Society of Surgical Oncology-American Society for Radiation Oncology-American Society of Clinical Oncology Consensus Guideline on Margins for Breast-Conserving Surgery with Whole-Breast Irradiation in Ductal Carcinoma In Situ.

PURPOSE: Controversy exists regarding the optimal negative margin width for ductal carcinoma in situ (DCIS) treated with breast-conserving surgery and whole-breast irradiation.
METHODS: A multidisciplinary consensus panel used a meta-analysis of margin width and ipsilateral breast tumor recurrence (IBTR) from a systematic review of 20 studies including 7,883 patients and other published literature as the evidence base for consensus.
RESULTS: Negative margins halve the risk of IBTR compared with positive margins defined as ink on DCIS. A 2-mm margin minimizes the risk of IBTR compared with smaller negative margins. More widely clear margins do not significantly decrease IBTR compared with 2-mm margins. Negative margins narrower than 2 mm alone are not an indication for mastectomy, and factors known to affect rates of IBTR should be considered in determining the need for re-excision.
CONCLUSION: Use of a 2-mm margin as the standard for an adequate margin in DCIS treated with whole-breast irradiation is associated with lower rates of IBTR and has the potential to decrease re-excision rates, improve cosmetic outcomes, and decrease health care costs. Clinical judgment should be used in determining the need for further surgery in patients with negative margins narrower than 2 mm.

Breast-conserving therapy (BCT), defined as surgical excision of the primary tumor with a margin of surrounding normal tissue followed by whole-breast irradiation (WBRT), results in long-term cause-specific survival rates of greater than 95% for women with ductal carcinoma in situ (DCIS), as demonstrated in both randomized trials1 and observational studies.2,3 Although the addition of WBRT to surgical excision does not improve survival, it substantially reduces rates of ipsilateral breast tumor recurrence (IBTR), even among patients with smaller, non-high-grade DCISs.1,4 Microscopically clear margins, defined as no ink on tumor, were required in three5–7 of the four early randomized trials of WBRT for DCIS, but not in the fourth.8 These studies provide no information on whether more widely clear margins than no ink on tumor would reduce rates of IBTR in patients receiving BCT.

Retrospective single-institution studies have suggested that a negative margin width of 1 cm or more may eliminate the reduction in IBTR seen with WBRT,9 leading some to conclude that larger margins are also beneficial in patients undergoing WBRT. Despite the widespread use of BCT for DCIS, there is still no consensus on what constitutes an optimal negative margin width.10 As a consequence, approximately one in three women attempting BCT for DCIS undergo re-excision.11 Re-excisions have the potential for added discomfort, surgical complications, compromise in cosmetic outcome, additional stress for patients and families, and increased health care costs and have been associated with conversion to bilateral mastectomy.12

Since BCT was established, the landscape of DCIS management has evolved, with advances in imaging and pathologic evaluation and the availability of adjuvant endocrine therapy, resulting in a decline in IBTR rates.13 In view of these changes and the lack of consensus on what represents adequate negative margins in DCIS, the Society of Surgical Oncology (SSO), American Society for Radiation Oncology (ASTRO), and American Society of Clinical Oncology (ASCO) convened a multidisciplinary margins panel (MP) to evaluate IBTR in relation to margin width. The primary question addressed was: “What margin width minimizes the risk of IBTR in patients with DCIS receiving breast-conserving surgery?” The guideline developed from this consensus panel is intended to assist treating physicians and patients in the clinical decision-making process based on the best available evidence. The key findings of the guideline are summarized in Table 1.

