Departments of 1 Health Care Studies and 2 Methodology and Statistics, Universiteit Maastricht, Maastricht; 3 Department of Internal Medicine, University Hospital Maastricht, Maastricht, The Netherlands; 4 School of Nursing and Faculty of Medicine, American University of Beirut, Beirut, Lebanon
Received 29 October 2003; revised 10 February 2004; accepted 11 February 2004
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ABSTRACT |
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The purpose of this study was to determine the prevalence of fatigue and the course of fatigue as a function of chemotherapy in breast cancer patients undergoing adjuvant chemotherapy.
Patients and methods:
In a prospective cohort study, a sample of 157 patients with breast cancer were interviewed, using the Rotterdam Symptom Checklist and the Multidimensional Fatigue Inventory, at the first, third and fifth cycle of adjuvant chemotherapy, as well as 4 and 12 weeks after the last cycle of adjuvant chemotherapy. Patients were treated with either a doxorubicin-containing schedule, or cyclophosphamide, methotrexate and 5-fluorouracil (CMF).
Results:
The courses of general and physical fatigue are to a large extent similar. After the last cycle of chemotherapy, the CMF group reported a significant increase in fatigue, which was followed by a significant reduction. In the doxorubicin group a significant increase in fatigue was only seen during the first cycles of chemotherapy. The fatigue experienced at the first and the last measurements do not differ significantly.
Conclusions:
The prevalence of fatigue increased significantly after the start of chemotherapy. After chemotherapy treatment the prevalence rate seemed to decline. A different impact of chemotherapy on the course of fatigue was found. In the doxorubicin group a direct increase in fatigue was found. In the CMF group a moderate direct increase occurred, followed by a delayed strong increase. An increase in fatigue was associated with a decrease in daily functioning. At all measurement occasions fatigue was affected by type of operation, such that women with a mastectomy were more fatigued than women that underwent a lumpectomy. Receiving radiotherapy also led to an increase in fatigue. With this knowledge breast cancer patients can be better informed about what they can expect. Further research should include interventions addressing how to reduce or cope with fatigue during as well as after receiving adjuvant chemotherapy.
Key words: adjuvant chemotherapy, breast cancer, fatigue
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Introduction |
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Fatigue is a universal experience and is normally relieved by a good nights sleep. For cancer patients fatigue often becomes a chronic and unpleasant sensation [3]. Fatigue can be a symptom of the disease itself and may accompany cancer treatment [4]. Cancer patients receiving chemotherapy may experience a variety of side-effects, such as pain, nausea, vomiting, hair loss, weight changes, fatigue and anxiety; however, the most commonly reported side-effect is fatigue.
Breast cancer has been the most frequent type of cancer in women since the early 1990s, not only in The Netherlands but also elsewhere. Adjuvant chemotherapy is part of the standard treatment in a large subset of patients.
According to the literature, 5894% of breast cancer patients experience fatigue during treatment with adjuvant chemotherapy [57]. In a study by Sitzia and Huggins, patients with breast cancer (n = 52) who were receiving six cycles of cyclophosphamide, methotrexate and 5-fluorouracil (CMF) were examined [6]. Data were collected after each cycle. An incidence rate of ~90% was found. Fatigue severity remained stable throughout the treatment cycles. Results from Berger [8], who showed that in 72 patients with breast cancer fatigue levels 48 h after each of the first three chemotherapy cycles were not significantly different over time [8] support this finding. Jacobsen et al. also reported similar results, though the prevalence and severity of fatigue significantly increased after the start of chemotherapy, after which the prevalence of fatigue showed a stable pattern [7]. The chemotherapy regimens in this study all contain doxorubicin. Data were collected before the start of each of the first four chemotherapy cycles [7].
Studies on fatigue in breast cancer patients after treatment with adjuvant chemotherapy show prevalence rates of between 56% and 95% [912]. Only Beisecker et al. reported prevalence rates at several time points after treatment with adjuvant chemotherapy [10]. They studied 21 patients with node-negative breast cancer who had undergone adjuvant chemotherapy. Shortly after completion the prevalence rate was 95% followed by 83% 6 months later.
