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Open Access 01.12.2013 | Research article

Obesity and survival in operable breast cancer patients treated with adjuvant anthracyclines and taxanes according to pathological subtypes: a pooled analysis

verfasst von: Bella Pajares, Marina Pollán, Miguel Martín, John R Mackey, Ana Lluch, Joaquín Gavila, Charles Vogel, Manuel Ruiz-Borrego, Lourdes Calvo, Tadeusz Pienkowski, Álvaro Rodríguez-Lescure, Miguel Angel Seguí, Olivier Tredan, Antonio Antón, Manuel Ramos, María del Carmen Cámara, César Rodríguez-Martín, Eva Carrasco, Emilio Alba

Erschienen in: Breast Cancer Research | Ausgabe 6/2013

Abstract

Introduction

Obesity is an unfavorable prognostic factor in breast cancer (BC) patients regardless of menopausal status and treatment received. However, the association between obesity and survival outcome by pathological subtype requires further clarification.

Methods

We performed a retrospective analysis including 5,683 operable BC patients enrolled in four randomized clinical trials (GEICAM/9906, GEICAM/9805, GEICAM/2003–02, and BCIRG 001) evaluating anthracyclines and taxanes as adjuvant treatments. Our primary aim was to assess the prognostic effect of body mass index (BMI) on disease recurrence, breast cancer mortality (BCM), and overall mortality (OM). A secondary aim was to detect differences of such prognostic effects by subtype.

Results

Multivariate survival analyses adjusting for age, tumor size, nodal status, menopausal status, surgery type, histological grade, hormone receptor status, human epidermal growth factor receptor 2 (HER2) status, chemotherapy regimen, and under-treatment showed that obese patients (BMI 30.0 to 34.9) had similar prognoses to that of patients with a BMI < 25 (reference group) in terms of recurrence (Hazard Ratio [HR] = 1.08, 95% Confidence Interval [CI] = 0.90 to 1.30), BCM (HR = 1.02, 0.81 to 1.29), and OM (HR = 0.97, 0.78 to 1.19). Patients with severe obesity (BMI ≥ 35) had a significantly increased risk of recurrence (HR = 1.26, 1.00 to 1.59, P = 0.048), BCM (HR = 1.32, 1.00 to 1.74, P = 0.050), and OM (HR = 1.35, 1.06 to 1.71, P = 0.016) compared to our reference group. The prognostic effect of severe obesity did not vary by subtype.

Conclusions

Severely obese patients treated with anthracyclines and taxanes present a worse prognosis regarding recurrence, BCM, and OM than patients with BMI < 25. The magnitude of the harmful effect of BMI on survival-related outcomes was similar across subtypes.

Additional file 1: List of Institutional Review Boards.(PDF 59 KB)

Additional file 2: Characteristics of women enrolled in the four clinical trials.(PDF 76 KB)

Authors’ original file for figure 1

Authors’ original file for figure 2

Authors’ original file for figure 3

Electronic supplementary material

The online version of this article (doi:10.1186/bcr3572) contains supplementary material, which is available to authorized users.

Bella Pajares, Marina Pollán contributed equally to this work.

Competing interests

All authors declare that they have no competing interests.

Authors’ contributions

BP, MP, and EA conceived the study. MM, JRM, AL, JG, CV, MRB, LC, TP, ARL, MAS, OT, AA, MR, MCC, CRM, EC and EA contributed to data collection. MP analyzed the data. BP and MP interpreted the results and wrote the first draft. All authors contributed to the writing and editing of the manuscript and approved the final version. EA had full access to all the data in the study and had final responsibility for the decision to submit for publication.

Breast cancer

BCIRG

Breast Cancer International Research Group

BCM

Breast cancer mortality

BMI

Body mass index

CMF

Cyclophosphamide, methotrexate, fluorouracil

Chemotherapy

Estrogen receptor

FAC

Fluorouracil, doxorubicin, cyclophosphamide

FEC

Fluorouracil, epirubicin, and cyclophosphamide

GEICAM

Spanish Breast Cancer Research Group

HER2

Human epidermal growth factor-2

Hazard ratio

Overall mortality

Progesterone receptor

RCT

Randomized controlled trial

Radiotherapy

TAC

Docetaxel, doxorubicin, cyclophosphamide

TNF

Tumor necrosis factor.

Introduction

Breast cancer (BC) is the most frequent invasive neoplasm in women. By 2015 the annual global incidence of BC is estimated at 1.6 million women [1]. The incidence in Europe alone will be over 450,000 new cases, resulting in 138,000 deaths [1]. Among others, obesity is a risk factor for several types of cancer, including BC [2], and has recently gained special relevance due in part to the dramatic increase in the prevalence of obesity observed worldwide. In fact, if current trends continue, over 50% of the world’s population will be obese by the year 2030 [3].

Recent cohort studies show that BC patients who are obese at diagnosis exhibit worse outcomes than their normal-weight counterparts in terms of probability of recurrence, contralateral BC, second primary malignancies, and overall mortality (OM) [4, 5]. Whereas obese women may be at risk for being diagnosed at a more advanced stage of disease than other women, multivariate analyses confirm obesity as an independent prognostic factor for risk of recurrence and survival [5]. Additionally, recently published meta-analyses confirm a negative effect of obesity on BC prognosis [5‐8]. These data, however, are mostly based on cohort studies with several limitations, such as sample heterogeneity regarding tumor stage, treatment received, follow-up period, and the use of self-reported height and weight data to calculate body mass index (BMI).

The association between obesity and prognosis is also explored in several clinical trials restricted to patients with early-stage BC. These studies were in patients receiving different treatments (for example, hormone therapy, chemotherapy protocols with/without anthracyclines) and reported conflicting results [9‐15]. Although most of these studies showed an increased risk of death related to obesity, in the modern era of adjuvant anthracyclines and taxanes the association between BMI and disease recurrence and/or breast cancer mortality (BCM) requires further exploration together with an examination of the magnitude of such associations by pathological subtype, that is estrogen receptor (ER)/progesterone receptor (PR)-positive/human epidermal growth factor-2 (HER2)-negative, HER2-positive, triple-negative). The pooling of data from all patients participating in four high-quality randomized clinical trials with similar treatment and follow-up protocols offers a unique opportunity to assess the influence of BMI on clinical outcomes while minimizing unexplained variability commonly found in observational studies. Thus, the aim of this study was to assess the prognostic effect of BMI on recurrence, breast cancer mortality (BCM), and overall mortality (OM) among BC patients treated with adjuvant anthracyclines and taxanes, enrolled in four phase-III Spanish Breast Cancer Research Group (GEICAM) and Breast Cancer International Research Group (BCIRG) clinical trials (GEICAM/9906, GEICAM/9805, GEICAM/2003–02, and BCIRG 001) [16‐20]. We also evaluated the prognostic role of obesity according to the different pathological BC subtypes as defined by immunohistochemistry.

