- Research article
- Open access
- Published:
Risk of second breast cancer in female Hodgkin’s lymphoma survivors: a meta-analysis
BMC Cancer volume 12, Article number: 197 (2012)
Abstract
Background
Women treated for Hodgkin’s lymphoma (HL) have an elevated risk of developing second breast cancer (SBC) compared with the general population. We planned this meta-analysis to quantify the long-term risk of SBC and analyze the contributing risk factors among HL survivors.
Methods
According to predefined selection criteria, literature search identified 34 studies that were included in the analyses.
Results
After eliminating overlapping or duplicate data, 957 incidences of SBC were encountered in 24,505 females with HL over a median follow-up of 14.9 years. The medians: age at the diagnosis of HL, age at diagnosis of SBC, and latency since HL treatment to the development of SBC were 23.7, 35.0, and 17.7 years, respectively. The pooled relative risk (RR) of SBC was 8.23 (95% CI, 5.43-12.47, I 2 = 96%), with a median absolute excess rate of 22.9 per 10,000 person-years. The RR was found inversely related to age at diagnosis of HL with the highest rate (68.7; [95%CI, 28.08-168.11], I 2 = 79%), occurred in young patients (≤ 15 years old), where the RR in older women (≥ 40 years old) was not significant (0.55; [95% CI, 0.09-3.52]). Analysis of RR by 5-year increments since the treatment of HL showed that the risk was highest after 15–19 years of latency (13.87; [95% CI, 7.91-24.30], I 2 = 89%). Analysis of the effect of treatment modalities showed that the RR rates were (4.70; [95% CI, 3.28-6.75], I 2 = 74%), (5.65; [95%CI, 2.94-10.88], I 2 = 91%), and (1.19; [95% CI, 0.50-2.82], I 2 = 65%), for radiotherapy (RT) only, combined RT and chemotherapy (CT), and CT only, respectively. To investigate the demonstrated heterogeneity, meta-regression analysis was performed when feasible. In most such analyses, the natural logarithm of RR was inversely associated with age at HL diagnosis.
Conclusions
We conclude that, the current meta-analysis provided the most recent comprehensive estimate of the risk of SBC in a broad-range of HL survivors. Younger age at diagnosis proved to be a dominant risk factor. The obtained results would serve providing breast cancer screening recommendations for HL survivors.
Background
Hodgkin’s lymphoma (HL) became a curable disease by radiation therapy (RT) and/or combination chemotherapy (CT) since the early 70s [1–3]. Long-term disease-free survival of 70% to 90%, depending on stage at diagnosis has been achieved [4], and even more favorable outcome has been demonstrated in pediatrics, with a 5-year survival exceeding 90% [5].
However, increased risk of second cancer following effective treatment of HL has long been reported [6]. More recently, second neoplasms after HL are being encountered with increasing frequency due to the marked improvement in survival [2, 7]. The particular elevated risk of second breast cancer (SBC) among this population is not surprising in view of the reported excess risks of breast cancer (BC) after incidental low doses of ionizing radiation [8, 9], therapeutic RT [10, 11], or as sequelae of the carcinogenic effects of CT [12, 13].
Two pertinent meta-analyses have been published and they have addressed different questions. The first meta-analysis was published in 2006 and examined all second malignancy risk associated with HL treatment in 31 randomized trials and it included 65 incidence of SBC [14]. In the second meta-analysis [15], SBC risk and BC surveillance were investigated in young females (≤ 30 years at the primary tumor diagnosis) receiving moderate to high doses of RT targeted to mantle and modified mantle fields, mediastinum, lung, and thorax [15]. The latter meta-analysis comprised 11 studies that were not restricted to patients with HL but included all primary neoplasms in that age group.
Research on the late consequences of HL has often been limited by the size and composition of the study populations and by the duration and completeness of patient follow-up. To the best of our knowledge, there is no recently published meta-analysis intended to examine the risk of SBC in a broad range of ages at HL diagnosis, various follow-up periods, and subsequent to different therapeutic modalities. Also not precisely known, is the effect of other contributing risk factors. The lack of such data has prompted the current meta-analysis.
Methods
Search strategy
Between January 1966 and October 2011, we identified studies of interest by first conducting an electronic literature search of the databases MEDLINE, EMBASE, and the Cochrane Library. We also searched for relevant abstracts in the annual conference proceedings between January 1984 to October 2011 for the American Society of Clinical Oncology, European Society for Medical Oncology, and the San Antonio Breast Cancer Symposium. All ages of HL patients were eligible for inclusion.
We used exploded Medical Subject Heading terms or key words terms ‘lymphoma’, ‘Hodgkin’, ‘Hodgkin’s disease’ and ‘Hodgkin’s lymphoma’. The terms were combined with ‘neoplasm, second neoplasm, second primary’ using the Boolean operator ‘and’. Search results were also filtered against the terms ‘breast, breast cancer, breast neoplasm). In the second step, these keywords were combined using the Boolean operator ‘and’ with ‘standardized incidence ratio’, ‘relative risk’, and ‘observed to expected’. In addition, we manually reviewed the reference lists of relevant studies to identify additional pertinent published articles.
Selection criteria
We included studies that met each of following criteria: (i) published in English language between January 1985 and October 2011; (ii) included naive patients at any age and with any stage of HL; (iii) investigated the risk for second malignant neoplasms (SMNs) in HL survivors; (iv) reported relative risk (RR) and/or specified as standardized incidence ratios (SIR) or data allowing such outcomes to be derived; and (v) published as original articles (no case reports, case series, reviews, comments, letters, or editorials).
When two or more references reported duplicate data, we only included in the analysis the most recent data, studies with the longer follow-up, or the most relevant studies. We excluded studies that mainly addressed the clinical characteristics of SBC. We also excluded studies that mainly intended to evaluate the potential benefits and harms associated with breast cancer surveillance among women with HL. Case–control designs, i.e. HL patients who developed BC compared with patients who did not were excluded.
Data extraction
Two authors (KMA, and GAK) independently inspected each reference title identified by the search and applied the inclusion criteria. For possibly relevant articles and in cases of disagreement between reviewers, the full article was obtained and inspected independently by the five authors. The data intended for extraction were discussed, and decisions were documented. We used the STROBE (Strengthening the Reporting of Observational Studies in Epidemiology) reporting criteria to assess the quality of studies included in the meta-analysis [16]. Any significant lack of concordance in the scores assigned by authors was discussed to reach a consensus.