Berger and Higginbotham studied 14 breast cancer patients during as well as after doxorubicincyclophosphamide chemotherapy [13]. In this pilot study, fatigue was a significant problem throughout cycle three of adjuvant breast cancer chemotherapy and continued at lower levels 2 months after the last treatment.
The impact of different chemotherapy regimens, such as doxorubicin-containing regimens, on the course of fatigue is unclear and less studied. Greene et al. reported no significant differences in intensity of fatigue related to whether doxorubicin was included [5]. Berger and Walker found recently that chemotherapy protocols which contain intravenous doxorubicin were directly associated with higher fatigue at the first treatment [14]. They studied 60 women during the first three cycles of adjuvant breast chemotherapy.
There is evidence that fatigue has a strong impact on daily functioning. Berger and Higginbotham reported that higher fatigue was associated with lower activity [13]; Berger and Far found similar results [15]. The latter studied 72 breast cancer patients during the first three chemotherapy cycles after surgery for stage I/II disease [15]. The study strongly supports the position that higher fatigue is associated with daytime inactivity. Berger reported in her study not only a negative correlation between fatigue and activity level, but also found that activity levels were significantly lower in women receiving doxorubicin-based protocols [8].
Taken together, these studies support the hypothesis that fatigue is highly prevalent during as well as after the treatment of chemotherapy. Additionally, these studies suggest that the intensity of fatigue stays stable throughout the treatment cycles and declines after completion. The impact of different chemotherapy regimens, such as doxorubicin-containing regimens, on the course of fatigue is unclear and will therefore be further examined in the present study. A last hypothesis is that fatigue will have a strong impact on daily functioning.
It should be noted that previous studies had several limitations [16], such as a small sample size, the lack of a well-validated measure of fatigue and the absence of a longitudinal design in which patients with breast cancer were studied during, as well as after, receiving adjuvant chemotherapy. The purpose of the present study was to investigate the course of fatigue during (two or three measurement points) as well as after (two measurement points) adjuvant chemotherapy in an attempt to circumvent the major weaknesses of previous studies.
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Patients and methods |
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Eligible breast cancer patients met the following criteria: (i) absence of metastasis or other malignancy; (ii) no previous treatment with cytostatics; (iii) adjuvant chemotherapy treatment was as an outpatient; (iv) absence of chronic disease (such as hypertension, kidney disease, heart problems, diabetes mellitus, etc.) or poor psychological state; (v) no use of morphine or narcoleptics; (vi) no deafness; (vii) 18 years of age; and (viii) Dutch-speaking.
Patients were interviewed five times using the Multidimensional Fatigue Inventory (MFI-20) [17] and the Rotterdam Symptom Checklist (RSCL) [18], except when receiving cyclophosphamide and doxorubicin (CA) treatment, in which case participants were interviewed four times. The first interview was at the start of chemotherapy, the second at the third cycle and the third at the fifth cycle, except for the CA regimen, where the third interview was omitted. The last two interviews were at 4 and 12 weeks, respectively, after the last cycle. The first three interviews took place in the hospital and were held directly before, during or after infusion. The last two interviews were done by phone. After the interviews the medical data were retrieved from charts.
Operationalisation of variables
Intensity of fatigue
The RSCL is an instrument to measure the quality of life of cancer patients [18]. In the present study, one item of the subscale physical symptom distress was used. At each measurement the patient was asked to answer the following question: have you been bothered, during the last 2 weeks, by tiredness? The answers given were not at all, a little, quite a bit and very much. This item was used to examine the prevalence of fatigue during the study and the scores discriminated significantly between patients scoring high and low on MFI [18].