Table 1

Summary of Clinical Practice Guideline Recommendations

Clinical question	Recommendation	Strength of recommendation	Level of evidence	Strength of evidence	Consensus on recommendation
Are positive margins associated with an increased risk of IBTR? Can the use of WBRT mitigate this increased risk?	A positive margin, defined as ink on DCIS, is associated with a significant increase in IBTR; this increased risk is not nullified by the use of WBRT	Strong	Meta-analysis (patient level) of RCTs (not primary end point); meta-analysis (study level) of observational studies; individual RCT	Strong	100%
What margin width minimizes the risk of IBTR in patients undergoing WBRT?	Margins ≥ 2 mm are associated with a reduced risk of IBTR relative to narrower negative margin widths in patients receiving WBRT	Moderate	Meta-analysis (study level) of observational studies	Moderate	100%
	The routine practice of obtaining negative margin widths > 2 mm is not supported by the evidence	Strong		Strong
Is treatment with excision alone and widely clear margins equivalent to treatment with excision and WBRT?	Treatment with excision alone, regardless of margin width, is associated with substantially higher rates of IBTR than treatment with excision and WBRT (even in predefined low-risk patients)	Strong	Meta-analysis (patient level) of RCTs; individual RCT	Strong	100%
What is the optimal margin width for patients treated with excision alone?	The optimal margin width for treatment with excision alone is unknown, but should be at least 2 mm. Some evidence suggests lower rates of IBTR with margin widths wider than 2 mm	Moderate	Meta-analysis (study level) of observational studies; prospective single-arm studies; retrospective studies	Moderate	100%
What are the effects of endocrine therapy on IBTR? Is the benefit of endocrine therapy associated with negative margin width?	Rates of IBTR are reduced with endocrine therapy, but there is no evidence of an association between endocrine therapy and negative margin width	Weak	RCTs	Weak	100%
Should margin widths > 2 mm be considered in the presence of unfavorable factors such as comedo necrosis, high grade, large size of DCIS, young patient age, negative ER status, or high-risk multigene panel scores?	Multiple factors have been shown to be associated with the risk of IBTR in patients treated with and without WBRT, but there are no data addressing whether margin widths should be influenced by these factors	Weak	Expert opinion	Weak	100%
Should margin width be taken into consideration when determining WBRT delivery technique?	Choice of WBRT delivery technique, fractionation, and boost dose should not be dependent on negative margin width; there is insufficient evidence to address optimal margin widths for APBI	Weak	Retrospective studies; expert opinion	Weak	100%
Should DCIS with microinvasion be considered as invasive carcinoma or DCIS when determining optimal margin width?	DCIS with microinvasion, defined as no invasive focus > 1 mm in size, should be considered as DCIS when considering the optimal margin width	Weak	Expert opinion	Weak	100%

APBI, accelerated partial-breast irradiation; DCIS, ductal carcinoma in situ; ER, estrogen receptor; IBTR, ipsilateral breast tumor recurrence; RCT, randomized controlled trial; WBRT, whole-breast irradiation

Methods

Guideline Development

The guideline development process was funded by a Susan G. Komen grant. Committee members were chosen by their respective organizations based on interest and expertise in DCIS management (Table 2). Processes recommended in the Institute of Medicine report “Clinical Practice Guidelines We Can Trust”14 that were followed as part of the guideline development process included: development of a systematic review– or study-level meta-analysis based on questions to be addressed by the MP to serve as the primary evidence base, with additional topic-specific literature reviews conducted by participants for questions not addressed in the meta-analysis; provision for each recommendation of a rating of the strength of the evidence and strength of the recommendation; ascertainment of the level of agreement of panel members with each recommendation by vote, and revision of recommendations to achieve greater than 90% consensus; and declaration by MP candidates of potential conflicts of interest before convening, and obtainment of written disclosures at the consensus meeting. (The co-chairs deemed no MP members had conflicts that could influence the process or development of specific recommendations.)

Table 2

Expert panel members

Panel Member	Society	Affiliation
Mariana Chavez-MacGregor, MD	ASCO	University of Texas MD Anderson Cancer Center
Jay R. Harris, MD	ASTRO	Harvard Medical School
Janet Horton, MD	ASTRO	Duke University Medical Center
Nehmat Houssami, MBBS, PhD	School of Public Health	Sydney Medical School, University of Sydney
E. Shelley Hwang, MD, MPH	ASBS	Duke University Medical Center
Peggy L. Johnson	Patient Advocate	Advocate in Science, Susan G. Komen
M. Luke Marinovich, PhD	School of Public Health	Sydney Medical School, University of Sydney
Meena S. Moran, MD (co-chair)	ASTRO	Yale University
Monica Morrow, MD (co-chair)	SSO	Memorial Sloan Kettering Cancer Center
Stuart J. Schnitt, MD	CAP	Beth Israel Deaconess Medical Center and Harvard Medical School
Lawrence Solin, MD	ASTRO	Albert Einstein Healthcare Network
Irene Wapnir, MD	SSO	Stanford University
Kimberly J. Van Zee, MS, MD	SSO	Memorial Sloan Kettering Cancer Center