Standardized Excel sheet was used for each study that fulfilled the inclusion criteria. Extracted data included paper characteristics (first author’s last name, publication year, country in which the study was carried out, and data source), study design, number of HL patients, mean/median age of patients, mean/median duration of follow-up, therapy details, number of observed and expected SBC cases, and RR or standardized-incidence rate (SIR) with corresponding 95% confidence interval (CI). The ratio of observed to expected numbers of cancers, SIR (referred to in the text as RR) was then used or calculated with likelihood-based 95% CI from Poisson models [17]. Where not reported, we computed the CI for the risk assuming a Poisson distribution for the observed number of cases. Standard error (SE) for the natural logarithm of RR (lnRR) was derived from CI, applying the following equation: SE = ln(upper 95% CI/lower 95% CI)/(2 x z1 - a/2). When appropriate, we also used the built-in calculator of the Review Manager Software (version 5.1.4 for Windows; The Cochrane Collaboration, Oxford, UK) to compute missing data. When studies showed that the observed number of cases was zero, we simply added 1 to both the observed and the expected number of cases to allow computation of an estimate of the lnRR and its associated SE [18].
Outcome measures
The primary outcome was the overall pooled RR of incidence of SBC among women survivors of HD. The secondary end points were RR vs. various variables: source of data, age at diagnosis of HD, length of follow-up, treatment modalities, and any additional relevant risk factors. RT in this meta-analysis is referred to supra-diaphragmatic irradiation with or without other radiation fields.
Statistical analyses
We assessed heterogeneity of the studies’ results by inspecting graphical presentations and by calculating an x 2 test of heterogeneity and the I 2 statistic of inconsistency [19, 20]. Statistically significant heterogeneity was defined as a x2 P value less than .1 or an I2 statistic greater than 50%. The estimates of RR, together with associated 95% CI, were obtained using the DerSimonian and Laird random-effects model [21]. Meta-regression analysis was performed to determine to what extent the heterogeneity is explained by various covariates using IBM SPSS statistical package v.19. The dependent variable was the lnRR weighted for the inverse of variance to perform weighted least square linear regression. We first conducted a univariate regression analysis for each variable followed by a multivariate regression including variables found significant in the univariate analysis.
Subgroup analyses were performed to assess potential contributions of various clinical variables to outcomes. A funnel plot estimating the precision of trials (plots of logarithm of the RR against the sample size) was examined for asymmetry to estimate publication bias [22]. Publication bias was also quantified by the regression asymmetry test by Egger [22].
All statistical tests were two-sided. RR was estimated according to the inverse of variance method with the use of Review Manager Software v5.1.4.
Results
Search results
We identified 1,647 potentially relevant articles (Figure 1). After exclusion of duplicate references, none-relevant literature, and those that did not satisfy inclusion criteria, 41 candidate articles were considered for the meta-analysis [23–62]. After careful review of the full text of these articles, 7 studies were excluded. In 5 studies the RR was reported based on case–control design, i.e. HL patients who developed SBC against patients who did not [33, 43, 47, 63, 64]. The RR in the sixth excluded study compared RR among HL patients according to presence or absence of a family history of BC [50]. The seventh excluded study was designed to examine RT dose and dose distribution in 41 HL patients (25 females) treated at a single Canadian institution [49].
Search results and the selection of 33 included studies.
The remaining 34 studies were included in the meta-analysis. The funnel plot of 25 non-overlapping studies showed mild asymmetry, however, the Egger linear regression test was not significant (P = .059).
Of the 34 included studies, there were several reports of overlapping and/or updated data with longer follow-up and more encountered events. For any analysis, only the updated results were used unless there were relevant data available in earlier report and were not included in more recent publication. That approach was used to deal with the overlapping data of van Leeuwen et al. [25] (2 Dutch institutes) and De Bruin et al. [55] (5 Dutch institutes); Mauch et al. [26] (5 USA institutes) and Ng et al. [41] (4 USA institutes); Aisenberg et al. [28] and Alm El-Din et al. [54] (single USA institute); Basu et al. [52] and Constine et al. [53] (5 USA institutes); Neglia et al. [39], Kenney et al. [45], and Castellino et al. [59] (the multi-institutional USA Childhood Cancer Survivor Study); Metayer et al. [35] (16 population-based cancer registries in North America and Europe, Hodgson et al. [48] (13 population-based cancer registries in North America and Europe), and that of Dores et al. [57] (9 population-based cancer registries in the USA); Hancock et al. [24], Wolden et al. (1998) [30], O'Brien [58], and Wolden et al. (2000) [37] (single USA institute); and Swerdlow et al. [36], and Swerdlow et al. [62] for the British National Lymphoma Investigation.
Tables 1 and 2 show the abstracted and computed data of the included studies. Overlapping studies were shaded together. The data sets included patients diagnosed as early as 1935 to the late 2000s. The median duration of follow-up since the diagnosis of HL was 14.9 years (95% CI, 13.0-16.2 years; ranging from 6 to 23.8 years), while the median age at the diagnosis of HL was 23.7 years (95% CI, 18.9-25.5 years; ranging from 11.8 to 40 years), and the median age at the diagnosis of SBC was 35.0 years (95% CI, 30.2-40.0 years; ranging from 12.8 to 44.4 years). The median interval between primary diagnosis and development of SBC was 17.7 years (95% CI, 15.2-18.6 years; ranging from 12.2 to 21.6 years).
After eliminating overlapping and duplicate studies, there were 25,305 women with HL and 957 incidences of SBC. The median absolute excess rate (AER) of SBC incidence per 10,000 person-years of observation was 22.9 excess cases (95%CI, 15.6-55.7, ranging from 1.1 to 174). Few studies reported the cumulative incidence of SBC after 20 and 30 years of follow-up (average: 5.4% and 12%, respectively).
Pooled RR
Figure 2 depicts the Forest plot for the pooled RR. The fixed-effects model showed significant heterogeneity (I 2 statistic = 96%; p <0.0001). The random-effects model was computed instead and it showed that patients with HL have an almost 9-fold increase in the risk of SBC (RR = 8.23; [95% CI, 5.43-12.47], I 2 = 96%). We performed meta-regression analysis to determine to what extent the heterogeneity is explained by the effects of study size, age at HL diagnosis, and the latency since the completion of HL treatment. The univariate analysis showed significant inverse association between lnRR and age at diagnosis and a positive relation to latency since HL treatment. With multivariate analysis (Table 3), only younger age at diagnosis remained significant (<0.0001).
Summary statistics and corresponding forest plot for the overall relative risk ( RR ) of second breast cancer as reported from 23 studies.
