Introduction
During decades of successful adjuvant radiotherapy for breast cancer, reduction of acute and late side effects such as skin reactions and pneumonitis has been an important topic of research, aiming at a continuous improvement of the therapeutic ratio [1, 2]. More recently, health-related quality of life (QoL) and patient-reported outcomes (PROs) have been evaluated as well, because physician-scored side effects are unable to mirror the complex patient experience during a typically multimodal sequence of different treatments [3]. Preceding treatment such as neoadjuvant drugs and definitive surgery (breast-conserving or mastectomy with different approaches regarding axillary lymph nodes) may cause symptoms that are still present when patients move forward to the adjuvant phase, where new drugs and/or radiotherapy can impact QoL and PROs [4]. A wide range of symptoms including but not limited to pain, fatigue, anxiety, and sleep disturbance are reported by many patients before they start with adjuvant radiotherapy.
Many different instruments have been used to evaluate QoL and PROs [5]. Currently, mobile apps and other digital solutions are gaining increasing importance [6, 7]. The Edmonton Symptom Assessment System (ESAS), originally developed in the palliative care setting [8], has occasionally been employed in curatively treated patients with breast cancer [9‐14]. ESAS is a short, one-sheet questionnaire addressing major symptoms and wellbeing on a numeric scale of 0–10, which can easily be integrated into routine workflow in radiation oncology departments [15]. The radiotherapy facility at Nordland Hospital started screening of all palliatively irradiated patients with the ESAS tool in 2012, following the routine procedure that already had been in place for outpatients receiving systemic anticancer therapy for several years. From 2016, patients seen for treatment planning of adjuvant radiotherapy for breast cancer also were asked to provide a symptom assessment, which may facilitate initiation of measures that contribute to better symptom control. Given that patients with more advanced disease who received more intense preceding treatment may be more likely to experience toxicity and related symptoms, we limited this initial study of ESAS data in our institution’s breast cancer patients to those referred to locoregional radiotherapy. Potential correlations between patient-related parameters, e.g., age or body mass index (BMI), comorbidity, disease-related parameters, and treatment parameters on one hand and pre-radiotherapy symptom severity on the other were assessed.
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Materials and methods
We performed a retrospective analysis of 132 unselected, consecutive female patients who started locoregional adjuvant radiotherapy at our hospital during the time period 2016–2021. Radiotherapy was administered after 3D planning, mostly with daily 2‑Gy fractions with or without sequential boost in deep-inspiration breath-hold. Hybrid intensity-modulated techniques were employed on an individual basis. The same was true for hypofractionation (15 fractions of 2.67 Gy), e.g., in elderly patients. The ESAS tool was administered by a registered oncology nurse immediately before radiation oncologist consultation and computed tomography imaging for treatment planning approximately 1 week before radiotherapy. All medical records were available in the hospital’s electronic patient record (EPR) system. Statistical analysis was performed with IBM SPSS Statistics 29 (IBM Corp., Armonk, NY, USA). In addition to relevant ESAS items of interest (continuous variables expressed as mean with standard deviations [SD]), we analyzed a large number of categorical baseline variables (dichotomized present/absent or categorized by quartiles or treatment groups). Analysis of variance (ANOVA) tables were employed for inter-group comparisons. A p-value ≤ 0.05 was considered statistically significant.
Results
The mean age was 59 years (SD 13), range 24–88 years. The mean BMI was 27.7 kgm-2 (SD 5), range 18–45 kgm-2. Most patients had pT1 or 2 node-positive (N1) disease. Table 1 shows additional baseline characteristics and Table 2 shows the ESAS data. The biggest patient-reported issues were fatigue, pain (while moving), and sleep problems. To reduce the likelihood of spurious findings from multiple testing, several items (appetite, nausea, constipation, dyspnea, dry mouth) were not carried forward to further individual analyses, unless special subgroups of interest appeared in the first round where all items were employed to create the point sum. In addition, the patient-reported item “overall wellbeing” possibly integrates all the different aspects, and was analyzed as a secondary outcome of interest.
