Abstract
Purpose
The survival rates of patients undergoing allogeneic hematopoietic stem cell transplantation (HSCT) have improved. However, HSCT can induce significant long-term complications. Therefore, we investigated the late complications and risk factors for quality of life (QOL) post-HSCT.
Methods
We retrospectively analyzed 67 adult survivors over 2 years after HSCT between 2015 and 2018 at Ulsan University Hospital, Ulsan, Korea. The survey data including FACT-BMT, Hospital Anxiety and Depression Scale, and NCCN Distress Thermometer were collected as patient-reported outcomes using a tablet PC during a routine practice of survivorship clinic.
Results
The median age was 46 years. The most common symptom was fatigue (80.6%). Younger age (< 60 years), acute lymphoblastic leukemia (ALL), chronic graft-versus-host disease (GVHD), and immunosuppressant use were significantly associated with worse QOL and depression. Additionally, younger survivors (< 60 years) showed significantly more fatigue and anxiety compared with elderly survivors (≥ 60 years). Female sex was significantly associated with lower physical well-being and higher distress than male sex.
Conclusion
Younger patients (< 60 years), female, ALL, chronic GVHD, and continuous immunosuppressant use were significant risk factors for worse QOL and depression. Hence, creating a more active survivorship care plan after HSCT, specifically for these patients, is required.
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Introduction
Allogeneic hematopoietic stem cell transplantation (HSCT) is the most effective therapy for most hematological malignancies [1]. The long-term survival probability for HSCT recipients continues to improve with several advancements in transplantation techniques and supportive care practices [2, 3]. However, most patients with hematologic malignancies should receive several cycles of intensive chemotherapies before undergoing HSCT to reduce relapse risks. Moreover, chemotherapy agents used especially in HSCT compared with other solid cancers are even more toxic, since conditioning regimens in HSCT are often administered at myeloablative doses within a short period of 1 week [4]. HSCT is physically and psychosocially demanding and can cause various late complications, including chronic graft-versus-host disease (GVHD), infection, cardiovascular, pulmonary, renal, neurological toxicity, endocrine dysfunction and secondary cancers, quality of life (QOL) impairment, psychosocial issues, sexual and fertility concerns, and financial toxicity [4,5,6]. Compared with autologous stem cell transplantation, HSCT can have a higher risk of transplantation-related mortality and lead to more late complications, because acute and chronic GVHD can be caused only in HSCT. HSCT survivors are at a higher risk of long-term mortality post-HSCT throughout life after HSCT, with a four- to ninefold greater mortality risk, compared with age-adjusted population norms [2,3,4]. Therefore, long-term survivorship care is more important in HSCT survivors than any other cancer survivors. Although there have been several reports for the late effects of HSCT [7,8,9,10,11,12,13,14], survivorship studies have been mostly conducted in children and young adults, and QOL data for adult patients undergoing HSCT is insufficient. Moreover, several aspects of survivorship care after HSCT remain elusive; hence, much further effort is required to understand, monitor, and integrate the management into routine survivorship care. Therefore, we aimed to investigate the unmet needs for late complications and risk factors affecting the QOL, fatigue, anxiety, depression, and distress for adult HSCT survivors.
Methods
We retrospectively analyzed 67 adult survivors without relapse over 2 years after undergoing HSCT between 2006 and 2017 at the Ulsan University Hospital, Korea. Patients who did not have survey data, had a relapse, or died from any cause within 2 years after HSCT were excluded. Patients who underwent autologous HSCT were also excluded. The survivorship surveys as patient-reported outcomes had been performed using a tablet PC as a routine practice to evaluate patients’ medical status at the survivorship clinic of Ulsan University Hospital, Korea, since 2015 and collected as the electronic medical records. We analyzed the survivorship survey data collected between 2015 and 2018 with a retrospective chart review. Written informed consent by the patients was waived due to the retrospective nature of our study. The median time of the survey was 25.7 months after HSCT. The survey questionnaire consisted of physical and psychological symptoms, socioeconomic status, QOL, lifestyle, and regular health screening tests. Data for baseline clinicopathological features, treatments, and outcomes were collected from the medical records of each patient. The Institutional Review Boards of Ulsan University Hospital, Korea (UUH 2018-12-004-002), approved this study.