Methods

Study design and participants

The cohort is comprised of 98% Caucasian women (reflecting the breast cancer patient population in Spain, as most patients included in this pooled analyses were from this country) from four randomized trials that evaluated systemic adjuvant chemotherapy (CT) based on anthracyclines and taxanes for lymph node-negative and lymph node-positive operable BC. These phase III trials accrued patients between 1996 and 2008 and evaluated the following CT protocols: 1) six cycles of docetaxel, doxorubicin, and cyclophosphamide (TAC) or fluorouracil, doxorubicin, and cyclophosphamide (FAC) for high-risk node-negative patients (GEICAM/9805) [17]; 2) six cycles of fluorouracil, epirubicin, and cyclophosphamide (FEC) or four cycles of FEC followed by weekly paclitaxel for node-positive patients (GEICAM/9906) [16]; 3) six cycles of TAC or FAC for node-positive patients (BCIRG 001) [18, 19]; and 4) six cycles of FAC or four cycles of FAC followed by weekly paclitaxel for node-negative patients (GEICAM/2003-02) [20]. Chemotherapy was prescribed by actual body weight and was adjusted for obese patients in about 2% of patients (151 of 5,683 patients). After completing the CT treatment, tamoxifen, aromatase inhibitors, or the switching strategy (that is, tamoxifen followed by aromatase inhibitor) were administered for five years to patients with ER-positive and/or PR-positive tumors. Radiotherapy (RT) was mandatory after breast-conserving surgery and was administered after mastectomy, according to each institution’s guidelines. These trials were conducted before the approval of adjuvant trastuzumab therapy. Further details of the trial designs and findings have been reported elsewhere [16‐20].

The Institutional Review Boards at the study sites approved these trials (see Additional file 1 for a list), and the participants provided written informed consent prior to randomization. For this analysis, we excluded patients who were randomized but not included in the corresponding trial (32 patients) and those who had incomplete height or weight data (9 women). The final cohort consisted of 5,683 patients.

Procedure

The independent variable of interest, BMI, was calculated based on the height and weight of each participant at the start of the study. According to the World Health Organization definition, patients were classified into five BMI subgroups: underweight (<18.5 kg/m²), normal weight (18.5 to 24.9 kg/m²), overweight (25.0 to 29.9 kg/m²), obese (30.0 to 34.9 kg/m²) and severely obese (≥35.0 kg/m²) [21]. Due to the small number of underweight patients, the first two groups were combined and, thus, BMI <25 kg/m² was used as the reference category. Other variables considered included: age, menopausal status, surgery type, histology type, histological grade, tumor size, nodal status, hormone receptor, and HER2 status. We included the category, HER2 unknown, due to the high number of participants with missing data in the GEICAM/9805 study. Regarding CT, the overall dose of each drug in the corresponding regimen was compared with the theoretical dose based on the patient’s estimated body weight using the real weight of the patient at enrollment [22]. As in other studies, we considered women who received a dose lower than 85% of the standard dose as undertreated [23]. Undertreatment was computed considering the initial dose (initial undertreatment) and the total amount of CT received (overall undertreatment). Toxicity was graded according to the National Cancer Institute Common Toxicity Criteria; we considered grade 3 and 4 adverse events to be clinically relevant [24].

We calculated the impact of obesity on different endpoints. Recurrence was defined as local, regional, or distant disease recurrence or the diagnosis of a second primary breast cancer, including contralateral breast tumors. In situ tumors were not considered as recurrence. BCM was defined as death due to BC, and overall mortality was defined as death from any cause. To guarantee the quality and homogeneity of the follow-up data all analyses were restricted to the first 10 years after recruitment.

Statistical analysis

The Kaplan-Meier method was used to estimate survival, and the log-rank test was used to assess the possible differences between subgroups. Cox proportional hazards regression analysis was performed to assess the prognostic effect of BMI on recurrence, BCM, and OM [25]. Basic models were adjusted for the clinical trial from which data originated (study) - which also acted as a proxy for nodal involvement - and treatment regimen. Full models included additional adjustment for age, menopausal status, tumor size, histological grade, hormone receptor status, HER2 status, surgery type, and overall undertreatment (yes/no) as potential confounders. In addition, to explore the shape of the dose–response curve for BMI without assuming a linear relationship, natural splines were used in the full model, including four knots based on Harrell’s recommended percentiles, namely 5%, 35%, 65%, and 95% [26]. Finally, to test the consistency of the excess risk associated with higher BMI, subgroup analyses were conducted to estimate the effect of having BMI ≥35 compared to BMI <25 per category of the following variables: clinical trial, age, menopausal status, histological type, pathologic primary tumor size, nodal involvement, surgery type, hormone therapy (yes/no), undertreatment (yes/no), and pathological subtype. We report two-sided P-values, and P <0.05 was considered statistically significant. Statistical analyses were performed using STATA 12 (StataCorp LP, College Station, TX, USA).

Results

The characteristics of the patients enrolled in each trial are provided as additional material (see Additional file 2). In total, 5,683 patients from four phase III trials with complete height and weight data were analyzed in the pooled data. The median follow-up time of patients who were alive at the time of this analysis was 93.4 months (range from 0.6 to 120). Table 1 describes sociodemographic and clinical characteristics of the sample and illustrates the relationship between patient characteristics and BMI category. For the sole purpose of simplifying the sample description here, we combined BMI into three categories. Using 30 kg/m² as the cut off, 4,307 patients (75.8%) were classified as non-obese (BMI <30), 945 patients (16.6%) had BMI between 30 and 34.9 (obese) and 431 patients (7.8%) had BMI greater than or equal to 35 (severely obese). The median age was 48 years in the non-obese patients (range 42 to 56), 56 years among obese patients (range 49 to 62) and 55 years among the severely obese (range 49 to 62). Severely obese patients were more likely to be postmenopausal, to present lymph node positivity, and to be undertreated compared to non-obese patients. Additionally, severely obese patients were less likely to present with a tumor size <2 cm, undifferentiated tumors, or HER2-positive tumors. Even though the prevalence of undertreatment was low, as expected in clinical trials, there were significant differences in the doses (calculated as mg/m²) of CT between severely obese patients and non-obese patients. A higher proportion of severely obese patients received doses below 85% of the theoretical dose of CT compared with the non-obese patients (6.0% versus 2.4% in the first dose and 15.0% versus 7.1% considering the cumulative dose, P <0.001). Patients with severe obesity were as likely to present with severe adverse events (grades 3 to 4) as non-obese patients (42.0% versus 40.4%, P = 0.498).

Table 1

Distribution of variables by BMI category (non-obese, obese, and severely obese women)