MFI-20 was used to assess the course of fatigue [17]. This 20-item questionnaire, especially designed for cancer patients, is a self-report instrument consisting of five subscales based on different dimensions: general fatigue, physical fatigue, reduced activity, reduced motivation and mental fatigue. Each subscale consists of four items and the score for each subscale was calculated as the sum of the scores of the four items. High scores indicate more subjective fatigue. The MFI-20 was previously tested and validated in cancer patients receiving radiotherapy, patients with chronic fatigue syndrome, psychology students, medical students, army recruits and junior physicians. The internal consistency for the different scales and different patient groups, as measured by Cronbachs , average 0.84 (range 0.530.93) [19]. In the present study, we focus on the results for the two subscales general and physical fatigue. In addition, correlations between the subscale reduced activity and these two subscales were calculated to give an impression of the impact of fatigue on daily functioning.
In this study, patients were asked to rate, in an interview, their fatigue as experienced during the previous 2 weeks. The items were administered in a face-to-face interview, instead of presenting the items in a self-report questionnaire, for the practical reason that the patients were already being interviewed. In addition, filling in a self-report questionnaire was expected to be too time-consuming for the patient.
Treatment of adjuvant chemotherapy
Patients were treated with one of the following adjuvant treatments: cyclophosphamide, 4-epi-doxorubicin and 5-fluorouracil (CEF), every 21 days; cyclophosphamide, doxorubicin and 5-fluorouracil (CAF), every 21 days; 4-epi-doxorubicin, every 28 days (on days 1 and 8); 4-epi-doxorubicintaxotere with the first three cycles every 28 days (on days 1 and 8) and the last three cycles every 21 days; cyclophosphamide and doxorubicin (CA) every 21 days; or CMF [cyclophosphamide, methotrexate (oral administration from days 1 to 14 or intravenous) and 5-fluorouracil] every 28 days (on days 1 and 8). Most regimens consist of six cycles, except for the CA regimen, which consists of four. The choice for either schedule was based on current practice in the participating hospitals. The involvement of different adjuvant chemotherapy regimens made it possible to create a sizeable sample in a relatively short period of time. In the analysis two groups were compared: the doxorubicin group (CEF, CAF, 4-epi-doxorubicin, 4-epi-doxorubicintaxotere and CA) and the CMF group.
Stage of breast cancer
The tumornodemetastasis TNM clinical classification is used to describe the anatomic extent of breast cancer [20].
Type of operation
Patients in the present study underwent a mastectomy or a lumpectomy with or without lymph nodes excision. Eventually, two groups were considered because of the small sizes of the other groups: (i) mastectomy with lymph nodes excision; and (ii) lumpectomy with lymph nodes excision. No reconstructive surgery was done during the study period.
Statistical analyses
First, it was tested statistically whether there were differences in patient characteristics between the CMF group and the doxorubicin group.
The prevalence of fatigue at each measurement point was determined by choosing a cut-off for the scores on the single item of the RSCL. This allowed for creating a fatigue and a non-fatigue group. Differences in prevalence across time were analysed through a logistic multilevel model using the MLwiN program (version 1.10.0006) [21]. The data consist of repeated measurements nested within hospitals and individual subjects. The data, which have a hierarchical nature, may be characterised by dependencies between units at lower levels of the hierarchy. In this case multilevel analysis is an appropriate technique [22]. The course of fatigue, using two subscales of the MFI-20, and the dependency on the type of adjuvant chemotherapy treatment, was analysed with a linear multilevel model also using the MLwiN program.
In the prevalence analyses, as well as the analyses concerning the effect of the chemotherapy regimen on the course of fatigue, dummy variables were included to represent the several measurement points. When the first measurement is taken as a reference, changes relative to the baseline measurement are analysed. The effect of chemotherapy on the course of fatigue was represented by interaction terms between these dummy variables and a binary variable chemotherapy. To correct for possibly confounding factors in this analysis, several covariates were added: age, marital status, having children, education, having a job, type of operation, stage of breast cancer, haemoglobin level (measured in mmol/l) before the first treatment of chemotherapy, the number of days between the operation and the first treatment of chemotherapy, the number of treatments at each measurement point and radiotherapy. For the covariate radiotherapy, three different variables were used: a variable indicating whether a patient had received radiotherapy at any point of measurement, the number of days of radiotherapy the patient had had at the time of measurement and the number of days between the last day of radiotherapy and the time of measurement. Also these covariates were included as interaction terms with the dummy variables representing the time points. In this way, possible differences in patient characteristics between the chemotherapy groups are corrected for.