In Figure 3, the random-effects analysis illustrates a higher risk in institutional studies (RR = 8.86; [95% CI, 5.26-14.94] compared with population-based analyses (6.70; [95% CI, 4.07-11.03]). The demonstrated heterogeneity (I 2 = 96%) was explored by meta-regression analysis, however, none of variables tested was found associated with lnRR in the univariate analysis (data not shown).
Summary statistics and corresponding forest plot for the relative risk ( RR ) of second breast cancer in institutional vs. population-based studies. RRs were calculated using a random- effects model.
RR and age at diagnosis of HL
The excess risk of SBC as a function of age at diagnosis of HL was also explored. Figure 4 (random-effects model) shows that the RR of developing SBC decreased significantly with increasing age at diagnosis from 68.7 (95% CI, 28.8-168.11, ≤ 15 years old) to 22.32 (95% CI, 13.4-37.16, 15–19 years old), 14.43 (95% CI, 11.65-17.88, 20–24 years old), and 6.6 (95% CI, 4.24-10.29, 25–29 years old). As a significant heterogeneity was shown (I 2 = 79%), we performed a meta-regression analysis, however, none of the explanatory variables was found significant (data not shown).
Summary statistics and corresponding forest plot for the relative risk ( RR ) of second breast cancer based on the age at Hodgkin’s lymphoma diagnosis. RRs were calculated using a random-effects model.
Several studies reported the RR at certain cut points of age at diagnosis and it also showed an inverse relation between risk and age (Figure 5, fixed-effects model). In the latter analysis and contrary to analysis of RR against more age intervals, no significant heterogeneity was noted (I 2 = 41%). Of note, the RR of SBC for women who developed HL above the age of 40 years was not significant (RR = 0.55; [95% CI, 0.09-3.52]).
Summary statistics and corresponding forest plot for the relative risk ( RR ) of second breast cancer based on specific cut points of age at Hodgkin’s lymphoma diagnosis. RRs were calculated using a fixed-effects model.
RR and follow-up latency
We performed analysis of RR by 5-year increments since the treatment of HL (Figure 6, random-effects model, I 2 = 73%). By and large, the analysis demonstrated an increasing RR by increased duration of follow-up latency reaching the highest after 15–19 years (RR = 13.87; [95% CI, 7.91-24.30]). While there was a decrease in RR noted after 20–24 years of follow-up, further rise occurred after 25–29 years. The latter rise may be attributed to the RR reported by De Bruin et al. [55], while all the other studies demonstrated a decreased RR after 25–29 years compared with that after 20–24 years of follow-up. Due to unreported data, meta-regression analysis of the heterogeneity could only include age at diagnosis of HL as the sole explanatory variable and it showed an inverse association with lnRR (Table 3).
Summary statistics and corresponding forest plot for the relative risk ( RR ) of second breast cancer based on follow-up latency since Hodgkin’s lymphoma diagnosis. RRs were calculated using a random-effects model.
After ≥ 20 years of latency since diagnosis, 9 studies [37, 40, 41, 44, 45, 48, 51, 54, 55] reported RR of 6.95 (95% CI, 4.8- 10.1). That RR was not significantly different from the rate encountered after ≥ 30 years of follow-up (RR = 7.03; [95% CI, 5.2-9.5]) as reported from 5 studies [42, 44, 51, 54, 55].
RR vs. Age at HL diagnosis and follow-up latency
To examine the interaction of both age at HL diagnosis and length of follow-up versus risk, few studies have reported adequate data. De Bruin et al. [55] reported that after 5–14 years of follow-up, those who were ≤ 20 years at HL diagnosis had significantly higher risk (RR = 20.0; [95% CI, 7.3-43.4]) as compared with those who were older (21–30 years old) (RR = 5.3; [95% CI, 1.9- 16.6]). Similarly, after ≥ 25 years of follow-up, the corresponding RRs for younger and older patients were 14.2 (95% CI, 7.9-25.4), and 9.0 (95% CI, 4.9-16.5), respectively.
RR and treatment modalities
Figure 7 shows the random-effects model for the RR according to HL treatment modalities. Significant heterogeneity was demonstrated (I 2 = 87%). RT used as the sole therapeutic modality was associated with an almost 5-fold increase in risk (RR = 4.70; [95% CI, 3.28-6.75]), I 2 = 74%) and even higher rate (RR = 14.08; [95% CI, 9.93-19.98]) when RT was used for patients ≤ 30 years of age [32, 36, 41]. Two studies [24, 54], reported on the mantle field RT dose where there was a small difference in RR between dose < 40 Gy and ≥ 40 Gy (5.99, and 6.13, respectively). In the first study [24], 1 patient per 567 person-years risk versus 23 patients per 7876 person-years developed SBC in the lower versus higher RT dose, respectively. In the second study, 17 of 135 versus 18 of 109 patients developed SBC in the lower versus higher RT dose, respectively [54]. When reported, almost all SBC arose within or at the margin of RT field.
Summary statistics and corresponding forest plot for the relative risk ( RR ) of second breast cancer vs. treatment modalities. RRs were calculated using a random-effects model. (R radiotherapy, C chemotherapy, RC combined radiotherapy and chemotherapy).
Figure 7 also shows that adding any CT to RT numerically increased the risk as compared with the risk associated with RT only (RR = 5.65; [95%CI, 2.94-10.88], I 2 = 91%). Nevertheless, adding alkylating CT to RT did not abate SBC risk (RR = 6.59; [95% CI, 1.72-25.20), while the combination of RT and non-alkylating CT caused a non-significant effect (RR = 4.40; [95% CI, 0.83-23.38]) (data not shown). Noteworthy, only a few studies have provided enough data about the nature of CT offered. The current meta-analysis showed that the use of CT only was not associated with significant risk (RR = 1.19; [95% CI, 0.50-2.82], I 2 = 87%).
To explore the heterogeneity of the RR vs. therapeutic modalities, we performed a univariate analysis that showed an inverse association between lnRR and age at HL diagnosis, positive interaction with latency, and no significant effect for study size. The multivariate meta-regression analysis, however, only showed that younger age at diagnosis retained a significant independent risk (Table 3).
RR and additional contributing factors
Comparing HL patients diagnosed from 1960s to the early 1970s, late 1970s to early 1980s, and more recent years the reported RRs were 3.7, 5.9, and 10.7, respectively [23, 28, 48, 51, 55].