	BMI <30.0	BMI 30 to 34.9	BMI ≥ 35.0
	Number (%)	Number (%)	Number (%)	P-value^a
Age at diagnosis, years				<0.001
20 to 44	1,473 (34.2%)	138 (14.6%)	56 (13.0%)
45 to 54	1,599 (37.1%)	284 (30.1%)	153 (35.5%)
55 to 64	932 (21.6%)	364 (38.5%)	147 (34.1%)
65 to 76	303 (7.0%)	159 (16.8%)	75 (17.4%)
Median (percentiles 25 to 75)	48 (42 to 56)	56 (49 to 62)	55 (49 to 62)
Menopausal status				<0.001
Postmenopausal	1,737 (40.3%)	631 (66.8%)	293 (68.0%)
Premenopausal	2,570 (59.7%)	314 (33.2%)	138 (32.0%)
Histology				0.730
Ductal	3,645 (84.6%)	788 (83.4%)	376 (87.2%)
Lobulillar	385 (8.9%)	93 (9.8%)	32 (7.4%)
Mixed	46 (1.1%)	12 (1.3%)	4 (0.9%)
Others	230 (5.3%)	52 (5.5%)	19 (4.4%)
Unknown	1 (0.0%)	0 (0.0%)	0 (0.0%)
Histological grade				0.054
1	384 (8.9%)	81 (8.6%)	34 (7.9%)
2	1,792 (41.6%)	416 (44.0%)	196 (45.5%)
3	1,823 (42.3%)	381 (40.3%)	187 (43.4%)
Unknown	308 (7.1%)	67 (7.1%)	14 (3.2%)
Pathologic primary tumor size				<0.001
T1	2,192 (50.9%)	423 (44.8%)	179 (41.5%)
T2	1,948 (45.2%)	485 (51.3%)	232 (53.8%)
T3	167 (3.9%)	37 (3.9%)	20 (4.6%)
Nodes				0.021
Negative	2,278 (52.9%)	487 (51.5%)	198 (45.9%)
Positive	2,029 (47.1%)	458 (48.5%)	233 (54.1%)
Estrogen receptor				0.647
Negative	1,398 (32.5%)	321 (34.0%)	137 (31.8%)
Positive	2,899 (67.3%)	623 (65.9%)	291 (67.5%)
Unknown	10 (0.2%)	1 (0.1%)	3 (0.7%)
Progesterone receptor				0.199
Negative	1,654 (38.4%)	373 (39.5%)	149 (34.6%)
Positive	2,576 (59.8%)	558 (59.0%)	276 (64.0%)
Unknown	77 (1.8%)	14 (1.5%)	6 (1.4%)
Human epidermal growth factor-2 status				0.030
Negative	3,036 (70.5%)	690 (73.0%)	329 (76.3%)
Positive	656 (15.2%)	123 (13.0%)	51 (11.8%)
Unknown	615 (14.3%)	132 (14.0%)	51 (11.8%)
Type of surgery				0.071
Mastectomy	2,021 (46.9%)	405 (42.9%)	195 (45.2%)
Conservative	2,286 (53.1%)	540 (57.1%)	236 (54.8%)
Hormonotherapy				0.334
None	1,068 (24.8%)	256 (27.1%)	115 (26.7%)
Yes	3,081 (71.5%)	664 (70.3%)	300 (69.6%)
Unknown	158 (3.7%)	25 (2.6%)	16 (3.7%)
Adverse events (grades 3,4)				0.498
No	2,565 (59.6%)	578 (61.2%)	250 (58.0%)
Yes	1,742 (40.4%)	367 (38.8%)	181 (42.0%)
Initial under-treatment (in the first dose) ^b				<0.001
No	4,205 (97.6%)	922 (97.6%)	405 (94.0%)
Yes	102 (2.4%)	23 (2.4%)	26 (6.0%)
Per type of treatment^c
Epirubicin <85%	5 (0.5%)	5 (2.3%)	4 (4.0%)	0.002
Cyclophosphamide <85%	12 (0.3%)	4 (0.4%)	8 (1.9%)	<0.001
Fluorouracil <85%	8 (0.2%)	4 (0.5%)	7 (2.2%)	<0.001
Doxorubicin <85%	4 (0.1%)	3 (0.4%)	7 (2.1%)	<0.001
Docetaxel <85%	24 (2.5%)	5 (2.4%)	6 (5.4%)	0.199
Paclitaxel <85%	62 (5.2%)	11 (4.2%)	7 (6.7%)	0.604
Overall undertreatment ^b				<0.001
No	3,903 (90.6%)	820 (86.8%)	360 (83.5%)
Yes	404 (9.4%)	125 (13.2%)	71 (16.5%)
Per type of treatment ^c
Epirubicin <85%	50 (5.5%)	15 (6.8%)	13 (13.1%)	0.011
Cyclophosphamide <85%	213 (4.9%)	49 (5.2%)	34 (7.9%)	0.032
Fluorouracil <85%	132 (3.9%)	25 (3.4%)	24 (7.5%)	0.005
Doxorubicin <85%	160 (4.7%)	40 (5.5%)	26 (7.8%)	0.040
Docetaxel <85%	117 (15.8%)	39 (18.9%)	10 (9.9%)	0.068
Paclitaxel <85%	159 (13.3%)	59 (22.6%)	26 (25.0%)	<0.001

^aP-values computed excluding women without information in the corresponding variable; ^bdefined as total dose received lower than 85% of the theoretical dose prescribed; ^cpercentages including only women receiving the corresponding type of treatment. BMI, body mass index.

To illustrate the relationship between BMI and survival, we calculated crude Kaplan-Meier curves for recurrence-free survival, breast cancer survival and overall survival for each BMI category (Figure 1). In the Cox regression basic model (Table 2), obese patients’ outcomes were not significantly different from those of the reference group (BMI18.5 to 24.9), in terms of recurrence (Hazard Ratio [HR] 0.98, 95% CI 0.82, 1.17, P = 0.831), BCM (HR 1.04, 95% CI 0.83, 1.29, P = 0.757), or OM (HR 1.07, 95% CI 0.87, 1.3, P = 0.526). However, patients with severe obesity presented significantly worse outcomes in terms of BCM (HR 1.32, 95% CI 1.01, 1.72, P = 0.043) and OM (HR 1.47, 95% CI 1.16, 1.85, P = 0.001). Differences in recurrence did not attain statistical significance (HR 1.14, 95% CI 0.91, 1.42, P = 0.249) (Table 2 and Figure 1). Initial undertreatment was not related to any of the endpoints of interest, and was not considered in subsequent analyses.

Table 2

Multivariate Cox proportional hazards regression analysis of effect of BMI and each study variable on overall mortality, breast cancer mortality, and recurrence in basic models (adjusted for study and treatment regimen only)