Stepwise deletion took place in which non-significant covariates were removed. The effect of the variable treatment of adjuvant chemotherapy was examined after the final model was determined in which only significant covariates were included. For the final model, fatigue scores, which are baseline differences and are also adjusted for differences between the chemotherapy groups, can be calculated. These will be denoted as adjusted baseline differences.
Correlations were also calculated between the subscales reduced activity and general fatigue, as well as between reduced activity and physical fatigue, to give an impression of their relationship.
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Results |
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General and physical fatigue
As far as the covariates are concerned, the following variables had significant effects on general as well as physical fatigue: type of operation [2(1) = 147.384, P <0.01 and
2 (1) = 153.968, P <0.01, respectively]; duration of radiotherapy [
2(1) = 19.529, P <0.01 and
2(1) = 33.404, P <0.01, respectively]; and interval between measurement point and the last radiotherapy [
2(1) = 11.347, P <0.01 and
2(1) = 6.831, P <0.01, respectively]. Women with a mastectomy were more fatigued than women that underwent a lumpectomy. The effects for radiotherapy were the longer the duration of radiotherapy, the higher the fatigue, and the longer the time interval between the last radiotherapy session and the measurement point, the less fatigue experienced at that measurement point.
The covariate marital status was only significant for general fatigue [2(3) = 10.736, P <0.05]. Divorced women were more fatigued than women living with a partner [
2(1) = 9.515, P <0.01] and were more fatigued than single women [
2(1) = 4.241, P <0.05]. The course of physical fatigue is significantly different for the number of treatments [
2(4) = 10.429, P <0.05]. The effect of this covariate on the course of physical fatigue will be described later.
Figure 1 displays the adjusted baseline differences for general fatigue. The course of general fatigue is significantly different for the CMF and doxorubicin groups [2(4) = 12.810, P <0.05]. The intersection of the two lines in Figure 1 reflects this significant difference. In addition to the significant increase in general fatigue between measurements one and three in the CMF group [
2(1) = 5.111, P <0.05], the only consecutive significant increase is between measurements three and four [
2(1) = 4.310, P <0.05] followed by a significant decrease [
2(1) = 8.555, P <0.01]. The significant increase after treatment with chemotherapy, the so-called late effect, is not seen in the doxorubicin group (Figure 1). For this group, the only significant difference between consecutive measurements is found directly after the start of chemotherapy, between measurements one and two [
2(1) = 13.344, P <0.01]. There is also an increase between measurements one and three [
2(1) = 8.393, P <0.01], followed by a significant decrease between measurements three and five [
2(1) = 4.455, P <0.05].
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An examination of the points at which the changes in general and physical fatigue between consecutive time points are different between the two chemotherapy groups, revealed a significant difference only for the changes between measurements three and four [2(1) = 10.547, P <0.01 and
2(1) = 10.896, P <0.01, respectively]. This again underlines that the interaction between chemotherapy and measurements is mainly due to the strong late effect in the CMF group. Besides, a significant impact of the number of treatments [
2(2) = 9.168, P <0.01] on physical fatigue is only found at the last measurement, indicating a delayed effect for this factor.
Impact of fatigue on activity of the patient
Table 6 presents the correlations between the subscales reduced activity and general fatigue and between reduced activity and physical fatigue at each measurement point. All correlations are significant at P <0.01. The lowest correlation is 0.57 and the highest 0.86. Fatigue is accompanied by a strong reduction in activity.