ASBS, American Society of Breast Surgeons; ASCO, American Society of Clinical Oncology; ASTRO, American Society for Radiation Oncology; CAP, College of American Pathology; SSO, Society of Surgical Oncology

The MP convened in November 2015; the resulting manuscript was approved by all panel members and externally reviewed, and feedback was incorporated. The final manuscript was approved by the SSO Executive Council, ASTRO Board of Directors, and ASCO Board of Directors, and endorsed by the Board of Directors of the American Society of Breast Surgeons. Patient-related materials will be available on the Susan G. Komen Web site.15

Meta-Analysis

The methodology for the systematic review/meta-analysis has been published elsewhere.16 Briefly, using Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) and Institute of Medicine guidelines, EMBASE, MEDLINE, PREMEDLINE, and evidence-based medicine databases were searched in October 2014 for eligible studies. A summary providing details of the methodology and statistical approaches is provided in the Appendix (online only). Analysis was performed using two different statistical approaches. In the frequentist approach, multiple margin cut points within studies, if reported, were condensed into a single cut point, whereas the Bayesian approach allowed for the use of multiple cut points.17 All reported odds ratio (ORs) were adjusted for study-specific median follow-up time (to account for the inherent increased risk of IBTR with longer follow-up) and are reported relative to positive (or positive/close) margins or to a minimal negative margin (no ink on tumor or margin > 1 mm).16

Inclusion and Exclusion Criteria

Studies that included a minimum of 50 patients with DCIS treated with local excision and reported IBTR in relation to microscopic margin widths with a minimum median follow-up of 4 years were eligible.16

Study Quality and Literature Limitations

All publications in the meta-analysis (except two) were retrospective and provided observational data at the study level. The characteristics of these studies have been reported elsewhere.16

Results

The meta-analysis included 20 studies, 7,883 patients with DCIS with known margin status, and 865 IBTRs.16 The median proportion of patients undergoing WBRT was 100% (interquartile range [IQR], 53.3% to 100.0%), and the median proportion receiving endocrine therapy was 20.8% (IQR, 0.0% to 31.4%). The median follow-up was 78.3 months, and the median incidence of IBTR was 8.3% (IQR, 5.0% to 11.9%). Because of heterogeneity in classification and reporting of margins data, both a frequentist analysis and a Bayesian network meta-analysis were conducted with sensitivity analyses. Characteristics of patients included in the studies are summarized in Table 3.16

Table 3

Summary of study characteristics included in meta-analysis

Characteristic	No. of Studies*	Value or Proportion Across Studies
		Median	Range
Patient age, years	20	53.7	43.0–62.1
Type of IBTR
DCIS	17	50.0%	0.0%–75.0%
Invasive	17	50.0%	25.0%–100.0%
Unknown	17	0.0%	0.0%–7.1%
Screen detected
Yes	14	85.8%	45.6%–100.0%
No	14	14.2%	0.0%–54.4%
Unknown	14	0.0%	0.0%–2.8%
Grade
I	13	17.5%	1.8%–64.5%
II	13	28.0%	5.5%–45.0%
I–II	16	57.3%	7.3%–92.5%
III	16	28.4%	3.5%–45.6%
Unknown	16	9.2%	0.0%–87.3%
Hormone receptor status
Positive	5	50.4%	23.0%–80.4%
Negative	5	8.7%	2.8%–14.3%
Unknown	5	40.9%	14.8%–69.8%
Median WBRT dose, Gy	11	50.0	42.5–50.0
Radiation boost	19	70.9%	0.0%–100%
Median boost dose, Gy	8	10.0	10.0-10.8

NOTE. Data adapted.16

Abbreviations: DCIS, ductal carcinoma in situ; IBTR, ipsilateral breast tumor recurrence; WBRT, whole-breast irradiation

*Refers to studies contributing information on the characteristic, including studies with subsets of patients missing data for the characteristic

Guideline Recommendations

Positive Margins

A positive margin, defined as ink on DCIS, is associated with a significant increase in IBTR. This increased risk is not nullified by the use of WBRT.