The Functional Assessment of cancer Therapy-Bone Marrow Transplantation
The QOL measurement using the Functional Assessment of Cancer Therapy-Bone Marrow Transplantation (FACT-BMT), Korean version 4.0 [15, 16], was obtained in 56 patients. The FACT-BMT is the Bone Marrow Transplantation Subscale (BMTS) added to the FACT-G that consisted of 27 items including four QOL categories (physical well-being [PWB], social/family well-being [SFWB], emotional well-being [EWB], and functional well-being [FWB]) [16]. The BMTS includes 23 items to evaluate QOL of HSCT survivors [15].
The Hospital Anxiety and Depression Scale
To screen for anxiety and depression, the Hospital Anxiety and Depression Scale (HADS), Korean version [17, 18], was included in the survey. The HADS consists of a 14-item, self-report measure for anxiety (7 items) (HADS-A) and depression (7 items) (HADS-D). For each item, respondents choose one of four options from 0 to 3, and the sum of scores for each item ranges from 0 (no anxiety and no depression) to 42 (extreme anxiety and depression) [17]. The cut-off value for screening anxiety and depression was defined as HADS score ≥ 8 for HADS-A and HADS-D, respectively [18].
The National Comprehensive Cancer Network’s Distress Thermometer
Distress was assessed using the National Comprehensive Cancer Network’s Distress Thermometer (NCCN DT) [19]. The NCCN DT is a visual analog tool that assesses distress levels to respondents in the past week on a scale of 0 (no distress) to 10 (extreme distress). The respondents indicated a yes or no for the NCCN DT in 34 questionnaires on practical, familial, emotional, spiritual/religious, and physical problems. We defined DT score ≥ 4 as clinical meaningful distress [19].
Brief Pain Inventory and fatigue
The Brief Pain Inventory (BPI) can measure pain intensity. The BPI uses the numeric rating scales from 0 (no pain) to 10 (pain as bad as you can imagine) [20]. Fatigue was measured on numeric scales from 0 (no fatigue) to 10 (fatigue as bad as you can imagine) [21].
Statistical analysis
To evaluate differences regarding physical and psychosocial needs, the referring questionnaires were analyzed according to the manufacturer’s instructions. Continuous variables were compared using the Mann-Whitney U test and one-way ANOVA test. Statistical analyses were performed using the Statistical Package for the Social Sciences version 21.0 software (IBM Statistics, Chicago, IL, USA). For all analyses, two-sided P < 0.05 was considered statistically significant.
Results
Patient characteristics
Table 1 presents the patient and clinical characteristics; the median age was 45 years (range, 21–70). Acute myeloid leukemia (AML), acute lymphoblastic leukemia (ALL), aplastic anemia (AA), and myelodysplastic syndrome (MDS) were noted in 42%, 22.5%, 18%, and 10.4% patients, respectively. Among included patients, 24% received HSCT from human leukocyte antigen (HLA)–matched sibling donors, 61% from unrelated donors, and 15% from haploidentical family donors. Reduced intensity conditioning (RIC) and myeloablative conditioning (MAC) regimens were administered in 75% and 25% patients, respectively. Anti-thymocyte globulin (ATG) was used in 76% of patients. After HSCT, all grades and grades 2–4 of acute GVHD were observed in 32.8% and 22.4% of patients, respectively. Chronic GVHD was observed in 54% of survivors. Immunosuppressive agents have been continuously administered to 28% HSCT survivors.
Patient-reported outcomes: symptoms and quality of life assessment
Table 2 represents symptom presentation categorized into organ systems among the included HSCT survivors. The most frequent symptom was fatigue (80.6% of patients). The mean brief fatigue inventory score was 3.2 (range, 0–10). The pain was observed in 23.9% of survivors. Headache, chest pain, dry eye, and conjunctival injection were observed in 13.4%, 14.9%, 37%, and 32.8% survivors, respectively. Oral mucosal problems such as dry mouth, gingivitis, and oral pain were noted in 22.4%, 23.9%, and 34.3% survivors, respectively. Additionally, insomnia, memory disturbance, and joint stiffness or pain were observed in 34.3%, 29.9%, and 20.9% survivors, respectively. HADS, NCCN DT, and QOL (FACT-BMT) data of all survivors are summarized in Table 2. Regarding the psychological aspect, anxiety (HADS-A score ≥ 8) and depression (HADS-D score ≥ 8) were detected in 14.9% and 13.6% survivors, respectively. Moreover, clinically significant distress (NCCN DT score ≥ 4) was observed in 10.4% of survivors.