Table 4 shows data related to potential contributing factors. Pooled analysis was not attempted due to the small number of studies with sufficient data. Table 4 shows that HL patients who presented with mediastinal mass had higher risk compared with those without mediastinal mass. Table 4 also shows the inconsistency of the reported RR among those who had splenectomy versus those who did no, however, the findings were based on three studies only. Table 4 also shows the potential protective role of pelvic RT as reported by De Bruin et al. [55], where patients receiving that modality showed a risk that was not as high compared with those who did not. HL survivors who received RT had a higher risk of developing estrogen receptor (ER)-negative/progesterone receptor (PR)-negative SBC as compared with ER-positive/PR-positive tumors [57].
Discussion
HL has been a successful model for the development of effective treatment approach in clinical oncology. Long-term survivors of that disease have also allowed better recognition and understanding of the late effects of therapy. In a large cohort of 25,305 women with HL, and with 957 incidences of SBC reported from North American and European institutions, the current meta-analysis quantified the risk of SBC. The overall pooled analysis showed that there was an approximate 9-fold increase in the risk of SBC incidence (pooled RR = 8.23), and AER of 23 patients per 10,000 person-years.
Patients included in this meta-analysis developed HD at a median age of 23.7 years. There has been incongruity about the influence of younger age at HL diagnosis and the higher risk of SBC, where some studies have failed to prove that effect [39, 42]. The current meta-analysis clearly showed that younger age at HL diagnosis was associated with increased risk of SBC, and the risk remained after adjusting for other covariates. Moreover, we demonstrated that the RR of SBC for women who developed HL above the age of 40 years was not significant. It is presumed that the higher risk associated with young age at HD diagnosis is attributed to the effect of RT delivered at a time when breast tissue is proliferating.
RT used as the sole therapeutic modality was associated with a 5-fold (RR = 4.70) increase in risk and a 14-fold (RR = 14.08) increase among young (≤ 30 years of age). Almost all SBC arose within or at the margin of the RT field. The RR of combined RT and any CT was slightly higher than that associated with RT only (5.65 vs. 4.70). An even higher, was the RR associated with the combination of RT and alkylating CT (RR = 6.59), thus, the potential protective effect of gonado-toxic alkylating CT was not demonstrated. Several studies showed an inverse association between the use of alkylating CT in HL and SBC risk [24, 65], however, other investigators reported increased risk [30, 66]. In this meta-analysis and based on data reported from three studies, the risk associated with the combination of RT and non-alkylating CT was not significant [37, 54, 58], also found insignificant, was the risk related to the use of CT only.
Analysis of potential additional risk factors was limited due to lack of sufficient data and/or inability to compute missing information, therefore, cautions should be exerted in interpreting results. Two studies [24, 54], reported on the mantle field RT dose where there was only a small difference in RR between dose < 40 Gy and ≥ 40 Gy (5.99, and 6.13, respectively). While some studies showed that subjects with SBC were found to be significantly more likely to have received higher doses of mantle RT [52], this observation was complicated by the fact that patients treated with higher radiation doses have had longer follow-up. Guibout et al. [46], did not find a significant association between RT dose and SBC, suggesting that the increased risk after HL may indicate a specific susceptibility for developing SBC, or a particular susceptibility to radiation and/or chemotherapy, or both. Conversely, De Bruin et al. showed that the risk of SBC is related to the RT volume [55], where mantle field irradiation was associated with a 2.7-fold increased risk of SBC compared with mediastinal irradiation alone. Besides, the meta-analysis reported by Franklin et al. showed a RR of 3 comparing extended field versus involved field RT [14].
The reason for failing to show a convincing evidence of RT dose–response effect associated with SBC risk is at best divisive. There is evidence for a strongly linear radiation dose response, but only in the lower dose range (up to 5 or 10 Gy) [67, 68]. It has been suggested that cell killing tends to decrease the carcinogenic effect of RT along an exponential curve at doses above 10 Gy [69]. However, it is known that BC is a known complication of low-dose breast radiation [67], thus BC may remain a risk among adolescent women who receive any dose of thoracic irradiation for HL.
Although new RT techniques and treatment strategies have the potential to reduce the future burden of late effects, nevertheless, we have shown that an even higher risk was reported in more recent years suggesting that there remains a significant cohort at an increased risk of SBC.
Pelvic RT was found to be associated with a protective effect as reported by De Bruin et al. [55]. The same effect was also noted by Basu et al., where 3.4% of patients who developed SBC received pelvic RT as compared with 26.3% among those who did not [52]. It is presumed that the protective effect of pelvic RT is attributed to the induction of premature menopause and the role played by hormone stimulation in RT-induced breast carcinogenesis [43, 70]. The influence of splenectomy on SBC risk has been controversial. While some studies reported a modest higher risk [71], other studies failed to show that effect [30, 52].
Only one study examined the receptor status of SBC [57]. The RR of ER-negative/PR-negative SBC was 66% higher than ER-positive/PR-positive SBC among 5-year HL survivors, and nearly two-fold higher among 15-year survivors. Conversely, other studies of small numbers of SBC patients have not found a significant variation in hormone-receptor status when compared with primary BC controls [72, 73]. While the incidence of hormone receptor-positive BC in the general population exceeds that of ER-negative/PR-negative BC, it is postulated, however, that young women treated for HL may experience premature ovarian failure related to HL therapy, and therefore, their hormonal BC risk factors may differ from those in the general population.
The present meta-analysis has several limitations. First, it is not possible to completely exclude the possibility that the HL itself carries with it an increased risk of second malignancy including SBC. Second, it is very difficult to quantify the possible effect of confounding factors such as lifestyle factors, personal risk, family history, etc. For example, Landgren et al. found increased RR (1.81) of breast cancer among HL patient with positive (vs. negative) family history of cancer [50]. Third, the analyses showed significant heterogeneity in risk estimate, nevertheless, investigating heterogeneity using meta-regression technique showed the dominant role of age at HL diagnosis. Other limitations include the lack of comprehensive treatment data including information on RT dose and additional treatments, and the lack of sufficient data to model the protective effect of endogenous hormone ablation against the risk associated with exposure to exogenous hormones. Moreover, it is not clear if a similar magnitude of risk is to be expected in a different patient population where the incidence of sporadic BC is low. Finally, the meta-analysis lacks the analysis of SBC outcome. However, SBC incidence rather its mortality was the main objective of the meta-analysis. Moreover, not all studies reported on mortality, besides, analysis of SBC mortality would be confounded by the mortality from HL itself or its therapy-related effect, ascertainment of the cause of death, age of diagnosis of HL or SBC, and length of follow-up.
