Introduction

The primary hypothesized mechanisms underlying the associations between physical activity and reduced breast cancer include reductions in adiposity, sex hormone levels, insulin resistance and chronic inflammation [1]. These pathways only explain some portion of the association and additional mechanisms require identification and further investigation.

Prolactin is a luteotropic peptide hormone involved in regular lactation which is produced by the anterior pituitary gland. Increased circulating levels of prolactin have been associated with increased risk of both in situ and invasive breast cancer [2]. Two previous exercise intervention trials in post-menopausal women did not observe changes in prolactin levels in response to moderate physical activity [3, 4] compared to controls. As part of the Breast cancer and Exercise Trial in Alberta (BETA) we investigated: 1) the effects of increased levels of moderate to vigorous physical activity (MVPA) on levels of prolactin and 2) whether a higher level of activity led to larger changes in prolactin levels.

Materials and methods

The design of the BETA study has been previously described in detail [5]. Briefly, 400 previously inactive but otherwise healthy postmenopausal women of age were randomized to 150 (MODERATE) or 300 (HIGH) minutes per week of aerobic physical activity for a year-long intervention. Women were eligible for randomization if they were between 50–74 years of age, with no previous diagnosis of invasive cancer, no major comorbidities, obtained physical approval for participation, had a body mass index of 22–40, were moderately sedentary, not a current smoker or excessive drinker, not currently on a weight loss program, English speaking and not planning to be out of the study site areas for more than 4 consecutive weeks during the subsequent 18 months. Both intervention arms were prescribed the same frequency (five days/week) and intensity (moderate-to-vigorous) of aerobic exercise. The training targets were 60 minutes/session (300 total minutes/week) for the HIGH group, and 30 minutes/session (150 total minutes/week) for the MODERATE group. Wrist-worn heart rate were given to each participant and used to ensure a 65–75% maximum heart rate reserve (HRR) was being achieved during each exercise session. A ramp-up period was included where the intensity, frequency and duration of exercise were gradually increased during the first three months of the intervention until the target exercise prescriptions were attained. Fasting blood samples were collected from all participants at baseline, 6 and 12 months following a 24 h abstinence from alcohol intake and exercise and at least 10 h after their last meal. Prolactin levels in plasma were measured with a custom-plex multiplex assay (Eve Technologies, Calgary, AB, Canada), using the Bio-Plex™ 200 system (Bio-Rad Laboratories, Inc., Hercules, CA, USA). The assay sensitivity for prolactin was 30.2 pg/ml and the inter-assay coefficient of variation was 5.5%. Samples for each participant at different time points were all analyzed in the same batch and each batch included an equal number of MODERATE and HIGH blood samples.

Predicted VO2 max was estimated from a modified Balke treadmill test [6] using the multistage model and the American College of Sports Medicine metabolic equations for estimating maximum oxygen consumption [7]. Body composition was estimated from full body dual energy X-ray absorptiometry (DXA) scans to assess overall percent body fat and total fat mass. Computed tomography (CT) scans were taken at the level of the umbilicus to measure subcutaneous and intra-abdominal adiposity.

We considered the comparison of means of 12-month outcomes (log transformed, with no adjustment for baseline values) for the prolactin outcomes. Standard deviation was estimated from previous reports [8]. A sample size of 200 participants per group provided 90% power to detect anticipated changes of 4% between the treatment groups at α = 0.05. Prolactin changes in the two arms were compared in both intention-to-treat and per-protocol analysis using linear mixed models as previously described, adjusting for baseline prolactin levels [9]. A per-protocol analysis was conducted on participants achieving ≥60% of prescribed exercise duration in their target heart rate zone. To investigate whether the effects of exercise were restricted to particular subgroups, stratified analyses were conducted on a priori variables including baseline body mass index (BMI (weight (kg)/height (m2)), estimated physical fitness (VO2max), and total percent body fat.

The study protocol was approved by the Alberta Cancer Research Ethics Committee and the Conjoint Health Research Ethics Board of the University of Calgary and the Health Research Ethics Board of the University of Alberta. All participants provided written informed consent.

Results

The distribution of the study participants’ baseline characteristics was similar in the two trial arms with no meaningful differences between arms [9]. Baseline prolactin levels were 10565 (SD = 6963) pg/ml in MODERATE group and 10478 (SD = 5150) pg/ml in HIGH group (p = 0.89). Overall, we did not observe statistically significant effects for increasing quartiles of physical activity and change in level of prolactin in the n = 384 women included in the analyses (non-randomized analysis – results not shown).

No statistically significant differences were observed in the treatment effect ratios of the two exercise groups in either intention-to-treat (TER 1.00, 95% CI 0.95 – 1.06) or per-protocol analyses (TER 1.02, 95% CI 0.93 – 1.13; Table 1). A per-protocol analysis examining the role of exercise intensity (< or ≥60% of prescribed exercise) also showed no change in prolactin levels between the two groups (Table 1). In stratified analyses by estimated physical fitness (VO2max) and total body fat, no treatment effect ratios in any of the subgroups were significantly different from 1.0 (Table 2).

Table 1 Intention-to-treat and per-protocol analyses of prolactin concentrations between high and moderate volume exercise groups in BETA, (n = 386)
Table 2 Stratified analyses of changes in prolactin between high volume and moderate volume exercise groups in BETA, 2010–2013 (n = 386)

Discussion

Overall, a higher volume of exercise compared to a standard volume did not reduce prolactin levels in BETA. Moreover, the effects did not vary according to exercise adherence or baseline fitness levels, BMI, and total body fat.

This exercise intervention trial is the first study to examine the effects of a high versus moderate volume of MVPA aerobic exercise on prolactin levels in postmenopausal women. Previous studies comparing 12 months of moderate-intensity aerobic exercise to no exercise have reported null effects on prolactin levels [3, 4]. Similarly, the results from these previous trials remained unchanged when exercise adherence, measured as minutes of exercise per day, was considered [3, 4]. In the study by Reding et al. [4], baseline BMI did not alter the treatment effect. In the study by Tworoger et al. [3], change in percent body fat did not mediate the intervention effect however, women in the exercise group who increased their VO2 max by >5% had a statistically significant reduction in prolactin levels.

Our analyses were motivated by the strong animal and in vitro data supporting an important role of prolactin in breast carcinogenesis [10] and epidemiologic data suggesting an association of increased levels with breast cancer risk [11]. While our study did not observe significant impacts of exercise on levels of prolactin, it is worth noting that there are complex relationships between exercise and prolactin levels which may explain our null findings. For example, threshold effects of exercise intensity have been observed in the literature [12], which suggests that the intensity of exercise in the BETA trial may not have been high enough despite a target >65% HRR. Furthermore, effects may differ by age as there are several studies among young athletic populations where increased levels of prolactin are reported post-acute bouts of exercise [12,13,14], while effects among older sedentary populations are less well characterized.

In conclusion, the results from the BETA study suggest that 300 min per week of moderate-intensity aerobic exercise does not reduce prolactin levels more than 150 min per week in a year-long intervention in postmenopausal women. It is unlikely that changes in prolactin levels mediate the reduced risk of breast cancer development in post-menopausal women associated with increased physical activity at any level.