Table 1
Baseline characteristics before adjuvant radiotherapy in 132 female patients
Variable | N | % |
|---|---|---|
Screening detected | 28 | 21 |
Pathological stage | ||
pT0 | 19 | 14 |
pT1 | 53 | 40 |
pT2 | 49 | 37 |
pT3 | 5 | 4 |
pT4 | 6 | 5 |
pN0 | 34 | 26 |
pN1 | 71 | 54 |
pN2 | 17 | 13 |
pN3 | 2 | 2 |
Microscopic nodal disease only | 8 | 6 |
Histology | ||
Ductal carcinoma | 113 | 86 |
Lobular carcinoma | 12 | 9 |
Both | 2 | 2 |
Others | 5 | 4 |
Histological grade | ||
G1 | 24 | 18 |
G2 | 57 | 43 |
G3 | 29 | 22 |
Uncertain after NATxa | 22 | 17 |
Receptor status | ||
Estrogen negative | 32 | 24 |
Progesterone negative | 54 | 41 |
Triple negative | 17 | 13 |
Her2 positive | 26 | 20 |
Others | ||
BRCA mutation | 4 | 3 |
Premenopausalb | 26 | 20 |
Perimenopausal | 13 | 10 |
Postmenopausal | 90 | 68 |
Diabetes mellitus | 8 | 6 |
Autoimmune disease | 15 | 11 |
Active smokerb | 12 | 9 |
Treatment | ||
Neoadjuvant systemic therapy | 65 | 49 |
Mastectomy | 75 | 57 |
Breast conservation | 57 | 43 |
Re-excision (second breast surgery) | 11 | 8 |
Axillary dissection | 69 | 52 |
Sentinel node biopsy | 63 | 48 |
Hypofractionated radiotherapy | 9 | 7 |
Tumor bed boost | 20 | 15 |
Adjuvant systemic therapy | 126 | 95 |
Table 2
Edmonton Symptom Assessment System (ESAS) before adjuvant radiotherapy in 132 female patients
Item | Median | Mean | Range |
|---|---|---|---|
Pain (not moving) | 0 | 1.65 | 0–9 |
Pain (while moving) | 2 | 2.38 | 0–10 |
Fatigue | 3 | 2.95 | 0–10 |
Nausea | 0 | 0.53 | 0–8 |
Dyspnea | 0 | 1.14 | 0–10 |
Dry mouth | 1 | 2.52 | 0–10 |
Appetite | 0 | 1.43 | 0–8 |
Constipation | 0 | 0.96 | 0–10 |
Anxiety/restlessness | 1 | 1.67 | 0–10 |
Sleep | 2 | 2.65 | 0–10 |
Sadness/depression | 0 | 1.36 | 0–10 |
Overall wellbeing | 2 | 2.35 | 0–10 |
Point sum | 19.5 | 21.50 | 0–86 |
All the different parameters displayed in Table 1 were analyzed for correlations with the ESAS point sum. Only two significant correlations were identified: patients with triple-negative breast cancer reported a higher symptom burden (mean 30 versus 20, p = 0.038). Patients assigned to adjuvant endocrine therapy (n = 72), which had typically not yet been started at the time of ESAS scoring, had the lowest point sum (mean 18), followed by those on Her-2-targeting agents without chemotherapy (n = 14, mean 19), those on chemotherapy with or without other drugs (n = 40, mean 26), and those without systemic therapy (n = 5, mean 41), p = 0.007. It should be noted that patients without adjuvant systemic therapy had triple-negative breast cancer. However, some patients with triple-negative disease received adjuvant chemotherapy.
The fact that patients with triple-negative disease had higher mean point sums resulted from three individual items: fatigue (mean 4.1 versus 2.8, p = 0.05), pain (not moving; mean 3.1 versus 1.4, p = 0.002), and pain (while moving; mean 4.1 versus 2.1, p = 0.004). Regarding adjuvant systemic therapy, the same three ESAS items were the main drivers of higher symptom burden. Mean fatigue scores were 2.2 (endocrine), 3.6 (chemotherapy), 4.0 (Her-2), and 6.0 (no adjuvant drugs), p < 0.001. Mean pain scores (not moving) were 1.2 (endocrine), 2.1 (chemotherapy), 2.0 (Her-2), and 4.4 (no adjuvant drugs), p = 0.003. The corresponding figures for pain in activity were 2.2 (endocrine), 3.6 (chemotherapy), 2.7 (Her-2), and 6.8 (no adjuvant drugs), p < 0.001.
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Additional differences were observed regarding dry mouth (mean 2.0 after adjuvant chemotherapy, 3.5 in the Her‑2 group, and 2.5 in both other groups, p = 0.045). Patients not receiving adjuvant systemic therapy had reduced appetite (mean 2.8 versus 1–2 in all other groups, p = 0.08).
After the primary analysis of the ESAS point sum, a second analysis was run with overall wellbeing as the endpoint, without identifying any significant correlations (all p-values > 0.1).
Finally, we were interested in the prognostically favorable group with stage ypT0, i.e., pathologic complete response at surgery due to neoadjuvant treatment. These patients had significantly lower mean anxiety scores (0.7 versus 1.8, p = 0.03) and a trend towards lower depression scores (mean 0.6 versus 1.5, p = 0.09) compared to all other patients (T1–4 with or without neoadjuvant treatment; n = 19 versus 113).