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Discussion |
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Prevalence of fatigue
For three different classifications into fatigue and non-fatigue groups the prevalence of fatigue was compared across time. The hypothesis that fatigue is highly prevalent during, as well as after, chemotherapy treatment can be supported, but, of course, it also dependent on the method of classification of patients into fatigue and non-fatigue groups. More interesting is the fact that the changes in prevalence over time, as found in our study, are comparable, regardless of how this classification was done. In the present study, as in the previous study by Jacobsen et al. [7], a significant increase in the prevalence rates of all groups is seen after the start of chemotherapy. After this increase, as in previous studies [6, 7], a stability in the prevalence rate is found during chemotherapy treatment. After the treatment of chemotherapy the prevalence rates seem to decline.
Course of fatigue
The results for the subscales general and physical fatigue are to a large extent similar.
The type of operation turns out to influence fatigue. Women with a mastectomy operation were significantly more fatigued during the whole observation period than women who underwent a lumpectomy. Probably, the extent of surgery influences the experience of fatigue, and the loss of a breast can have devastating psychological effects on women [23].
Supplementary to chemotherapy, 69% of women in the present study received radiotherapy. Receiving radiotherapy led to an increase in fatigue. More specifically, the longer the duration of radiotherapy (number of days receiving radiotherapy), the higher the fatigue, and the longer the time interval between the last radiotherapy session and the measurement point, the less fatigue experienced at that measurement point. The findings with regard to radiotherapy are logically explicable. The accumulation of radiotherapy treatments increased the experience of fatigue. This may be explained by the trip to the treatment centre. Women had to go each weekday to the treatment centre during a period of about 5 weeks. This could be rather intensive. Besides, daily routine activities had to be adjusted to the treatments. Finally, it may be the effect of radiotherapy itself or a combination of therapies that makes these patients more fatigued [24]. After radiotherapy treatment, women recover from this intensive period, which makes the normalisation after the last treatment comprehensible. The work of Irvine et al. [25] partially supports this reasoning.
Only general fatigue was influenced by marital status: divorced women were more fatigued than women living with a partner or single women. An explanation for the significant differences between the groups might be the change in the domestic atmosphere in the (recent) past and emotional distress caused by the divorce. The finding that women living with a partner reported less fatigue might also be dependent on whether there is tangible support reducing fatigue.
The course of fatigue during the study is different for the CMF and doxorubicin groups. Although the measurement points did not cover each treatment cycle, the intensity of fatigue in the CMF group seems to be relatively stable throughout the treatment cycles. This finding supports the hypothesis that the intensity of fatigue stays stable throughout the treatment cycles. Sitzia and Huggins [6] and Berger [8] found similar results. A reason for the stability could be habituation to the experience of fatigue. The standard for determining the level of fatigue might be changing, a shift in the internal norm. This process of changing ones internal standard is called response shift [26].
In the doxorubicin group only a significant increase in fatigue was seen during the initial measurements. Berger and Walker [14] found similar results. They found that chemotherapy protocols that contain intravenous doxorubicin were directly associated with higher fatigue levels at the first treatment. Jacobsen et al. [7] also reported that breast cancer patients receiving chemotherapy protocols all containing intravenous doxorubicin experienced significantly more fatigue after the start of chemotherapy.
The CMF group shows a late effect on fatigue, which was not seen in the doxorubicin group. The CMF group reported significantly more fatigue 4 weeks after the completion of chemotherapy than that in the fifth cycle of chemotherapy. An explanation for this finding might be that healthcare providers become a support system for patients. The end of chemotherapy marks the loss of this support system and a change in routine. The support system is suddenly not available at a time when the patients fear of recurrence is enhanced [10]. This may have a negative impact on fatigue. The contact the women in the CMF group have with healthcare providers is probably more intensive than in the doxorubicin group, because they had to visit the hospital more frequently. After the significant increase in the CMF group, a significant decrease in the level of fatigue is seen 12 weeks after chemotherapy, probably because the patients have become accustomed to their daily activities again. An alternative explanation may be that the metabolism of the orally administered drug in the CMF schedule is different resulting in this delayed effect.
