those patients with a scheduled appointment at the clinic, but we could not exclude image based- selection and study examination biases. Readerorder biases were avoided since the radiologist and pathologists were unaware of the pathological and radiological report respectively. Unfortunately, a proper comparison between MX and MRI was not possible in our study since only a few patients had both exams performed. In conclusion, occult tumour involvement of the NAC is detected in a minority of breast cancer patients submitted to mastectomy. Although, several parameters may predict the likelihood of NAC involvement, our data suggest that multiparametric models do not increase the overall accuracy obtained by the measurement of tumour–NAC distance. A distance of at least 10 mm, especially if measured by MRI, allows optimal discriminative power between cases at high versus low likelihood of NAC involvement and can virtually exclude NAC involvement. Caution is required in interpreting our data, since numbers are small and the study may be underpowered to detect significant differences. Furthermore, only prospective studies of NAC-sparing mastectomy in breast cancer patients will be able to assess the best parameters to predict NAC involvement and long term follow up data will be required to assess the oncological safety of the procedure. In the meantime, it appears that the decision to preserve the NAC in breast cancer patients undergoing mastectomy may be guided by MRI measurement of tumour–NAC distance in addition to the intraoperative pathological evaluation of the retroareolar ducts.
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