There is no debate that a positive margin, defined as the presence of ink from the specimen surface on ducts containing DCIS, implies a potentially incomplete resection and is associated with a higher rate of IBTR. In the Early Breast Cancer Trialists’ Collaborative Group (EBCTCG) meta-analysis of randomized DCIS trials,1 patients with positive margins had a two-fold higher IBTR risk compared with patients with negative margins despite receiving WBRT (10-year IBTR rate, 24% v 12 %), and approximately 50% were invasive recurrences. The relationship between margin status and WBRT was examined in a subset analysis of the National Surgical Adjuvant Breast and Bowel Project (NSABP) B-17 trial by central pathology review of 573 of 818 participants.18 The annual hazard rate for IBTR after lumpectomy alone was 8.1 % for those with positive margins compared with 3.3% for patients with negative margins, reduced by WBRT to 2.7% and 1.2%, respectively. Positive margins were significantly associated with IBTR in a multivariable analysis of the long-term results of the European Organisation for Research and Treatment of Cancer (EORTC) 10853 trial.19 In the meta-analysis by Marinovich et al16 using the Bayesian analytic approach, similar results were obtained. After adjustment for study-level follow-up, patients with negative margins were significantly less likely to experience IBTR than patients with positive margins (OR, 0.45; 95% credible interval [CrI], 0.30 to 0.62). Similar findings were observed in the frequentist analysis, which necessitated combining positive and close margins (OR, 0.53; 95% CI, 0.45 to 0.62; P < .001). This result persisted after study-level adjustment for age, median recruitment year, grade of DCIS, use of WBRT, and use of endocrine therapy.

Negative Margin Widths

Margins of at least 2 mm are associated with a reduced risk of IBTR relative to narrower negative margin widths in patients undergoing WBRT. The routine practice of obtaining negative margin widths wider than 2 mm is not supported by the evidence.

To address the question of optimal negative margin width, the MP considered data on the distribution of DCIS in the breast. Studies of mastectomy specimens using whole-organ sectioning and radiologic–pathologic correlation have demonstrated that although most cases of DCIS are unicentric, the involvement of the segment may be multifocal, with so-called gaps of uninvolved tissue between foci of DCIS.20 Given this, a negative margin does not guarantee the absence of residual DCIS in the breast.

There are also technical limitations to margin assessment that affect the relationship between margin width and IBTR. For example, margins are artifactually narrower ex vivo, when specimens become flattened from lack of surrounding supportive tissue, a phenomenon exaggerated by compression for specimen radiography. Additionally, surface ink can track into deeper portions of the specimen, posing significant challenges in determining true margin location. Finally, tumor-to-ink distance on any single slide may not be representative of the entire specimen; an adequate margin on one section may become positive if additional or deeper sections are examined. Two common methods for margin evaluation include sectioning perpendicular to ink (to determine tumor-to-ink width) or en-face examination of shaved margins (where any residual tumor in the shaved specimen is considered a positive margin). Although an advantage of the shaved method is greater surface-area examination, a known disadvantage is the higher frequency of margins categorized as positive that are, in comparison, negative by the perpendicular method, which may in turn result in unnecessary re-excision or even mastectomy.21 Specimen sampling is also highly variable, and even total sequential embedding results in only a small proportion (< 1%) of the specimen margins being examined.22 Together, these studies highlight the substantial variability in margin assessment irrespective of the technique used.

Despite variability in margin assessment, great emphasis has been placed on achieving specific negative margin widths. In the frequentist meta-analysis by Marinovich et al,16 comparison of specific margin width thresholds (2, 3 or 5, and 10 mm) relative to negative margins defined as wider than 0 or 1 mm included 7,883 patients with a median follow-up of 6.5 years. The ORs for 2 mm (0.51; 95% CI, 0.31 to 0.85; P = .01), 3 or 5 mm (0.42; 95% CI, 0.18 to 0.97; P = .04), and 10 mm (0.60; 95% CI, 0.33 to 1.08; P = .09) showed comparable reductions in the odds of IBTR compared with wider than 0 or 1 mm, and pairwise comparisons found no significant differences in the odds of IBTR between the 2-, 3- or 5-, and 10-mm margin thresholds (all P > .40). In this model, the predicted 10-year IBTR probability for 2-mm negative margins was 10.1% (95% CI, 6.3% to 16.0%) compared with 8.5% for 3- or 5-mm (95% CI, 3.6% to 18.9%) and 11.7% (95% CI, 6.7% to 19.4%) for 10-mm margins. In the Bayesian network meta-analysis (Table 4),16 the ORs of incrementally wider negative margins relative to the positive margin category were 0.45 (95% CrI, 0.32 to 0.61) for wider than 0 or 1 mm, 0.32 (95% CrI, 0.21 to 0.48) for 2 mm, 0.30 (95% CrI, 0.12 to 0.76) for 3 mm, and 0.32 (95% CrI, 0.19 to 0.49) for 10 mm. Adjustments for clinically relevant covariates, including sensitivity analysis limited to studies using radiation therapy (RT), did not alter these mean OR estimates (Table 4). In this analysis, the relative OR of IBTR between the 10- and 2-mm threshold groups compared with positive margins was 0.99 (95% CrI, 0.61 to 1.64), indicating no statistically meaningful difference.