Differences in quality of life (FACT-BMT) according to clinical factors
The QOL measurement by FACT-BMT was analyzed in subgroups for clinical factors (Table 3). Younger survivors (< 60 years) showed significantly worse QOL for physical (P = 0.002), emotional (P = 0.006), and functional well-being (P = 0.014), and Bone Marrow Transplantation Subscale (BMTS) (P = 0.021) and Total Outcome Index (TOI) (P = 0.002) except SFWB than elderly survivors (≥ 60 years). The differences in FACT-BMT by age groups are shown in Fig. 1. Female sex was significantly associated with lower PWB (mean, 23.7 vs. 25.8, respectively, P = 0.046) and BMTS (mean, 27.3 vs. 30.7, respectively, P = 0.036) than male sex. Regarding disease types, ALL was associated with worse QOL than other diseases such as AML, MDS, CML, AA, and lymphoma. ALL survivors had significantly lower scores in emotional (mean, 16.7 vs. 20.2, respectively, P = 0.004) and functional well-being (mean, 15.8 vs. 21.8, respectively, P = 0.002) and general functional assessment of cancer therapy (mean, 72.8 vs. 85.9, respectively, P = 0.002), BMTS (mean, 25.5 vs. 30.1, respectively, P = 0.029), and TOI (mean, 63.9 vs. 77.2, respectively, P = 0.006) than those with other diseases.
On the contrary, no significant difference in QOL was noted by donor types such as matched sibling, unrelated, and haploidentical family donors. Moreover, conditioning intensity, types of conditioning regimens, and the use of ATG did not significantly affect QOL after HSCT. The history of acute GVHD (grades 2–4) was not significantly associated with QOL. However, chronic GVHD had a significant adverse impact on QOL, specifically in PWB (23.3 vs. 26.6, respectively, P = 0.001) and TOI (70.7 vs. 79.1, respectively, P = 0.024). Similarly, continuous immunosuppressant use significantly adversely affected QOL including PWB (P = 0.007), BMTS (P = 0.023), and TOI (P = 0.033) (Fig. 1).
Risks of fatigue, anxiety, and depression according to clinical factors
Table 4 represents fatigue, anxiety (HADS-A), and depression (HADS-D) of HSCT survivors according to clinical factors. Younger survivors (< 60 years) showed a significantly higher tendency toward fatigue (P = 0.008), anxiety (P = 0.001), and depression (P = 0.025) than elderly survivors (≥ 60 years). ALL was significantly associated with higher depression scores than other diseases (AML, MDS, CML, AA, and lymphoma) (mean, 6.5 vs. 4.0, P = 0.028, respectively). Busulfan plus fludarabine regimen was significantly associated with lower fatigue scores than busulfan plus cyclophosphamide or other regimens (mean, 2.3 vs. 4.4, respectively, P = 0.008). Conditioning intensity, use of ATG, and donor types such as matched sibling, unrelated, and haploidentical family donors were not associated with fatigue, anxiety, depression, and distress. Depression risk was significantly associated with chronic GVHD (mean, 3.6 vs. 5.4, respectively, P = 0.015) and continuous immunosuppressant use (mean, 3.9 vs. 6.3, respectively, P = 0.019). However, the history of grades 2–4 of acute GVHD had no significant association with fatigue (P = 0.353), anxiety (P = 0.267), depression (P = 0.215), and distress (P = 0.328).
Lifestyle and health screening status
Table 5 represents the lifestyle and health screening status of survivors. Body weight gain and loss were observed in 40% and 9.0% of survivors, respectively. Regular exercise more than 3 times a week was performed in 47.7% of survivors, whereas 21% of survivors did not exercise at all. Moreover, 52.2% of survivors returned to their work, 17.9% of HSCT survivors were alcohol consumers, and 7.5% of survivors were current smokers even after HSCT. Furthermore, 28.4% of survivors have taken herbal medications or health supplements. A regular health screening test has been conducted only in 59.7% of survivors.