		Overall mortality				Breast cancer mortality				Recurrence
Variable	Number	Events	HR^a	95% CI	P-value	Events	HR	95% CI	P-value	Events	HR	95% CI	P-value
Body mass index, k/m ²
<18.5	66	11	1.08	0.59, 1.98	0.796	9	1.06	0.54, 2.06	0.864	12	0.88	0.49, 1.56	0.650
18.5 to 24.9	2,297	312	1.00			256	1.00			419	1.00
25.0 to 29.9	1,944	265	0.99	0.84, 1.16	0.880	220	1.00	0.83, 1.20	0.984	348	0.95	0.83, 1.10	0.522
30.0 to 34.9	945	139	1.07	0.87, 1.30	0.526	111	1.04	0.83, 1.29	0.757	173	0.98	0.82, 1.17	0.831
≥35.0	431	91	1.47	1.16, 1.85	0.001	68	1.32	1.01, 1.72	0.043	95	1.14	0.91, 1.42	0.249
				P for trend	0.002			P for trend	0.074			P for trend	0.287
Age at diagnosis, years
23 to 44	1,667	276	1.00			245	1.00			416	1.00
45 to 54	2,036	228	0.66	0.55, 0.78	<0.001	187	0.61	0.50, 0.73	<0.001	296	0.54	0.47. 0.63	<0.001
55 to 64	1,443	202	0.92	0.77, 1.11	0.380	156	0.81	0.66, 0.99	0.036	231	0.66	0.56, 0.78	<0.001
65 to 76	537	112	1.41	1.13, 1.76	0.002	76	1.08	0.83, 1.39	0.583	104	0.81	0.65, 1.00	0.049
				P for trend	0.030			P for trend	0.655			P for trend	<0.001
Menopausal status
Postmenopausal	2,661	421	1.00			322	1.00			461	1.00
Premenopausal	3022	397	0.75	0.66, 0.86	<0.001	342	0.85	0.73, 0.98	0.031	586	1.05	0.93, 1.19	0.415
Histology
Ductal	4,809	700	1.00			571	1.00			892	1.00
Lobular	510	66	0.79	0.62, 1.02	0.072	52	0.76	0.57, 1.01	0.062	96	0.92	0.75, 1.14	0.446
Mixed	364	52	0.92	0.69, 1.22	0.561	41	0.89	0.65, 1.22	0.456	59	0.82	0.63, 1.07	0.150
Others	389	66	2.32	1.54, 3.49	<0.001	55	2.92	1.79, 4.75	<0.001	87	2.01	1.44, 2.83	0.000
Histological grade
1	499	35	1.00			23	1.00			55	1.00
2	2,404	277	2.09	1.47, 2.97	<0.001	217	2.51	1.63, 3.87	<0.001	382	1.84	1.39, 2.45	<0.001
3	2,391	440	3.70	2.62, 5.23	<0.001	369	4.77	3.13, 7.28	<0.001	523	2.82	2.13, 3.72	<0.001
Unknown	389	66	2.32	1.54, 3.49	<0.001	55	2.92	1.79, 4.75	<0.001	87	2.01	1.44, 2.83	<0.001
Pathologic primary tumor size
T1	2,794	249	1.00			194	1.00			349	1.00
T2	2,665	510	1.96	1.68, 2.28	<0.001	417	2.03	1.71, 2.41	<0.001	628	1.78	1.57, 2.04	<0.001
T3	224	59	2.14	1.61, 2.84	<0.001	53	2.39	1.76, 3.25	<0.001	70	1.98	1.53, 2.57	<0.001
				P for trend	<0.001			P for trend	<0.001			P for trend	<0.001
Estrogen receptor/progesterone receptor
Both negative	1,502	300	1.00			256	1.00			349	1.00
Any of them positive	4,132	503	0.49	0.43, 0.57	<0.001	394	0.45	0.38, 0.53	<0.001	679	0.59	0.51, 0.67	<0.001
Unknown	49	15	0.77	0.46, 1.31	0.338	14	0.82	0.48, 1.41	0.471	19	1.00	0.63, 1.59	0.998
Human epidermal growth factor-2 status
Negative	4,055	518	1.00			407	1.00			660	1.00
Positive	830	182	1.34	1.13, 1.59	0.001	153	1.42	1.18, 1.71	<0.001	223	1.38	1.18, 1.61	<0.001
Unknown	798	118	1.04	0.85, 1.28	0.690	104	1.17	0.94, 1 · 45	0.172	164	1.14	0.95, 1.36	0.157
Type of surgery
Mastectomy	2,621	512	1.00			420	1.00			633	1.00
Conservative	3,062	306	0.71	0.61, 0.82	<0.001	244	0.71	0.60, 0.83	<0.001	414	0.73	0.65, 0.83	<0.001
Hormonotherapy
No	1,439	314	1.00			263	1.00			354	1.00
Yes	4,045	451	0.42	0.36, 0.48	<0.001	356	0.39	0.33, 0.46	<0.001	622	0.51	0.45, 0.58	<0.001
Unknown	199	53	0.79	0.58, 1.06	0.112	45	0.77	0.56, 1.07	0.120	71	1.05	0.81, 1.37	0.692
Initial undertreatment (first dose <85%)
No	5,532	648	1.00
Yes	151	16	1.01	0.78,1.31	0.932	16	1.06	0.64, 1.75	0.820	20	0.84	0.54, 1.31	0.447
Overall undertreatment (dose <85%)
None	5,083	725	1.00			599	1.00			943	1.00
Epirubicine <85%	78	24	1.55	1.02, 2.36	0.040	20	1.56	0.98, 2.47	0.059	25	1.29	0.86, 1.93	0.226
Cyclophosphamide <85%	296	56	1.28	0.98, 1.69	0.074	41	1.13	0.82, 1.56	0.446	63	1.14	0.88, 1.47	0.323
Fluorouracil <85%	181	33	1.20	0.84, 1.70	0.316	23	1.01	0.66, 1.53	0.977	34	0.98	0.69, 1.38	0.888
Doxorubicin <85%	226	38	1.30	0.93, 1.81	0.119	27	1.12	0.76, 1.65	0.576	42	1.13	0.82, 1.54	0.451
Docetaxel <85%	176	32	1.08	0.74, 1.57	0.696	24	0.96	0.62, 1.47	0.846	39	1.04	0.74, 1.46	0.814
Paclitaxel <85%	244	27	1.43	0.94, 2.18	0.092	16	1.05	0.62, 1.78	0.863	30	1.09	0.74, 1.61	0.662

^aHazard ratio, 95% CI and P-value adjusted for study and treatment regimen.

In fully-adjusted models (Table 3), compared to the reference group (BMI 18.5 to 24.9) obesity remained a non-significant prognostic factor, but severe obesity independently increased the risk of recurrence (HR 1.25, 95% CI 0.99, 1.57, P = 0.052), BCM (HR 1.32, 95% CI 1.00, 1.74, P = 0.053), and OM (HR 1.35, 95% CI 1.06, 1.72, P = 0.016).

Table 3

Summary of multivariate Cox proportional hazards regression analysis of effect of BMI and each study variable on overall mortality, breast cancer mortality, and recurrence in full models

	Overall mortality			Breast cancer mortality			Recurrence
Variable	HR^a	95% CI	P -value	HR	95% CI	P -value	HR	95% CI	P -value
Body mass index, k/m2
<18.5	0.98	0.53, 1.79	0.945	0.95	0.48, 1.85	0.871	0.77	0.43, 1.37	0.377
18.5 to 24.9	1.00			1.00			1.00
25.0 to 29.9	0.95	0.80, 1.12	0.549	1.01	0.84, 1.22	0.905	1.03	0.89, 1.19	0.728
30.0 to 34.9	0.98	0.79, 1.20	0.814	1.02	0.81, 1.29	0.860	1.07	0.89, 1.29	0.460
≥35	1.35	1.06, 1.72	0.016	1.32	1.00, 1.74	0.053	1.25	0.99, 1.57	0.052
Age
Per 5 years	0.92	0.87, 0.97	0.003	0.86	0.81, 0.92	<0.001	0.84	0. 80, 0.89	<0.001
Menopausal status
Postmenopausal	1.00			1.00			1.00
Premenopausal	0.60	0.48, 0.74	<0.001	0.56	0.44, 0.71	<0.001	0.64	0.53, 0.77	<0.001
Pathologic primary tumor size
T1	1.00			1.00			1.00
T2	1.82	1.56, 2.32	<0.001	1.87	1.57, 2.22	<0.001	1.67	1.46, 1.91	<0.001
T3	1.88	1.40, 2.53	<0.001	2.07	1.51, 2.84	<0.001	1.71	1.31, 2.23	<0.001
Histological grade
1	1.00			1.00			1.00
2, 3, or unknown	1.26	1.07, 1.48	0.006	1.32	1.10, 1.58	0.003	1.24	1.07, 1.43	0.004
Type of surgery
Mastectomy	1.00			1.00			1.00
Conservative	0.82	0.70, 0.95	0.008	0.83	0.70, 0.98	0.028	0.84	0.74, 0.96	0.011
Estrogen receptor/progesterone receptor
Both negative	1.00			1.00			1.00
Any positive	0.56	0.48, 0.64	<0.001	0.51	0.44, 0.60	<0.001	0.66	0.57, 0.75	<0.001
Unknown	0.85	0.51, 1.44	0.558	0.89	0.52, 1.54	0.689	1.10	0.69, 1.75	0.699
Human epidermal growth factor-2 status
Negative	1.00			1.00			1.00
Positive	1.19	1.00, 1.42	0.048	1.23	1.01, 1.49	0.037	1.23	1.05, 1.44	0.009
Unknown	1.00	0.82, 1.23	0.965	1.11	0.89, 1.38	0.361	1.09	0.91, 1.30	0.335
Undertreatment
None	1.00			1.00			1.00
Epirubicine <85%	2.36	1.18, 4.72	0.015	3.06	1.47, 6.36	0.003	1.84	0.93, 3.63	0.078
Cyclophosph <85%	0.86	0.35, 2.13	0.74	0.93	0.34, 2.53	0.880	1.31	0.58, 2.95	0.519
Fluorouracil <85%	0.64	0.30, 1.34	0.235	0.45	0.19, 1.07	0.069	0.50	0.26, 0.99	0.046
Doxorubicin <85%	1.86	0.89, 3.88	0.097	1.86	0.82, 4.22	0.134	1.29	0.63, 2.64	0.478
Docetaxel <85%	0.84	0.46, 1.53	0.559	0.70	0.35, 1.40	0.315	0.75	0.44, 1.28	0.294
Paclitaxel <85%	1.37	0.90, 2.09	0.147	1.06	0.62, 1.81	0.824	1.15	0.78, 1.70	0.491