Conclusions
We conclude that the current meta-analysis provided the most recent comprehensive estimate of the risk of SBC in a broad-range of HL survivors with inclusive analysis of relevant clinical and treatment variables. Based on the derived data where the median age at the diagnosis of SBC was 35.0 years and at a median latency of 17.7 years, screening recommendations for HL survivors need to be reemphasized. The results from the current meta-analysis support the favorable outcome of the risk-guided BC screening for such patients according to three prospective studies [74–76]. It is probably more appropriate that female patients with HL who are at a higher risk for developing SBC to be screened annually and at an earlier age rather than biennially starting at the age of 50 years as currently recommended for general population [77]. Our data also support the recent trend of risk-adapted management of HL to reduce the risk of short- and long-term adverse events associated with needless overtreatment [78].
References
Herbst C, Rehan FA, Skoetz N, Bohlius J, Brillant C, Schulz H, Monsef I, Specht L, Engert A: Chemotherapy alone versus chemotherapy plus radiotherapy for early stage Hodgkin lymphoma. Cochrane Database Syst Rev. 2011, 2: CD007110-
Rathore B, Kadin ME: Hodgkin's lymphoma therapy: past, present, and future. Expert Opin Pharmacother. 2010, 11 (17): 2891-2906. 10.1517/14656566.2010.515979.
Evens AM, Hutchings M, Diehl V: Treatment of Hodgkin lymphoma: the past, present, and future. Nat Clin Pract Oncol. 2008, 5 (9): 543-556. 10.1038/ncponc1186.
Weiner MA, Leventhal B, Brecher ML, Marcus RB, Cantor A, Gieser PW, Ternberg JL, Behm FG, Wharam MD, Chauvenet AR: Randomized study of intensive MOPP-ABVD with or without low-dose total-nodal radiation therapy in the treatment of stages IIB, IIIA2, IIIB, and IV Hodgkin's disease in pediatric patients: a Pediatric Oncology Group study. J Clin Oncol. 1997, 15 (8): 2769-2779.
Hodgson DC, Hudson MM, Constine LS: Pediatric hodgkin lymphoma: maximizing efficacy and minimizing toxicity. Semin Radiat Oncol. 2007, 17 (3): 230-242. 10.1016/j.semradonc.2007.02.009.
Canellos GP: Letter: second malignancies complicating Hodgkin's disease in remission. Lancet. 1975, 1 (7919): 1294-
Baxi SS, Matasar MJ: State-of-the-art issues in Hodgkin's lymphoma survivorship. Curr Oncol Rep. 2010, 12 (6): 366-373. 10.1007/s11912-010-0123-2.
Miller AB, Howe GR, Sherman GJ, Lindsay JP, Yaffe MJ, Dinner PJ, Risch HA, Preston DL: Mortality from breast cancer after irradiation during fluoroscopic examinations in patients being treated for tuberculosis. N Engl J Med. 1989, 321 (19): 1285-1289. 10.1056/NEJM198911093211902.
Tokunaga M, Land CE, Yamamoto T, Asano M, Tokuoka S, Ezaki H, Nishimori I: Incidence of female breast cancer among atomic bomb survivors, Hiroshima and Nagasaki, 1950–1980. Radiat Res. 1987, 112 (2): 243-272. 10.2307/3577254.
Neugut AI, Weinberg MD, Ahsan H, Rescigno J: Carcinogenic effects of radiotherapy for breast cancer. Oncology (Williston Park). 1999, 13 (9): 1261-1245. discussion 1257
Wolf J, Schellong G, Diehl V: Breast cancer following treatment of Hodgkin's disease–more reasons for less radiotherapy?. Eur J Cancer. 1997, 33 (14): 2293-2294.
Rieche K: Carcinogenicity of antineoplastic agents in man. Cancer Treat Rev. 1984, 11 (1): 39-67. 10.1016/0305-7372(84)90016-1.
Dorr FA, Coltman CA: Second cancers following antineoplastic therapy. Curr Probl Cancer. 1985, 9 (2): 1-43. 10.1016/S0147-0272(85)80033-7.
Franklin J, Pluetschow A, Paus M, Specht L, Anselmo AP, Aviles A, Biti G, Bogatyreva T, Bonadonna G, Brillant C, et al: Second malignancy risk associated with treatment of Hodgkin's lymphoma: meta-analysis of the randomised trials. Ann Oncol. 2006, 17 (12): 1749-1760. 10.1093/annonc/mdl302.
Henderson TO, Amsterdam A, Bhatia S, Hudson MM, Meadows AT, Neglia JP, Diller LR, Constine LS, Smith RA, Mahoney MC, et al: Systematic review: surveillance for breast cancer in women treated with chest radiation for childhood, adolescent, or young adult cancer. Ann Intern Med. 2010, 152 (7): 444-455. W144-454
Vandenbroucke JP, von Elm E, Altman DG, Gotzsche PC, Mulrow CD, Pocock SJ, Poole C, Schlesselman JJ, Egger M: Strengthening the reporting of observational studies in epidemiology (STROBE): explanation and elaboration. Epidemiology. 2007, 18 (6): 805-835. 10.1097/EDE.0b013e3181577511.
Clayton D, Hills M: Statistical Models in Epidemiology. 1993, Oxford, England, Oxford University Press
Alder N, Fenty J, Warren F, Sutton AJ, Rushton L, Jones DR, Abrams KR: Meta-analysis of mortality and cancer incidence among workers in the synthetic rubber-producing industry. Am J Epidemiol. 2006, 164 (5): 405-420. 10.1093/aje/kwj252.
Higgins JP, Thompson SG: Quantifying heterogeneity in a meta-analysis. Stat Med. 2002, 21 (11): 1539-1558. 10.1002/sim.1186.
Higgins JP, Thompson SG, Deeks JJ, Altman DG: Measuring inconsistency in meta-analyses. BMJ. 2003, 327 (7414): 557-560. 10.1136/bmj.327.7414.557.
DerSimonian R, Laird N: Meta-analysis in clinical trials. Control Clin Trials. 1986, 7 (3): 177-188. 10.1016/0197-2456(86)90046-2.
Egger M, Davey Smith G, Schneider M, Minder C: Bias in meta-analysis detected by a simple, graphical test. BMJ. 1997, 315 (7109): 629-634. 10.1136/bmj.315.7109.629.
Coleman MP, Bell CM, Fraser P: Second primary malignancy after Hodgkin's disease, ovarian cancer and cancer of the testis: a population-based cohort study. Br J Cancer. 1987, 56 (3): 349-355. 10.1038/bjc.1987.201.