Discussion
We found the unmet needs of 67 survivors undergoing HSCT over 2 years in terms of physical and psychological problems, QOL, lifestyle, and healthcare. Fatigue was the most common symptom (80.6% of survivors). The etiology may be multifactorial, including reduced physical activity and adverse side effects of taking medications after HSCT [22]. Additionally, late effects such as pain and discomfort after HSCT were manifested in most body organs (Table 2). Clinically meaningful distress was observed in 10.4% of survivors. According to HADS scores ≥ 8, anxiety and depression were observed in 14.9% and 13.6% survivors, respectively. Besides, we found that insomnia and memory disturbance was significant in more than one-third of survivors.
Previous studies regarding late complications and QOL in long-term survivors have been mostly conducted in children or young adult patients who underwent HSCT with MAC [11, 23]. However, in our data, the median age of survivors was 45 years. Moreover, the majority of patients (74.7%) were treated with RIC. Regarding conditioning intensity, long-term QOL after HSCT was comparable between the MAC and RIC groups. Clavert et al. reported similar results in a study of 100 adult patients who underwent RIC HSCT [24]. Moreover, no significant differences between the MAC and RIC groups were noted [13, 14, 25]. RIC patients are expected to experience good QOL in the early post-transplantation period because of lower regimen-related toxicities, and an impaired QOL might be observed in the later post-transplantation period because of high rates of chronic GVHD [24]. However, patients treated with MAC experienced more fatigue than those with RIC.
In a study of 155 patients with AML or ALL undergoing HSCT at CR status, Bonifazi et al. reported that the ATG group had better survival rates without relapse than the no-ATG group [26]. However, we showed that ATG use was not associated with long-term QOL, fatigue, anxiety, depression, and distress after HSCT. In recent years, HSCT with unrelated or haploidentical donors as well as HLA-matched sibling donors have significantly increased [27]. No significant differences in QOL among donor types such as matched sibling, unrelated, or haploidentical familial donors were noted.
Interestingly, younger age (< 60 years) was more significantly associated with poor QOL (FACT-BMT score) and a higher risk of fatigue than older age (≥ 60 years). Generally, elderly patients are considered to have more comorbidity than younger patients, but QOL and fatigue were not associated with comorbidity in our data. Younger survivors (< 60 years) showed more anxiety and depression than elderly survivors, and this might influence their QOL and fatigue negatively. Associations between anxiety or depression and QOL were demonstrated in several previous studies [28, 29].
ALL survivors showed significantly higher depression score (HADS-D) and worse QOL score (FACT-BMT) than those with other diseases. It might be because patients with ALL could usually be treated with more intensive chemotherapies than other diseases including AML, MDS, and AA. In a recent study, Haykawa et al. showed that glucocorticoid therapy was a risk factor for decreased body mass index, delayed recovery of muscle strength, and avascular necrosis [10, 30]. More use of glucocorticoid usually combined with chemotherapy regimens for ALL might adversely affect QOL, although we could not analyze glucocorticoid use among the survivors. Major depression is a possible risk factor for survival after HSCT [31]. Psychological problems such as anxiety and depression are easily underestimated during the HSCT treatment period. Therefore, regular screening and management for psychological problems including anxiety, depression, insomnia, and memory disturbance are important to improve QOL for survivors post-HSCT.
Moreover, the significant adverse factors affecting QOL and depression after HSCT were chronic GVHD and continuous immunosuppressant use, whereas severe acute GVHD was not associated with long-term QOL after HSCT. The negative impact of chronic GVHD on QOL has been reported [9, 10, 24]. However, patients with resolved chronic GVHD had comparable QOL with survivors who had never been diagnosed with chronic GVHD [9]. Therefore, chronic GVHD management is important to improve QOL for HSCT survivors. In chronic GVHD, the eye and mouth are the most commonly involved sites, and more than one-third of survivors showed eye and oral problems including dryness or pain, consistent with a recent review article [8]. Therefore, regular consultation with ophthalmologists and dentists is recommended for HSCT survivors. Chronic GVHD can result in joint destruction and associated pain and loss of range of motion [30]. Joint stiffness or pain caused by chronic GVHD needs regular examination by physicians. Moreover, active physical therapy after HSCT can be beneficial for muscle relaxation and strength [30].