Models were adjusted for all the other variables in the table. ^aHazard ratio, 95% CI and P-value adjusted for study, treatment regimen and the rest of variables in the table.

Figure 2 depicts the fully-adjusted HR dose–response curve (dark line) and upper and lower limits of the CI (lighter lines) for BMI for each of the three endpoints of interest. For OM, the dose–response curve showed higher HRs at both BMI extremes, but the 95% CIs did not include the one only at the right end of the curve, that is, for BMI ≥35. BCM and recurrence results also indicated a positive dose–response relationship, but the trend was not as pronounced and failed to reach statistical significance.

Figure 3 presents the HR and 95% CIs associated with severe obesity (BMI ≥35) for each survival outcome by the categories of each covariate, considering the different pathological BC subtypes. For these analyses, in order to increase our statistical power, BMI <25 was considered the reference category. These HR values were adjusted for the rest of the variables included in the full model. No statistically significant differences in the effect of severe obesity were observed per category of the other explanatory variables, but the effect seemed to be more pronounced in younger women (age <45 years). Furthermore, the magnitude of the negative effect of severe obesity on survival outcomes was similar across the three BC subtypes (ER/PR-positive/HER2-negative, HER2-positive, triple-negative).

Discussion

In this retrospective survival analysis of pooled data from four large, well-conducted, randomized phase III trials of adjuvant CT, severe obesity (BMI ≥35) was significantly associated with worse survival outcomes (OM and BCM) and a higher risk of disease recurrence. Additionally, the magnitude of the negative effect of BMI on survival was similar across pathological subtypes (ER/PR-positive/HER2-negative, HER2-positive, triple-negative). However, obese patients (BMI 30.0 to 34.9) displayed similar prognosis to patients with BMI below 25.0, not unexpected given that most studies of women participating in clinical trials show a relatively modest effect of obesity on prognosis compared with population-based studies. A recent multi-analysis [8] concluded that there was a (non-statistically significant) tendency to report higher prognostic effects of obesity in BC patients in observational studies than in randomized controlled trials (RCTs). In this regard, our study supports the harmful prognostic effect of severe obesity among operable BC patients treated with the most up-to-date CT schedules based on anthracyclines and taxanes.

To the best of our knowledge, this is the largest analysis of RCTs examining obesity as a prognostic factor in operable BC patients treated with anthracyclines and taxanes, and adjusting for hormone receptor and HER2 status. It is also the second study to confine significant prognostic effects to severely obese patients, supporting previous work by Dignam and colleagues [27]. In a study conducted by Berclaz et al., data from 6,792 BC patients randomized in seven trials of the International Breast Cancer Study Group from 1978 to 1993 were analyzed [9]. These trials included observation (no adjuvant therapy), endocrine therapy (tamoxifen), or cyclophosphamide, methotrexate and fluorouracil (CMF)-based CT. Their results showed that BMI independently predicted OM (P = 0.03) but not risk of recurrence (P = 0.12). Azambuja et al. analyzed 2,887 node-positive BC patients included in the BIG 02–98 trial who were treated with a CT regimen based on anthracyclines. In this study, obesity emerged as an independent unfavorable prognostic factor for OM (P = 0.008) and recurrence (P = 0.04) [11]. A retrospective analysis of 4,077 women from the National Surgical Adjuvant Breast and Bowel Project clinical trials with ER-negative, node-negative BC, treated with several CT regimens with or without anthracyclines, showed higher mortality only among severely obese patients but not among obese patients [27]. Also our results are consistent with those obtained by Sparano et al. in the ECOG 1199 study [12] in which there was also a correlation between increased BMI and poorer disease-free survival and overall survival. However, in our study the correlation between BMI >35 and worse prognosis was observed in all pathological subtypes, whereas in the ECOG 1199 this effect seemed to be limited to ER-positive patients. These differences may be due to a different definition of ER-positive status (>10% in ECOG 1199 versus >1% in our studies). Furthermore, the percentage of obese patients was lower in our study (16.6 versus 36.6% respectively) and we did not include black patients. This is relevant because the ECOG 1199 has shown a significant association between black race, increased frequency of obesity and a worse prognosis in ER-positive patients [28].

Certain characteristics of our study may explain the differences between our results and previous work. First, the homogeneity of our sample, which included only patients with low comorbidity, could partially explain the stronger prognostic role of obesity observed in population-based studies than in our study. Such differences in effect may be attributed to other conditions such as diabetes, metabolic syndrome, and other chronic diseases that are associated both with obesity and with poorer prognoses. Because of the criteria used in clinical trials, obese patients with impaired health due to these conditions have a lower probability of being included in a clinical trial. Second, the assessment necessary to establish patient eligibility for a clinical trial may result in more accurate staging and consequently less confounding between obesity and delayed diagnosis often observed in obese women. Third, our results are based on a large sample size of more than 5,600 patients. Pooled analyses have shown that risk estimates based on retrospective analysis of clinical trials often decline as the sample size increases [9‐11]. Finally, all our patients were treated homogeneously with anthracycline-based CT, such an effective treatment that it may have partly counteracted the adverse prognostic effect of obesity when compared to the obesity effect found in population and cohort studies, or even in clinical trials with suboptimal CT schedules like CMF. It should also be anticipated that undertreatment is less frequent when patients are treated within the context of a clinical trial.

In fact, undertreatment may also contribute to poorer survival rates in obese BC patients [22, 29]. Several studies have shown that obese BC patients are more likely to receive reduced doses of CT compared to normal-weight women [22, 29, 30]. Obese patients treated with CMF-based CT were significantly more likely to receive a lower CT dose for the first course (<85% of expected dose) than those with normal or intermediate BMI values (39% versus 16%, P <0.0001) and this undertreatment was associated with a significantly worse outcome for ER-negative patients [27]. However, several studies found that obese women receiving full doses of CT did not experience more toxicity than normal-weight patients [22, 30, 31]. In our study, although undertreatment was generally low, severely obese patients were also more likely to be undertreated, despite the prevalence of serious adverse events being similar to that observed in non-obese patients. Even in the context of a clinical trial, severely obese patients were almost three times more likely to receive suboptimal doses from the start, and this insufficient dose was maintained in subsequent cycles in more than 90% of cases. Oncologists should be aware of the importance of prescribing full weight-based doses in agreement with the recommendations of the American Society of Clinical Oncology [22].