Table 4

Margin threshold and IBTR: Bayesian network meta-analysis

Analysis	Threshold distance for negative margins relative to positive (mm)
	Mean OR (95% CrI)*
	>0 or 1	2	3	10
Main model, no. of patients	2,230	2,412	289	1,963
All studies	0.45 (0.32 to 0.61)	0.32 (0.21 to 0.48)	0.30 (0.12 to 0.76)	0.32 (0.19 to 0.49)
Sensitivity analysis, no. of patients	1,957	1,851	272	1,079
RT cohorts only	0.45 (0.34 to 0.61)	0.33 (0.23 to 0.47)	0.22 (0.08 to 0.53)	0.37 (0.24 to 0.57)
Sensitivity analysis, no. of patients	1,781	1,524	289	616
Van Zee et al22 excluded	0.43 (0.31 to 0.57)	0.29 (0.19 to 0.45)	0.32 (0.14 to 0.75)	0.27 (0.16 to 0.47)
Sensitivity analysis, no. of patients	2,230	2,412	—	1,963
3 mm excluded	0.47 (0.34 to 0.63)	0.34 (0.23 to 0.49)	—	0.36 (0.23 to 0.56)
Sensitivity analysis, no. of patients	2,692	2,555	322†	2,160
Adding studies with no summary age data‡	0.44 (0.30 to 0.63)	0.31 (0.19 to 0.51)	0.32 (0.14 to 0.73)	0.20 (0.11 to 0.35)§
Adjustment for covariates (based on main model)
Age	0.46 (0.33 to 0.63)	0.34 (0.22 to 0.51)	0.33 (0.13 to 0.83)	0.33 (0.20 to 0.51)
Median recruitment year	0.45 (0.31 to 0.62)	0.31 (0.19 to 0.46)	0.29 (0.12 to 0.68)	0.32 (0.20 to 0.49)
Proportion with RT	0.46 (0.33 to 0.63)	0.33 (0.22 to 0.49)	0.29 (0.12 to 0.74)	0.32 (0.20 to 0.50)
Proportion with endocrine therapy⊤	0.45 (0.29 to 0.70)	0.33 (0.18 to 0.57)	0.29 (0.10 to 0.79)	0.31 (0.17 to 0.57)
Proportion with high-grade DCIS⊤	0.45 (0.32 to 0.62)	0.33 (0.21 to 0.48)	0.31 (0.12 to 0.74)	0.39 (0.25 to 0.59)

Data adapted.16

Abbreviations: CrI, credible interval; DCIS, ductal carcinoma in situ; IBTR, ipsilateral breast tumor recurrence; OR, odds ratio; RT, radiation therapy

* Adjusted for follow-up

†Two studies using a 5 mm threshold were included with the 3 mm threshold group

‡These studies were ineligible for inclusion in the meta-analysis from Marinovich et al because of lack of summary age data (see eligibility criteria); hence sensitivity analysis reports estimates if these were included in models

§95% CrI for relative odds ratio of 10 v > 0 or 1 mm did not cross 1 (Methods Meta-Analysis)

⊤Because of missing covariate information, these analyses were undertaken in a reduced number of studies (19 for endocrine therapy; 16 for high-grade DCIS)