Hancock SL, Tucker MA, Hoppe RT: Breast cancer after treatment of Hodgkin's disease. J Natl Cancer Inst. 1993, 85 (1): 25-31. 10.1093/jnci/85.1.25.
van Leeuwen FE, Klokman WJ, Hagenbeek A, Noyon R, van den Belt-Dusebout AW, van Kerkhoff EH, van Heerde P, Somers R: Second cancer risk following Hodgkin's disease: a 20-year follow-up study. J Clin Oncol. 1994, 12 (2): 312-325.
Mauch PM, Kalish LA, Marcus KC, Coleman CN, Shulman LN, Krill E, Come S, Silver B, Canellos GP, Tarbell NJ: Second malignancies after treatment for laparotomy staged IA-IIIB Hodgkin's disease: long-term analysis of risk factors and outcome. Blood. 1996, 87 (9): 3625-3632.
Sankila R, Garwicz S, Olsen JH, Dollner H, Hertz H, Kreuger A, Langmark F, Lanning M, Moller T, Tulinius H: Risk of subsequent malignant neoplasms among 1,641 Hodgkin's disease patients diagnosed in childhood and adolescence: a population-based cohort study in the five Nordic countries. Association of the Nordic Cancer Registries and the Nordic Society of Pediatric Hematology and Oncology. J Clin Oncol. 1996, 14 (5): 1442-1446.
Aisenberg AC, Finkelstein DM, Doppke KP, Koerner FC, Boivin JF, Willett CG: High risk of breast carcinoma after irradiation of young women with Hodgkin's disease. Cancer. 1997, 79 (6): 1203-1210. 10.1002/(SICI)1097-0142(19970315)79:6<1203::AID-CNCR20>3.0.CO;2-2.
Hudson MM, Poquette CA, Lee J, Greenwald CA, Shah A, Luo X, Thompson EI, Wilimas JA, Kun LE, Crist WM: Increased mortality after successful treatment for Hodgkin's disease. J Clin Oncol. 1998, 16 (11): 3592-3600.
Wolden SL, Lamborn KR, Cleary SF, Tate DJ, Donaldson SS: Second cancers following pediatric Hodgkin's disease. J Clin Oncol. 1998, 16 (2): 536-544.
Gervais-Fagnou DD, Girouard C, Laperriere N, Pintillie M, Goss PE: Breast cancer in women following supradiaphragmatic irradiation for Hodgkin's disease. Oncology. 1999, 57 (3): 224-231. 10.1159/000012035.
Munker R, Grutzner S, Hiller E, Aydemir U, Enne W, Dietzfelbinger H, Busch M, Haas R, Emmerich B, Schmidt M, et al: Second malignancies after Hodgkin's disease: the Munich experience. Ann Hematol. 1999, 78 (12): 544-554. 10.1007/s002770050556.
Garwicz S, Anderson H, Olsen JH, Dollner H, Hertz H, Jonmundsson G, Langmark F, Lanning M, Moller T, Sankila R, et al: Second malignant neoplasms after cancer in childhood and adolescence: a population-based case–control study in the 5 Nordic countries. The Nordic Society for Pediatric Hematology and Oncology. The Association of the Nordic Cancer Registries. Int J Cancer. 2000, 88 (4): 672-678. 10.1002/1097-0215(20001115)88:4<672::AID-IJC24>3.0.CO;2-N.
Green DM, Hyland A, Barcos MP, Reynolds JA, Lee RJ, Hall BC, Zevon MA: Second malignant neoplasms after treatment for Hodgkin's disease in childhood or adolescence. J Clin Oncol. 2000, 18 (7): 1492-1499.
Metayer C, Lynch CF, Clarke EA, Glimelius B, Storm H, Pukkala E, Joensuu T, Van Leeuwen FE, Van't Veer MB, Curtis RE, et al: Second cancers among long-term survivors of Hodgkin's disease diagnosed in childhood and adolescence. J Clin Onco. 2000, 18 (12): 2435-2443.
Swerdlow AJ, Barber JA, Hudson GV, Cunningham D, Gupta RK, Hancock BW, Horwich A, Lister TA, Linch DC: Risk of second malignancy after Hodgkin's disease in a collaborative British cohort: the relation to age at treatment. J Clin Oncol. 2000, 18 (3): 498-509.
Wolden SL, Hancock SL, Carlson RW, Goffinet DR, Jeffrey SS, Hoppe RT: Management of breast cancer after Hodgkin's disease. J Clin Oncol. 2000, 18 (4): 765-772.
Cellai E, Magrini SM, Masala G, Alterini R, Costantini AS, Rigacci L, Olmastroni L, Papi MG, Spediacci MA, Innocenti F, et al: The risk of second malignant tumors and its consequences for the overall survival of Hodgkin's disease patients and for the choice of their treatment at presentation: analysis of a series of 1524 cases consecutively treated at the Florence University Hospital. Int J Radiat Oncol Biol Phys. 2001, 49 (5): 1327-1337. 10.1016/S0360-3016(00)01513-3.
Neglia JP, Friedman DL, Yasui Y, Mertens AC, Hammond S, Stovall M, Donaldson SS, Meadows AT, Robison LL: Second malignant neoplasms in five-year survivors of childhood cancer: childhood cancer survivor study. J Natl Cancer Inst. 2001, 93 (8): 618-629. 10.1093/jnci/93.8.618.
Foss Abrahamsen A, Andersen A, Nome O, Jacobsen AB, Holte H, Foss Abrahamsen J, Kvaloy S: Long-term risk of second malignancy after treatment of Hodgkin's disease: the influence of treatment, age and follow-up time. Ann Oncol. 2002, 13 (11): 1786-1791. 10.1093/annonc/mdf289.
Ng AK, Bernardo MV, Weller E, Backstrand K, Silver B, Marcus KC, Tarbell NJ, Stevenson MA, Friedberg JW, Mauch PM: Second malignancy after Hodgkin disease treated with radiation therapy with or without chemotherapy: long-term risks and risk factors. Blood. 2002, 100 (6): 1989-1996. 10.1182/blood-2002-02-0634.
Bhatia S, Yasui Y, Robison LL, Birch JM, Bogue MK, Diller L, DeLaat C, Fossati-Bellani F, Morgan E, Oberlin O, et al: High risk of subsequent neoplasms continues with extended follow-up of childhood Hodgkin's disease: report from the Late Effects Study Group. J Clin Oncol. 2003, 21 (23): 4386-4394. 10.1200/JCO.2003.11.059.
Travis LB, Hill DA, Dores GM, Gospodarowicz M, van Leeuwen FE, Holowaty E, Glimelius B, Andersson M, Wiklund T, Lynch CF, et al: Breast cancer following radiotherapy and chemotherapy among young women with Hodgkin disease. JAMA. 2003, 290 (4): 465-475. 10.1001/jama.290.4.465.