The pathways involved in the relationship between obesity and BC outcomes remain unclear, but obesity is known to affect several hormones and growth factors that are potentially associated with BC [32]. Consequently, obese patients may have elevated tumor cell proliferation and metastasis due to undefined adipokine effects on tumor cells [33]. For instance, hyperinsulinism has been correlated with BMI, recurrence, and BCM, regardless of hormone receptor status [34]. The pro-angiogenic and pro-inflammatory adipokines such as leptin, IL6, TNF-α, and vascular endothelial growth factor (VEGF), secreted by fat tissue, are commonly elevated in obese patients [35, 36]. As BMI is directly related to circulating estrogen levels, the production of estrogens by adipose tissue has also been postulated as a factor in the more biologically aggressive ER-positive tumors in postmenopausal women [37]. Also higher rates of angiolymphatic invasion among obese women with breast cancer may contribute to their poorer outcomes, as described by Gillespie et al. in their retrospective series [38].

Several studies have evaluated the role of obesity as a risk factor for BC development according to different BC subtypes [39‐42]. However, data on the role of obesity on patient prognosis according to these subtypes are scarce. A recent meta-analysis found no evidence of the prognostic role of obesity varying by hormone receptor status [7], although HER2 receptor data were not available until recently. In fact, a study on 4,770 operable BC patients treated with a CT regimen based on anthracyclines and taxanes reported a worse outcome specifically in hormone receptor-positive/HER2-negative disease patients, but not among patients with HER2-positive or triple-negative disease [12]. In contrast, our analyses failed to detect a difference in the observed prognostic role of severe obesity by subtype.

Although the shortcomings of our study are not uncommon in retrospective analyses of clinical trials, our results should be interpreted in the context of the study limitations. BMI was measured only at the beginning of follow up and further changes were not considered, in part due to the difficulty in assessing changes influenced by CT/hormone treatment side effects. For the analysis by tumor subtype, hormone receptor positivity was assessed in each trial under the available criteria at that moment, and the lack of information on HER2 in the GEICAM/9805 trial substantially decreases the statistical power of the analyses. Major strengths of this study include a large sample size (n >5,600), precise BMI information at baseline, and a standardized CT treatment based on the most active drugs in the adjuvant setting available at that time (anthracyclines and taxanes).

In summary, this study shows that obesity (BMI 30.0 to 34.9) is not associated with worse survival outcomes in operable BC patients treated with anthracycline- and taxane-based CT. Severely obese patients (BMI ≥35.0), however, present an increased risk of recurrence, BCM, and OM compared to patients with BMI <25.0. Further, the magnitude of the negative effect of BMI on survival outcomes was similar across pathological BC subtypes.

Conclusions

Based on a large retrospective analysis of four randomized clinical trials of operable BC patients treated with anthracyclines and taxanes, and adjusting for hormone receptor and HER2 status, we found that severe obesity, but not obesity, emerged as a statistically and clinically significant unfavorable prognostic factor regardless of BC subtype. These findings support further basic and clinical research on the mechanisms of the association between severe obesity and survival outcomes in BC patients in order to maximize treatment benefits among these patients.

Acknowledgments

This work was supported by the Spanish Breast Cancer Research Group (Grupo Español de Investigación de Cáncer de Mama) (GEICAM). No funding was received for the data analyses or the writing of this manuscript. Clinical trials GEICAM/9805 and BCIRG 001 were funded by Sanofi Aventis. GEICAM/9906 and GEICAM/2003-02 were partially funded by Bristol-Myers Squibb. These funding bodies were not involved in the collection and interpretation of the data or in the decision to publish. EA and MM were also supported by FEDER (RECTICC-RD12/0036/0076). We thank all the participating patients, clinicians, GEICAM and local research staff. We thank Hosanna Soler Vila, PhD, who provided medical writing services on behalf of GEICAM.

Competing interests

All authors declare that they have no competing interests.

Authors’ contributions

Electronic supplementary material

Additional file 1: List of Institutional Review Boards.(PDF 59 KB)

Additional file 2: Characteristics of women enrolled in the four clinical trials.(PDF 76 KB)

Authors’ original submitted files for images

Below are the links to the authors’ original submitted files for images.

Authors’ original file for figure 1

Authors’ original file for figure 2

Authors’ original file for figure 3

Ferlay J, Shin HR, Bray F, Forman D, Mathers C, Parkin DM: GLOBOCAN 2008 v2.0, cancer incidence and mortality worldwide: iarc cancer base No. 10. Lyon, France: International Agency for Research on Cancer. 2010, [http://globocan.iarc.fr]

Renehan AG, Tyson M, Egger M, Heller RF, Zwahlen M: Body-mass index and incidence of cancer: a systematic review and meta-analysis of prospective observational studies. Lancet. 2008, 371: 569-578. 10.1016/S0140-6736(08)60269-X.CrossRefPubMed

Kelly T, Yang W, Chen CS, Reynolds K, He J: Global burden of obesity in 2005 and projections to 2030. Int J Obes (Lond). 2008, 32: 1431-1437. 10.1038/ijo.2008.102.CrossRef

Ewertz M, Jensen MB, Gunnarsdottir KA, Højris I, Jakobsen EH, Nielsen D, Stenbygaard LE, Tange UB, Cold S: Effect of obesity on prognosis after early-stage breast cancer. J Clin Oncol. 2011, 29: 25-31. 10.1200/JCO.2010.29.7614.CrossRefPubMed

Majed B, Moreau T, Senouci K, Salmon RJ, Fourquet A, Asselain B: Is obesity an independent prognosis factor in woman breast cancer?. Breast Cancer Res Treat. 2008, 111: 329-342. 10.1007/s10549-007-9785-3.CrossRefPubMed

IOM (Institute of Medicine): The role of obesity in cancer survival and recurrence: Workshop summary. 2012, Washington, DC: The National Academies Press

Niraula S, Ocana A, Ennis M, Goodwin PJ: Body size and breast cancer prognosis in relation to hormone receptor and menopausal status: a meta-analysis. Breast Cancer Res Treat. 2012, 134: 769-781. 10.1007/s10549-012-2073-x.CrossRefPubMed

Protani M, Coory M, Martin JH: Effect of obesity on survival of women with breast cancer: systematic review and meta-analysis. Breast Cancer Res Treat. 2010, 123: 627-635. 10.1007/s10549-010-0990-0.CrossRefPubMed

Berclaz G, Li S, Price KN, Coates AS, Castiglione-Gertsch M, Rudenstam CM, Holmberg SB, Lindtner J, Erien D, Collins J, Snyder R, Thürlimann B, Fey MF, Mendiola C, Werner ID, Simoncini E, Crivellari D, Gelber RD, Goldhirsch A: International breast cancer study group: body mass index as a prognostic feature in operable breast cancer: the International breast cancer study group experience. Ann Oncol. 2004, 15: 875-884. 10.1093/annonc/mdh222.CrossRefPubMed

10.

Dignam JJ, Wieand K, Johnson KA, Fisher B, Xu L, Mamounas EP: Obesity, tamoxifen use, and outcomes in women with estrogen receptor-positive early-stage breast cancer. J Natl Cancer Inst. 2003, 95: 1467-1476. 10.1093/jnci/djg060.CrossRefPubMedPubMedCentral

11.

de Azambuja E, McCaskill-Stevens W, Francis P, Quinaux E, Crown JP, Vicente M, Giuliani R, Nordenskjöld B, Gutiérez J, Andersson M, Vila MM, Jakesz R, Demol J, Dewar J, Santoro A, Lluch A, Olsen S, Gelber RD, Di Leo A, Piccart-Gebhart M: The effect of body mass index on overall and disease-free survival in node-positive breast cancer patients treated with docetaxel and doxorubicin-containing adjuvant chemotherapy: the experience of the BIG 02–98 trial. Breast Cancer Res Treat. 2010, 119: 145-153. 10.1007/s10549-009-0512-0.CrossRefPubMed

12.