The level of fatigue at the last measurement did not significantly differ from the pre-treatment measurement. The hypothesis that the intensity of fatigue declines after completion is therefore supported. A limitation of the present study is the absence of a healthy control group to compare fatigue levels. Everyone experiences fatigue on a daily basis. It is not known whether the fatigue at the last measurement can be regarded as normal fatigue. Probably, it cannot be regarded as normal fatigue. First, previous studies have shown that the time span after completion of chemotherapy considered in our study is most probably too short [2729]. Secondly, it should be noted that women might be fatigued before the start of treatment. Cimprich [30] found a prevalence of fatigue in 77% of patients before primary surgery. This increased level of fatigue in patients before the start of chemotherapy may reflect lingering physical and psychological stress associated with having recently undergone breast cancer surgery [7]. It should be noted that the comparability of the results of this study to other studies may be limited because of the different measurement points that are used during, as well as after, receiving adjuvant chemotherapy [16].
Impact of fatigue on the activity of the patient
Fatigue has a strong impact on daily function. This finding is supported by previous studies [8, 13, 15].
One limitation of the present study may be the lack of homogeneity in the doxorubicin group, in which five different chemotherapy regimens are represented. This may have affected the power to detect more changes in fatigue over time for this particular group. From this study we may conclude that CMF is likely to result in a delayed increase in fatigue. However, note that no measurement took place at the last chemotherapy treatment. The possibility exists that fatigue levels at the last treatment were higher than levels one cycle before the end of treatment. Further research, in which an assessment at the last chemotherapy treatment is included is needed to conclude whether there is really a late effect in the CMF group. In addition, ongoing studies should include a comparison group of healthy subjects; fatigue tends to decline after completion of chemotherapy, but whether the fatigue levels can be regarded as normal is not yet clear.
Based on the results of this study, more specific information about fatigue can be given to breast cancer patients receiving adjuvant chemotherapy. In addition, ongoing research should include interventions addressing how to reduce or to cope with fatigue during, as well as after, receiving adjuvant chemotherapy.
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Acknowledgements |
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FOOTNOTES |
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REFERENCES |
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2. Atkinson A, Barsevick A, Cella A et al. NCCN practice guidelines for cancer-related fatigue. Oncology 2000; 14: 151161. [Medline]
3. Piper BF, Lindsey AM, Dodd MJ. Fatigue mechanisms in cancer patients: developing nursing theory. Oncol Nurs Forum 1987; 14: 1723.
4. Nail LM, King KB. Symptom distress. Fatigue. Semin Oncol Nurs 1987; 3: 257262. [Medline]
5. Greene D, Nail LM, Fieler VK et al. A comparison of patient-reported side effects among three chemotherapy regimens for breast cancer. Cancer Pract 1994; 2: 5762. [Medline]
6. Sitzia J, Huggins L. Side effects of cyclophosphamide, methotrexate, and 5-fluorouracil (CMF) chemotherapy for breast cancer. Cancer Pract 1998; 6: 1321. [CrossRef][ISI][Medline]
7. Jacobsen PB, Hann DM, Azzarello LM et al. Fatigue in women receiving adjuvant chemotherapy for breast cancer: characteristics, course, and correlates. J Pain Sympt Management 1999; 18: 233242. [CrossRef][ISI][Medline]