Discussion
The present study addressed patient-reported symptoms in an unselected real-world cohort, which included patients with different disease characteristics and treatment pathways. At the time of treatment planning, 132 patients scored their symptoms with the ESAS tool. Canadian researchers have also published several studies on ESAS and curative breast cancer treatment. Chow et al. reported no statistical difference in ESAS scores for mastectomy and lumpectomy patients [9], a finding confirmed in our study. Neither re-resection nor the extent of surgical axillary treatment were associated with ESAS scores in the present cohort. Barbera et al. evaluated the impact of screening with ESAS on emergency department (ED) visit rates in women with breast cancer receiving adjuvant chemotherapy [10]. Interestingly, screening with ESAS was associated with decreased ED visits. Chow et al. performed a longitudinal radiotherapy study including both ESAS and QoL [11]. Of the ESAS symptoms identified as significant predictors of QoL, pain, fatigue, and anxiety correlated with overall wellbeing at all timepoints. Given that such data provide reasons to believe that overall wellbeing to some degree integrates many of the individual items, our own data failed to show that overall wellbeing is of major importance as a global symptom burden criterion. We would rather advocate for employment of the ESAS point sum when researchers try to summarize the symptom burden. While the latter may facilitate statistical comparisons, clinicians need to look at the complete picture, trying to identify the individual problems of each patient in order to increase care-associated satisfaction [16].
At our department, ESAS assessment during radiotherapy and follow-up has not been performed. Lam et al. reported longitudinal data showing that patient-reported pain associated with breast irradiation peaked 1 week after treatment completion [12]. Younger patients (40–49 or 50–59 years of age) reported significantly more overall pain and breast pain compared with patients ≥ 60 years of age. Our own study did not specifically address different locations of pain, but rather collected overall pain data only. In principle, the latter may be influenced by comorbidities and age as well as medications. It should also be noticed that the Canadian studies were larger than the present one. Behroozian et al. compared breast cancer patients with and without regional nodal irradiation and included 781 patients in the longitudinal analysis [13]. Baseline symptom reporting was similar between cohorts. Across all timepoints, differences in outcomes between cohorts were minimal, except for lack of appetite (p = 0.03), which was significantly aggravated in patients treated with regional nodal irradiation.
A major finding from the present study was the impact of adjuvant systemic treatment, which is connected to tumor type, because specific drugs are restricted to patients with Her-2-positive disease, while triple-negative histology restricts adjuvant options in a broader sense, especially in the earlier years of this study before capecitabine was introduced. Akkila et al. studied patients treated between February 2018 and September 2020 [14]. They compared baseline scores between adjuvant and neoadjuvant chemotherapy patients (n = 338). Comparison of baseline ESAS scores revealed that patients who received adjuvant chemotherapy were more likely to report higher scores, reflecting higher symptom burden, compared to patients receiving neoadjuvant chemotherapy, including fatigue (p = 0.005), lack of appetite (p = 0.0005), and dyspnea (p < 0.0001). So far, no other studies have examined all the baseline and treatment parameters we were able to include. Our results suggest that patients with triple-negative disease may require particular attention. Previous research showed that women with triple-negative tumors had worse QoL compared to those with non-triple-negative tumors [17]. Recently, a different study with less-well studied endpoints showed that chemotherapy, triple-negative tumor, reconstructive surgery, number of outpatient visits, and income were associated with prolonged sick leave [18].
The present study also showed a certain impact of pathologic complete response at surgery due to neoadjuvant treatment on some ESAS items. Exceedingly chemosensitive patients had significantly lower mean anxiety scores (p = 0.03) and a trend towards lower depression scores (p = 0.09). Awareness of the excellent prognosis would explain why these patients were less worried in the adjuvant setting. Interestingly, triple-negative patients were not even close to reporting significantly higher anxiety or depression scores than their non-triple-negative counterparts. This fact would argue against prognostic worries as a reason for a mainly fatigue- and pain-driven higher ESAS sum. Additional research is needed to fully elucidate our findings.
When interpreting the present results, the following limitations must be acknowledged: our study cohort was comprised of Norwegian-speaking patients covered by the national publicly funded health care system. In a more diverse setting, socioeconomic factors may interfere with QoL and PROs. Since the study size and consequently statistical power were limited, we may have overlooked additional correlations that a larger study could have revealed. Longitudinal data from various timepoints during radiotherapy may provide additional information when trying to provide comprehensive, individualized supportive measures such as physical exercise, physiotherapy, psycho-oncology referral, rehabilitation, and others [19, 20], aiming at high rates of treatment completion, better QoL and role-functioning, and minimum interference of breast cancer treatment with survivors’ daily life.
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Declarations
Conflict of interest
C. Nieder, S.K. Johnsen, A.M. Winther, and B. Mannsåker declare that they have no competing interests.
Ethical standards
All procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and/or national research committee and with the 1964 Helsinki Declaration and its later amendments or comparable ethical standards. This research project was carried out according to our institutions’ guidelines and with permission to access the patients’ data.
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