The choice of the 2-mm threshold rather than wider than 0 (no ink on tumor) or 1 mm was based on evidence of a statistically significant decrease in IBTR for 2 mm compared with 0 or 1 mm in the frequentist analysis (OR, 0.51; 95% CI, 0.31 to 0.85; P = .01), coupled with weak evidence in the Bayesian model of a reduction in IBTR with the 2-mm distance compared with smaller distances (relative OR, 0.72; 95% CrI, 0.47 to 1.08). However, although the MP felt that there was evidence that the 2-mm margin optimized local control, clinical judgment must be used in determining whether patients with smaller negative margin widths (> 0 or 1 mm) require re-excision. Factors felt to be important to consider include assessment of IBTR risk (residual calcifications on postexcision mammography, extent of DCIS in proximity to margin, and which margin is close [i.e. anterior excised to skin or posterior excised to pectoral fascia v margins associated with residual breast tissue]), cosmetic impact of re-excision, and overall life expectancy. The conclusion that re-excision could be selectively employed with margins smaller than 2 mm was influenced by the high long-term rates of local control reported in the NSABP DCIS trials,7 which required a margin of no ink on tumor, as well as the study by Van Zee et al,23 which, after adjusting for multiple covariates, found no difference in risk between margins of 2 mm or narrower and more widely clear margins in patients receiving WBRT.

Treatment with Excision Alone

Treatment with excision alone, regardless of margin width, is associated with substantially higher rates of IBTR than treatment with excision and WBRT, even in predefined low-risk patients. The optimal margin width for treatment with excision alone is unknown but should be at least 2 mm. Some evidence suggests lower rates of IBTR with margin widths wider than 2 mm.

The EBCTCG DCIS meta-analysis showed that the 10-year IBTR rate for patients treated with excision alone was higher than that with excision and WBRT, both for those with negative (26.0% v 12.0%; P < .001) and positive margins (48.3% v 24.2%; P < .001).1 The same proportional benefit for WBRT was seen in women treated with local excision and those having large sector resections. In the Radiation Therapy Oncology Group (RTOG) 9804 trial, where patients with small, mammographically detected low- to intermediate-grade DCIS and margins of 3 mm or wider were randomly assigned to excision alone or excision plus WBRT, 7-year IBTR rates were 6.7% and 0.9% (P < .001), respectively.4 The prospective, multi-institutional Eastern Cooperative Oncology Group (ECOG) E5194 study of patients with low-risk DCIS treated with excision alone (negative margin width ≥ 3 mm) reported 12-year rates of IBTR of 14.4% for non–high-grade DCIS 2.5 cm or smaller in size and 24.6% for high-grade DCIS 1 cm or smaller in size. However, IBTR rates did not differ significantly for margins narrower than 5, 5 to 9, or 10 mm or wider (P = .85).24 A prospective single-arm study of patients with mammographically detected DCIS 2.5 cm or smaller in size reported a 10-year IBTR rate of 15.6%,25 despite requiring margins of 1 cm or wider.4 In contrast, Van Zee et al23 found in 1,266 patients treated with excision alone that the 10-year IBTR rate was 16% for margins wider than 10 mm and increased to 23% for margins between 2.1 and 10 mm, 27% for margins greater than 0 to 2 mm, and 41% for positive margins. After adjustment for multiple factors, margin width was a more highly significant predictor of IBTR (P < .001). The MP felt that overall, the heterogeneity of the evidence among these studies did not allow for a definitive recommendation for margin widths greater than 2 mm in patients foregoing RT.

Endocrine Therapy

Rates of IBTR are reduced with endocrine therapy, but there is no evidence of an association between endocrine therapy and negative margin width.

Tamoxifen reduces the incidence of both IBTR and contralateral breast cancer, but the absolute benefit is relatively small.7,26 In the NSABP B-24 trial, patients treated with lumpectomy and WBRT were randomly assigned to tamoxifen or placebo; 25% of the population had positive or unknown margins. The 15-year IBTR rate for the placebo group was 17.4% in those with positive margins compared with 7.4% for clear margins. Adjuvant tamoxifen lowered IBTR rates among those with positive margins to levels similar to those in the negative-margin cohort (placebo, 17.4%; tamoxifen, 11.5%); conversely, there was little impact of tamoxifen in the negative-margin cohort (IBTR: placebo, 7.4%; tamoxifen, 7.5%).7 Hence, the MP felt that although tamoxifen decreased IBTR in patients with positive margins, there was no evidence to suggest an association between negative margin width and benefit of endocrine therapy.