Sparano JA, Wang M, Zhao F, Stearns V, Martino S, Ligibel JA, Perez EA, Saphner T, Wolff AC, Sledge GW, Wood WC, Fetting J, Davidson NE: Obesity at diagnosis is associated with inferior outcomes in hormone receptor-positive operable breast cancer. Cancer. 2012, 118: 5937-5946. 10.1002/cncr.27527.CrossRefPubMedPubMedCentral

13.

Sestak I, Distler W, Forbes JF, Dowsett M, Howell A, Cuzick J: Effect of body mass index on recurrences in tamoxifen and anastrozole treated women: an exploratory analysis from the ATAC trial. J Clin Oncol. 2010, 28: 3411-3415. 10.1200/JCO.2009.27.2021.CrossRefPubMed

14.

Ewertz M, Gray KP, Regan MM, Ejlertsen B, Price KN, Thürlimann B, Bonnefoi H, Forbes JF, Paridaens RJ, Rabaglio M, Gelber RD, Colleoni M, Láng I, Smith IE, Coates AS, Goldhirsch A, Mouridsen HT: Obesity and risk of recurrence or death after adjuvant endocrine therapy with letrozole or tamoxifen in the breast international group 1–98 trial. J Clin Oncol. 2012, 30: 3967-3975. 10.1200/JCO.2011.40.8666.CrossRefPubMedPubMedCentral

15.

Pfeiler G, Königsberg R, Fesl C, Mlineritsch B, Stoeger H, Singer CF, Pöstlberger S, Steger GG, Seifert M, Dubsky P, Taucher S, Samonigg H, Bjelic-Radisic V, Greil R, Marth C, Gnant M: Impact of body mass index on the efficacy of endocrine therapy in premenopausal patients with breast cancer: an analysis of the prospective ABCSG-12 trial. J Clin Oncol. 2011, 29: 2653-2659. 10.1200/JCO.2010.33.2585.CrossRefPubMed

16.

Martin M, Rodriguez-Lescure A, Ruiz A, Alba E, Calvo L, Ruiz-Borrego M, Munárriz B, Rodríguez CA, Crespo C, de Alava E, López García-Asenjo JA, Guitián MD, Almenar S, González-Palacios JF, Vera F, Palacios J, Ramos M, Gracia Marco JM, Lluch A, Alvarez I, Seguí MA, Mayordomo JI, Antón A, Baena JM, Plazaola A, Modolell A, Pelegrí A, Mel JR, Aranda E, Adrover E, GEICAM 9906 Study Investigators, et al: Randomized phase 3 trial of fluorouracil, epirubicin, and cyclophosphamide alone or followed by Paclitaxel for early breast cancer. J Natl Cancer Inst. 2008, 100: 805-814. 10.1093/jnci/djn151.CrossRefPubMed

17.

Martin M, Segui MA, Anton A, Ruiz A, Ramos M, Adrover E, Aranda I, Rodríguez-Lescure A, Grosse R, Calvo L, Barnadas A, Isla D, Martinez Del Prado P, Ruiz-Borrego M, Zaluski J, Arcusa A, Muñoz M, López Vega JM, Mel JR, Munarriz B, Llorca C, Jara C, Alba E, Florián J, Li J, López García-Asenjo JA, Sáez A, Rios MJ, Almenar S, Peiró G, GEICAM 9805 Investigators, et al: Adjuvant docetaxel for high-risk, node-negative breast cancer. N Engl J Med. 2010, 363: 2200-2210. 10.1056/NEJMoa0910320.CrossRefPubMed

18.

Martin M, Pienkowski T, Mackey J, Pawlicki M, Guastalla JP, Weaver C, Tomiak E, Al-Tweigeri T, Chap L, Juhos E, Guevin R, Howell A, Fornander T, Hainsworth J, Coleman R, Vinholes J, Modiano M, Pinter T, Tang SC, Colwell B, Prady C, Provencher L, Walde D, Rodriguez-Lescure A, Hugh J, Loret C, Rupin M, Blitz S, Jacobs P, Murawsky M, Breast Cancer International Research Group 001 Investigators, et al: Adjuvant docetaxel for node-positive breast cancer. N Engl J Med. 2005, 352: 2302-2313. 10.1056/NEJMoa043681.CrossRefPubMed

19.

Mackey JR, Martin M, Pienkowski T, Rolski J, Guastalla JP, Sami A, Glaspy J, Juhos E, Wardley A, Fornander T, Hainsworth J, Coleman R, Modiano MR, Vinholes J, Pinter T, Rodríguez-Lescure A, Colwell B, Whitlock P, Provencher L, Laing K, Walde D, Price C, Hugh JC, Childs BH, Bassi K, Lindsay MA, Wilson V, Rupin M, Houé V, Vogel C, TRIO/BCIRG 001 investigators: Adjuvant docetaxel, doxorubicin, and cyclophosphamide in node-positive breast cancer: 10-year follow-up of the phase 3 randomised BCIRG 001 trial. Lancet Oncol. 2013, 14: 72-80. 10.1016/S1470-2045(12)70525-9.CrossRefPubMed

20.

Martín M, Ruiz A, Borrego MR, Barnadas A, González S, Calvo L, Vila MM, Antón A, Rodríguez-Lescure A, Seguí-Palmer MA, Muñoz-Mateu M, Ribugent JD, López-Vega JM, Jara C, Espinosa E, Fernández CM, Andrés R, Ribelles N, Plazaola A, Sánchez-Rovira P, Bofill JS, Crespo C, Carabantes FJ, Servitja S, Chacón JI, Rodríguez CA, Hernando B, Alvarez I, Carrasco E, Lluch A: Fluorouracil, doxorubicin, and cyclophosphamide (FAC) versus FAC Followed by weekly paclitaxel as adjuvant therapy for high-risk, node-negative breast cancer: results from the GEICAM/2003-02 study. J Clin Oncol. 2013, 31: 2593-2599. 10.1200/JCO.2012.46.9841.CrossRefPubMed

21.

World Health Organization: Global database on body mass index. BMI Classification. Table 1: The International Classification of adult underweight, overweight and obesity according to BMI. 2013, http://apps.who.int/bmi/index.jsp?introPage=intro_3.html. Access on 17^th February

22.

Griggs JJ, Mangu PB, Anderson H, Balaban EP, Dignam JJ, Hryniuk WM, Morrison VA, Pini TM, Runowicz CD, Rosner GL, Shayne M, Sparreboom A, Sucheston LE, Lyman GH, American Society of Clinical Oncology: Appropriate chemotherapy dosing for obese adult patients with cancer: American Society of Clinical Oncology clinical practice guideline. J Clin Oncol. 2012, 30: 1553-1561. 10.1200/JCO.2011.39.9436.CrossRefPubMed

23.

Bonadonna G, Valagussa P: Dose–response effect of adjuvant chemotherapy in breast cancer. N Engl J Med. 1981, 304: 10-15. 10.1056/NEJM198101013040103.CrossRefPubMed

24.

Arbuck SG IP, Setser A: Common toxicity criteria (CTC) version 2.0: highlights and tools.Annals of Oncology. 1998, 9: 12-12.CrossRef

25.