Wahner-Roedler DL, Nelson DF, Croghan IT, Achenbach SJ, Crowson CS, Hartmann LC, O'Fallon WM: Risk of breast cancer and breast cancer characteristics in women treated with supradiaphragmatic radiation for Hodgkin lymphoma: Mayo Clinic experience. Mayo Clin Proc. 2003, 78 (6): 708-715. 10.4065/78.6.708.
Kenney LB, Yasui Y, Inskip PD, Hammond S, Neglia JP, Mertens AC, Meadows AT, Friedman D, Robison LL, Diller L: Breast cancer after childhood cancer: a report from the childhood cancer survivor study. Ann Intern Med. 2004, 141 (8): 590-597.
Guibout C, Adjadj E, Rubino C, Shamsaldin A, Grimaud E, Hawkins M, Mathieu MC, Oberlin O, Zucker JM, Panis X, et al: Malignant breast tumors after radiotherapy for a first cancer during childhood. J Clin Oncol. 2005, 23 (1): 197-204.
Travis LB, Hill D, Dores GM, Gospodarowicz M, van Leeuwen FE, Holowaty E, Glimelius B, Andersson M, Pukkala E, Lynch CF, et al: Cumulative absolute breast cancer risk for young women treated for Hodgkin lymphoma. J Natl Cancer Inst. 2005, 97 (19): 1428-1437. 10.1093/jnci/dji290.
Hodgson DC, Gilbert ES, Dores GM, Schonfeld SJ, Lynch CF, Storm H, Hall P, Langmark F, Pukkala E, Andersson M, et al: Long-term solid cancer risk among 5-year survivors of Hodgkin's lymphoma. J Clin Oncol. 2007, 25 (12): 1489-1497. 10.1200/JCO.2006.09.0936.
Koh ES, Tran TH, Heydarian M, Sachs RK, Tsang RW, Brenner DJ, Pintilie M, Xu T, Chung J, Paul N, et al: A comparison of mantle versus involved-field radiotherapy for Hodgkin's lymphoma: reduction in normal tissue dose and second cancer risk. Radiat Oncol. 2007, 2: 13-10.1186/1748-717X-2-13.
Landgren O, Pfeiffer RM, Stewart L, Gridley G, Mellemkjaer L, Hemminki K, Goldin LR, Travis LB: Risk of second malignant neoplasms among lymphoma patients with a family history of cancer. Int J Cancer. 2007, 120 (5): 1099-1102.
Taylor AJ, Winter DL, Stiller CA, Murphy M, Hawkins MM: Risk of breast cancer in female survivors of childhood Hodgkin's disease in Britain: a population-based study. Int J Cancer. 2007, 120 (2): 384-391. 10.1002/ijc.22261.
Basu SK, Schwartz C, Fisher SG, Hudson MM, Tarbell N, Muhs A, Marcus KJ, Mendenhall N, Mauch P, Kun LE, et al: Unilateral and bilateral breast cancer in women surviving pediatric Hodgkin's disease. Int J Radiat Oncol Biol Phys. 2008, 72 (1): 34-40. 10.1016/j.ijrobp.2008.04.068.
Constine LS, Tarbell N, Hudson MM, Schwartz C, Fisher SG, Muhs AG, Basu SK, Kun LE, Ng A, Mauch P, et al: Subsequent malignancies in children treated for Hodgkin's disease: associations with gender and radiation dose. Int J Radiat Oncol Biol Phys. 2008, 72 (1): 24-33. 10.1016/j.ijrobp.2008.04.067.
Alm El-Din MA, Hughes KS, Finkelstein DM, Betts KA, Yock TI, Tarbell NJ, Aisenberg AC, Taghian AG: Breast cancer after treatment of Hodgkin's lymphoma: risk factors that really matter. Int J Radiat Oncol Biol Phys. 2009, 73 (1): 69-74. 10.1016/j.ijrobp.2008.03.066.
De Bruin ML, Sparidans J, Van't Veer MB, Noordijk EM, Louwman MW, Zijlstra JM, Van Den Berg H, Russell NS, Broeks A, Baaijens MH, et al: Breast cancer risk in female survivors of Hodgkin's lymphoma: lower risk after smaller radiation volumes. J Clin Oncol. 2009, 27 (26): 4239-4246. 10.1200/JCO.2008.19.9174.
Howell SJ, Searle C, Goode V, Gardener T, Linton K, Cowan RA, Harris MA, Hopwood P, Swindell R, Norman A, et al: The UK national breast cancer screening programme for survivors of Hodgkin lymphoma detects breast cancer at an early stage. Br J Cancer. 2009, 101 (4): 582-588. 10.1038/sj.bjc.6605215.
Dores GM, Anderson WF, Beane Freeman LE, Fraumeni JF, Curtis RE: Risk of breast cancer according to clinicopathologic features among long-term survivors of Hodgkin's lymphoma treated with radiotherapy. Br J Cancer. 2010, 103 (7): 1081-1084. 10.1038/sj.bjc.6605877.
O'Brien MM, Donaldson SS, Balise RR, Whittemore AS, Link MP: Second malignant neoplasms in survivors of pediatric Hodgkin's lymphoma treated with low-dose radiation and chemotherapy. J Clin Oncol. 2010, 28 (7): 1232-1239. 10.1200/JCO.2009.24.8062.
Castellino SM, Geiger AM, Mertens AC, Leisenring WM, Tooze JA, Goodman P, Stovall M, Robison LL, Hudson MM: Morbidity and mortality in long-term survivors of Hodgkin lymphoma: a report from the Childhood Cancer Survivor Study. Blood. 2011, 117 (6): 1806-1816. 10.1182/blood-2010-04-278796.
Behringer K, Josting A, Schiller P, Eich HT, Bredenfeld H, Diehl V, Engert A: Solid tumors in patients treated for Hodgkin's disease: a report from the German Hodgkin Lymphoma Study Group. Ann Oncol. 2004, 15 (7): 1079-1085. 10.1093/annonc/mdh273.
Inskip PD, Curtis RE: New malignancies following childhood cancer in the United States, 1973–2002. Int J Cancer. 2007, 121 (10): 2233-2240. 10.1002/ijc.22827.
Swerdlow AJ, Higgins CD, Smith P, Cunningham D, Hancock BW, Horwich A, Hoskin PJ, Lister TA, Radford JA, Rohatiner AZ, et al: Second cancer risk after chemotherapy for hodgkin's lymphoma: a collaborative british cohort study. J Clin Oncol. 2011, 29 (31): 4096-4104. 10.1200/JCO.2011.34.8268.