8. Berger AM. Patterns of fatigue and activity and rest during adjuvant breast cancer chemotherapy. Oncol Nurs Forum 1998; 25: 5162. [Medline]
9. Berglund G, Bolund C, Fornander T et al. Late effects of adjuvant chemotherapy and postoperative radiotherapy on quality of life among breast cancer patients. Eur J Cancer 1991; 27: 10751081. [ISI][Medline]
10. Beisecker AE, Cook MR, Ashworth J et al. Side effects of adjuvant chemotherapy: perceptions of node-negative breast cancer patients. Psychooncology 1997; 6: 8593. [ISI][Medline]
11. Gaston Johansson F, Fall Dickson JM, Bakos AB et al. Fatigue, pain, and depression in pre-autotransplant breast cancer patients. Cancer Pract 1999; 7: 240247. [CrossRef][ISI][Medline]
12. Okuyama T, Akechi T, Kugaya A et al. Factors correlated with fatigue in disease-free breast cancer patients: application of the Cancer Fatigue Scale. Supportive Care Cancer 2000; 8: 215222. [CrossRef][ISI]
13. Berger AM, Higginbotham P. Correlates of fatigue during and following adjuvant breast cancer chemotherapy: a pilot study. Oncol Nurs Forum 2000; 27: 14431448. [Medline]
14. Berger A, Walker SN. An explanatory model of fatigue in women receiving adjuvant breast cancer chemotherapy. Nursing Res 2001; 50: 164164. [ISI]
15. Berger AM, Farr L. The influence of daytime inactivity and night-time restlessness on cancer-related fatigue. Oncol Nurs Forum 1999; 26: 16631671. [Medline]
16. de-Jong N, Courtens AM, Abu-Saad H et al. Fatigue in patients with breast cancer receiving adjuvant chemotherapy: a review of the literature. Cancer Nurs 2002; 25: 283297. [ISI][Medline]
17. Smets EMA, Garssen B, Bonke B. Het meten van vermoeidheid met de Multidimensionele Vermoeidheids Index (MVI-20): Een handleiding. Amsterdam, The Netherlands: Medische Psychologie, Academisch Medisch Centrum 1995.
18. Haes de JCM, Olschewski M, Fayers P et al. Measuring the Quality of Life of Cancer Patients with the Rotterdam Symptom Checklist (RSCL): A Manual. Groningen, The Netherlands: Northern Centre for Health Care Research (NCH), University of Groningen 1996.
19. Smets EMA, Garssen B, Bonke B et al. The Multidimensional Fatigue Inventory (MFI) Psychometric Qualities of an Instrument to Assess Fatigue. J Psychosom Res 1995; 39: 315325. [CrossRef][ISI][Medline]
20. Beahrs OH. Manual for Staging of Cancer, 4th edition. Philadelphia, PA: Lippincott 1992.
21. Rasbash J, Browne W, Healy M et al. MLwiN (ed 1.10.0006). London, UK: Multilevel Models Project Institute of Education 2000.
22. Snijders TAB, Bosker RJ. Multilevel Analysis: An Introduction to Basic and Advanced Multilevel Modelling. London, UK: Sage 1999.
23. Spencer KW. Significance of the breast to the individual and society. Plast Surg Nurs 1996; 16: 131132. [Medline]
24. Woo B, Dibble SL, Piper BF et al. Differences in fatigue by treatment methods in women with breast cancer. Oncol Nurs Forum 1998; 25: 915920. [Medline]
25. Irvine DM, Vincent L, Graydon JE et al. Fatigue in women with breast cancer receiving radiation therapy. Cancer Nurs 1998; 21: 127135.[ISI][Medline]
26. Breetvelt IS, Van Dam FS. Underreporting by cancer patients: the case of response-shift. Soc Sci Med 1991; 32: 981987. [CrossRef][ISI][Medline]
27. Broeckel JA, Jacobsen PB, Horton J et al. Characteristics and correlates of fatigue after adjuvant chemotherapy for breast cancer. J Clin Oncol 1998; 16: 16891696. [Abstract]
28. Bower JE, Ganz PA, Desmond KA et al. Fatigue in breast cancer survivors: occurrence, correlates, and impact on quality of life. J Clin Oncol 2000; 18: 743753.
29. Leddy SK. Healthiness, fatigue, and symptom experience in women with and without breast cancer. Holist Nurs Pract 1997; 12: 4853. [Medline]
30. Cimprich B. Pretreatment symptom distress in women newly diagnosed with breast cancer. Cancer Nurs 1999; 22: 185194. [ISI][Medline]