Cox DR: Regression models and life-tables (with discussion). J Royal Stat Sc B. 1972, 34: 187-220.

26.

Harrell FJ: General aspects of fitting regression models. Relaxing linearity assumption for continuous predictors. Regression Modeling Strategies with Applications to Linear Models, Logistic Regression, and Survival Analysis. 2001, New York: Springer, 16-26.

27.

Dignam JJ, Wieand K, Johnson KA, Raich P, Anderson SJ, Somkin C, Wickerham DL: Effects of obesity and race on prognosis in lymph node-negative, estrogen receptor-negative breast cancer. Breast Cancer Res Treat. 2006, 97: 245-254. 10.1007/s10549-005-9118-3.CrossRefPubMed

28.

Sparano JA, Wang M, Zhao F, Stearns V, Martino S, Ligibel JA, Perez EA, Saphner T, Wolff AC, Sledge GW, Wood WC, Davidson NE: Race and hormone receptor-positive breast cancer outcomes in a randomized chemotherapy trial. J Natl Cancer Inst. 2012, 104: 406-414. 10.1093/jnci/djr543.CrossRefPubMedPubMedCentral

29.

Colleoni M, Li S, Gelber RD, Price KN, Coates AS, Castiglione-Gertsch M, Goldhirsch A, International Breast Cancer Study Group: Relation between chemotherapy dose, oestrogen receptor expression, and body-mass index. Lancet. 2005, 366: 1108-1110. 10.1016/S0140-6736(05)67110-3.CrossRefPubMed

30.

Hunter RJ, Navo MA, Thaker PH, Bodurka DC, Wolf JK, Smith JA: Dosing chemotherapy in obese patients: actual versus assigned body surface area (BSA). Cancer Treat Rev. 2009, 35: 69-78. 10.1016/j.ctrv.2008.07.005.CrossRefPubMed

31.

Rosner GL, Hargis JB, Hollis DR, Rosner GL, Hargis JB, Hollis DR, Budman DR, Weiss RB, Henderson IC, Schilsky RL: Relationship between toxicity and obesity in women receiving adjuvant chemotherapy for breast cancer: results from cancer and leukemia group B study 8541. J Clin Oncol. 1996, 14: 3000-3008.PubMed

32.

Calle EE, Kaaks R: Overweight, obesity and cancer: epidemiological evidence and proposed mechanisms. Nat Rev Cancer. 2004, 4: 579-591. 10.1038/nrc1408.CrossRefPubMed

33.

Daling JR, Malone KE, Doody DR, Johnson LG, Gralow JR, Porter PL: Relation of body mass index to tumor markers and survival among young women with invasive ductal breast carcinoma. Cancer. 2001, 92: 720-729. 10.1002/1097-0142(20010815)92:4<720::AID-CNCR1375>3.0.CO;2-T.CrossRefPubMed

34.

Goodwin PJ, Ennis M, Pritchard KI, Trudeau ME, Koo J, Madarnas Y, Hartwick W, Hoffman B, Hood N: Fasting insulin and outcome in early-stage breast cancer: results of a prospective cohort study. J Clin Oncol. 2002, 20: 42-51. 10.1200/JCO.20.1.42.CrossRefPubMed

35.

Catalano S, Marsico S, Giordano C, Mauro L, Rizza P, Panno ML, Andò S: Leptin enhances, via AP-1, expression of aromatase in the MCF-7 cell line. J Biol Chem. 2003, 278: 28668-28676. 10.1074/jbc.M301695200.CrossRefPubMed

36.

Rose DP, Komninou D, Stephenson GD: Obesity, adipocytokines, and insulin resistance in breast cancer. Obes Rev. 2004, 5: 153-165. 10.1111/j.1467-789X.2004.00142.x.CrossRefPubMed

37.

McTiernan A, Rajan KB, Tworoger SS, Irwin M, Bernstein L, Baumgartner R, Gilliland F, Stanczyk FZ, Yasui Y, Ballard-Barbash R: Adiposity and sex hormones in postmenopausal breast cancer survivors. J Clin Oncol. 2003, 21: 1961-1966. 10.1200/JCO.2003.07.057.CrossRefPubMedPubMedCentral

38.

Gillespie EF, Sorbero ME, Hanauer DA, Sabel MS, Herrmann EJ, Weiser LJ, Jagielski CH, Griggs JJ: Obesity and angiolymphatic invasion in primary breast cancer. Ann Surg Oncol. 2010, 17: 752-759. 10.1245/s10434-009-0797-6.CrossRefPubMed

39.

Beral V: Breast cancer and hormone-replacement therapy in the Million Women Study. Lancet. 2003, 362: 419-427.CrossRefPubMed

40.

Chlebowski RT, Hendrix SL, Langer RD, Stefanick ML, Gass M, Lane D, Rodabough RJ, Gilligan MA, Cyr MG, Thomson CA, Khandekar J, Petrovitch H, McTiernan A, WHI Investigators: Influence of estrogen plus progestin on breast cancer and mammography in healthy postmenopausal women: the women’s health initiative randomized trial. JAMA. 2003, 289: 3243-3253. 10.1001/jama.289.24.3243.CrossRefPubMed

41.

Kwan ML, Kushi LH, Weltzien E, Maring B, Kutner SE, Fulton RS, Lee MM, Ambrosone CB, Caan BJ: Epidemiology of breast cancer subtypes in two prospective cohort studies of breast cancer survivors. Breast Cancer Res. 2009, 11: R31-10.1186/bcr2261.CrossRefPubMedPubMedCentral

42.

Millikan RC, Newman B, Tse CK, Moorman PG, Conway K, Dressler LG, Smith LV, Labbok MH, Geradts J, Bensen JT, Jackson S, Nyante S, Livasy C, Carey L, Earp HS, Perou CM: Epidemiology of basal-like breast cancer. Breast Cancer Res Treat. 2008, 109: 123-139. 10.1007/s10549-007-9632-6.CrossRefPubMed

Titel: Obesity and survival in operable breast cancer patients treated with adjuvant anthracyclines and taxanes according to pathological subtypes: a pooled analysis
verfasst von: Bella Pajares
Marina Pollán
Miguel Martín
John R Mackey
Ana Lluch
Joaquín Gavila
Charles Vogel
Manuel Ruiz-Borrego
Lourdes Calvo
Tadeusz Pienkowski
Álvaro Rodríguez-Lescure
Miguel Angel Seguí
Olivier Tredan
Antonio Antón
Manuel Ramos
María del Carmen Cámara
César Rodríguez-Martín
Eva Carrasco
Emilio Alba
Publikationsdatum: 01.12.2013
Verlag: BioMed Central
Erschienen in: Breast Cancer Research / Ausgabe 6/2013
Elektronische ISSN: 1465-542X
DOI: https://doi.org/10.1186/bcr3572

Neu im Fachgebiet Onkologie

Umsetzung der POMGAT-Leitlinie läuft

03.05.2024 DCK 2024 Kongressbericht

Seit November 2023 gibt es evidenzbasierte Empfehlungen zum perioperativen Management bei gastrointestinalen Tumoren (POMGAT) auf S3-Niveau. Vieles wird schon entsprechend der Empfehlungen durchgeführt. Wo es im Alltag noch hapert, zeigt eine Umfrage in einem Klinikverbund.

Springer Medizin

Obesity and survival in operable breast cancer patients treated with adjuvant anthracyclines and taxanes according to pathological subtypes: a pooled analysis