Janov AJ, Tulecke M, O'Neill A, Lester S, Mauch PM, Harris J, Schnitt SJ, Shapiro CL: Clinical and pathologic features of breast cancers in women treated for Hodgkin's disease: a case–control study. Breast J. 2001, 7 (1): 46-52. 10.1046/j.1524-4741.2001.007001046.x.
Hill DA, Gilbert E, Dores GM, Gospodarowicz M, van Leeuwen FE, Holowaty E, Glimelius B, Andersson M, Wiklund T, Lynch CF, et al: Breast cancer risk following radiotherapy for Hodgkin lymphoma: modification by other risk factors. Blood. 2005, 106 (10): 3358-3365. 10.1182/blood-2005-04-1535.
Tucker MA, Coleman CN, Cox RS, Varghese A, Rosenberg SA: Risk of second cancers after treatment for Hodgkin's disease. N Engl J Med. 1988, 318 (2): 76-81. 10.1056/NEJM198801143180203.
Kaldor JM, Day NE, Clarke EA, Van Leeuwen FE, Henry-Amar M, Fiorentino MV, Bell J, Pedersen D, Band P, Assouline D, et al: Leukemia following Hodgkin's disease. N Engl J Med. 1990, 322 (1): 7-13. 10.1056/NEJM199001043220102.
Boice JD: Radiation and breast carcinogenesis. Med Pediatr Oncol. 2001, 36 (5): 508-513. 10.1002/mpo.1122.
Preston DL, Mattsson A, Holmberg E, Shore R, Hildreth NG, Boice JD: Radiation effects on breast cancer risk: a pooled analysis of eight cohorts. Radiat Res. 2002, 158 (2): 220-235. 10.1667/0033-7587(2002)158[0220:REOBCR]2.0.CO;2.
Harris JR, Lippman ME, Veronesi U, Willett W: Breast cancer (1). N Engl J Med. 1992, 327 (5): 319-328. 10.1056/NEJM199207303270505.
Van Leeuwen FE, Klokman WJ, Stovall M, Dahler EC, Van't Veer MB, Noordijk EM, Crommelin MA, Aleman BM, Broeks A, Gospodarowicz M, et al: Roles of radiation dose, chemotherapy, and hormonal factors in breast cancer following Hodgkin's disease. J Natl Cancer Inst. 2003, 95 (13): 971-980. 10.1093/jnci/95.13.971.
Chung CT, Bogart JA, Adams JF, Sagerman RH, Numann PJ, Tassiopoulos A, Duggan DB: Increased risk of breast cancer in splenectomized patients undergoing radiation therapy for Hodgkin's disease. Int J Radiat Oncol Biol Phys. 1997, 37 (2): 405-409. 10.1016/S0360-3016(96)00498-1.
Gaffney DK, Hemmersmeier J, Holden J, Marshall J, Smith LM, Avizonis V, Tran T, Neuhausen SL: Breast cancer after mantle irradiation for Hodgkin's disease: correlation of clinical, pathologic, and molecular features including loss of heterozygosity at BRCA1 and BRCA2. Int J Radiat Oncol Biol Phys. 2001, 49 (2): 539-546. 10.1016/S0360-3016(00)01481-4.
Castiglioni F, Terenziani M, Carcangiu ML, Miliano R, Aiello P, Bertola L, Triulzi T, Gasparini P, Camerini T, Sozzi G, et al: Radiation effects on development of HER2-positive breast carcinomas. Clin Cancer Res. 2007, 13 (1): 46-51. 10.1158/1078-0432.CCR-06-1490.
Diller L, Medeiros Nancarrow C, Shaffer K, Matulonis U, Mauch P, Neuberg D, Tarbell NJ, Litman H, Garber J: Breast cancer screening in women previously treated for Hodgkin's disease: a prospective cohort study. J Clin Oncol. 2002, 20 (8): 2085-2091. 10.1200/JCO.2002.08.031.
Kwong A, Hancock SL, Bloom JR, Pal S, Birdwell RL, Mariscal C, Ikeda DM: Mammographic screening in women at increased risk of breast cancer after treatment of Hodgkin's disease. Breast J. 2008, 14 (1): 39-48. 10.1111/j.1524-4741.2007.00524.x.
Lee L, Pintilie M, Hodgson DC, Goss PE, Crump M: Screening mammography for young women treated with supradiaphragmatic radiation for Hodgkin's lymphoma. Ann Oncol. 2008, 19 (1): 62-67.
Gregory KD, Sawaya GF: Updated recommendations for breast cancer screening. Curr Opin Obstet Gynecol. 2010, 22 (6): 498-505. 10.1097/GCO.0b013e3283404e71.
Hodgson DC: Late effects in the era of modern therapy for Hodgkin lymphoma. Hematology Am Soc Hematol Educ Program. 2011, 2011: 323-329. 10.1182/asheducation-2011.1.323.
Pre-publication history
The pre-publication history for this paper can be accessed here:http://www.biomedcentral.com/1471-2407/12/197/prepub
Author information
Authors and Affiliations
Corresponding author
Additional information
Competing interests
All authors declare that they have no competing interests.
Authors’ contributions
EMI, KMA, GAK, OAA, and MA Conception and design of the meta-analysis. EMI Study coordination and tasks’ assignment. KMA, and GAK Initial literature search. EMI, KMA, GAK, OAA, and MA Review of all potential studies. EMI, KMA, GAK, OAA, and MA Data extraction. EMI, KMA, GAK, OAA, and MA Assessing quality of included studies. EMI Statistical analysis. EMI, KMA, and GAK Investigating heterogeneity. EMI, KMA, GAK, OAA, and MA Preparation of the manuscript. EMI, KMA, GAK, OAA, and MA Reading the final manuscript. EMI, KMA, GAK, OAA, and MA Approval of the final manuscript. All authors read and approved the final manuscript.
Authors’ original submitted files for images
Below are the links to the authors’ original submitted files for images.
Rights and permissions
This article is published under license to BioMed Central Ltd. This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
About this article
Cite this article
Ibrahim, E.M., Abouelkhair, K.M., Kazkaz, G.A. et al. Risk of second breast cancer in female Hodgkin’s lymphoma survivors: a meta-analysis. BMC Cancer 12, 197 (2012). https://doi.org/10.1186/1471-2407-12-197
Received:
Accepted:
Published:
DOI: https://doi.org/10.1186/1471-2407-12-197