Patient and Tumor Features

Multiple factors have been shown to be associated with the risk of IBTR in patients treated with and without WBRT, but there are no data addressing whether margin widths should be influenced by these factors.

Young patient age has consistently been associated with IBTR, and tumor factors such as histologic pattern, comedo necrosis, and nuclear grade and size of DCIS also modify the risk of IBTR.18,27,28 More recently, unfavorable gene profile scores have also been associated with IBTR.29,30 However, there are no data addressing whether margin widths should be influenced by these factors, and this represents an appropriate area for further study.

Radiation Delivery

Choice of WBRT delivery technique, fractionation, and boost dose should not be dependent on negative margin width. There is insufficient evidence to address optimal margin widths for accelerated partial-breast irradiation (APBI).

A vast majority of patients treated in the five prospective randomized DCIS trials of excision with or without WBRT underwent conventionally fractionated WBRT without a boost. Only one of the trials allowed the option of hypofractionated WBRT in addition to standard WBRT,4 and 10% or fewer of the patients in three of the trials received a boost.6–8 None of the randomized trials varied RT technique according to margin status, and neither intensity-modulated RT nor APBI were used. There is no direct evidence from randomized trials to support the use of a boost to the primary tumor site for patients with DCIS, although in patients with invasive breast carcinoma, the long-term value of a boost in reducing IBTR has been demonstrated.31

Two ASTRO consensus guidelines have addressed technical issues in the setting of BCT. Although largely focusing on invasive breast carcinoma, the ASTRO statement on hypofractionated WBRT concluded there was insufficient evidence to recommend for or against hypofractionated WBRT in the setting of DCIS.32 In the ASTRO statement on APBI, DCIS was placed in the cautionary group based on the lack of evidence from randomized trials; however, it was noted that patients with DCIS have been included in some retrospective cohort studies.33

Therefore, there is no evidence that margin width, in isolation, should determine radiation delivery technique, fractionation of WBRT, or use or dose of a boost. The MP considered the evidence base insufficient to address optimal margin width in APBI.

DCIS in Presence of Invasive Breast Cancer

DCIS with microinvasion (DCIS-M), defined as no invasive focus larger than 1 mm in size, should be considered DCIS when determining optimal margin width.

There are two diagnoses for which there is overlap between our DCIS margin guideline and the SSO-ASTRO invasive cancer margin guideline:34 DCIS-M and invasive carcinoma associated with DCIS (extensive intraductal component or lesser amounts of scattered DCIS). In DCIS-M, defined by the American Joint Committee on Cancer as the extension of cancer cells beyond the basement membrane with no focus more than 0.1 cm in greatest dimension,35 small retrospective studies have suggested that rates of IBTR are similar to those seen with pure DCIS.36,37 In the absence of specific data to address margin width in DCIS-M, the MP, based on expert opinion, felt that DCIS-M should be considered DCIS when determining the optimal margin width, given that the majority of the lesion is composed of DCIS and that systemic therapy utilization for DCIS-M more closely reflects the treatment pattern for DCIS than for invasive carcinoma.

In contrast, when considering margin width for an invasive cancer with a DCIS component, regardless of extent, the MP felt that the invasive cancer guideline34 was applicable, primarily because the natural history and treatment of these lesions are more similar to those of invasive cancer than DCIS, even when the close margin contains DCIS. In particular, a vast majority of patients with invasive cancer receive systemic therapy, which remains less common for pure DCIS. The invasive cancer guideline34 does note that an extensive intraductal component is a marker for a potential heavy burden of residual DCIS and that postexcision mammography, presence of multiple close margins, and young patient age can be used to select patients who will benefit from re-excision. These statements echo the discussion of the MP regarding the use of re-excision in pure DCIS with margins narrower than 2 mm discussed previously, and thus, we believe the guidelines are compatible.

Discussion

There are limitations to this guideline. It applies to patients with DCIS and DCIS-M treated with WBRT. The findings should not be extrapolated to patients with DCIS treated with APBI or those with invasive carcinoma, for whom a separate guideline has been developed.34 Although studies including patients treated with and without WBRT were included in the meta-analysis, a meta-analysis of studies of treatment with excision alone was not conducted. Additionally, all of the studies included in the meta-analysis were retrospective. However, in the absence of any planned prospective randomized trials addressing the question of margin width and local recurrence, these studies represent the best available evidence for clinical decision making.