Additionally, compared with male, female survivors showed significantly worse PWB and higher distress (P = 0.046 and P = 0.05, respectively). Impairment of PWB on QOL questionnaires was associated with the most altered exercise capacity and the degree of physical health impairment [32, 33]. In previous studies on exercise programs after HSCT, fatigue, aerobic capacity, muscle strength, and QOL were improved [34]. Therefore, controlling physical symptoms and creating programs to improve exercise capacity might be important to improve QOL, specifically for female survivors.
Reduced exercise capacity has been associated with fatigue, disability, and poor QOL [17, 35]. Dirou et al. reported that a high proportion (75.4%) of HSCT survivors had mild to severe exercise capacity impairment at 1-year post-HSCT. Significant improvements in QOL and potential physiological and psychosocial benefits have been reported after HSCT in the previous exercise intervention studies by Juan et al. [36] and Bogg et al. [37]. Therefore, exercise or physical therapy is routinely recommended before, during, and after HSCT aimed at improving QOL, reducing disease burden, improving physical function, assisting reintegration to social activities, and returning to work and normal activities of daily life [30]. In this study, 52.2% of survivors did not exercise sufficiently (no exercise or 1–2 times a week) after HSCT; regular exercise (3–5 times a week) should be advised for HSCT survivors to reduce fatigue and improve QOL.
Gastrointestinal side effects including GI GVHD can be observed during HSCT, and malnutrition and weight loss after HSCT may occur; thus, adequate nutritional support is emphasized to the survivors [38]. However, it should be also educated that the beneficial effects of most herbal medications or health supplements were not demonstrated, because 28.4% of survivors administered herbal medication or health supplements as shown in our data.
Among survivors, 7.5% and 17.9% were current smokers and alcohol consumers survivors, respectively. To prevent late comorbidity and secondary malignancies, survivors need to be continuously educated to stop smoking and drinking alcohol. Low QOL and depression are associated with a higher risk of smoking and higher difficulties of smoking cessation [39]. Therefore, the screening and management of depression would be helpful for HSCT survivors to quit smoking. Moreover, regular health screening tests for late complications and secondary malignancies had not been conducted in 40% of HSCT survivors. Therefore, education for lifestyle modification such as regular exercise, diet, and smoking and alcohol cessation, and regular health screening should be incorporated when creating a survivorship care plan for HSCT survivors. In this study, employment after HSCT was maintained in 52.2% of survivors. High unemployment might affect healthcare status and compliance for monitoring secondary malignancies and relapse and might result in socioeconomic problems and distress. Hence, consultations with the social welfare team are essential when creating a survivorship care plan.
To our knowledge, this is the first study of PRO using a tablet PC during routine survivorship care for HSCT survivors. There are some limitations that this is not a prospective study. Nevertheless, we have routinely conducted a general assessment regarding the physical, psychological, and socioeconomic aspects, QOL, and lifestyle for over 2 years in non-relapse HSCT patients. Hundreds of questionnaires assessing whole organ problems, depression, anxiety, QOL, and lifestyle can be easily screened and assessed using a tablet PC approximately 30 min before meeting a physician in real practice. The survey of PRO using a tablet PC for HSCT survivors is considered an easy and fast method, although it is sometimes not applicable for elderly patients who have a visual impairment or not used to dealing with a tablet PC.
In conclusion, younger age (< 60 years), female, ALL, chronic GVHD, and continuous immunosuppressant use are high risk factors for poor QOL and depression. Considering our understanding regarding the risk factors of late effects and unmet needs for HSCT survivors, we have to build a more active patient-directed survivorship care plan after HSCT.
Abbreviations
- HSCT:
-
Allogeneic hematopoietic stem cell transplantation
- GVHD:
-
Graft-versus-host disease
- QOL:
-
Quality of life
- FACT-BMT:
-
Functional Assessment of Cancer Therapy-Bone Marrow Transplantation
- BMTS:
-
Bone Marrow Transplantation Subscale
- PWB:
-
Physical well-being
- SFWB:
-
Social/family well-being
- EWB:
-
Emotional well-being
- FWB:
-
Functional well-being
- HADS:
-
Hospital Anxiety and Depression Scale
- HADS-A:
-
HADS-anxiety
- HADS-D:
-
HADS-depression
- NCCN DT:
-
National Comprehensive Cancer Network’s Distress Thermometer
- BPI:
-
Brief Pain Inventory
- AML:
-
Acute myeloid leukemia
- ALL:
-
Acute lymphoblastic leukemia
- AA:
-
Aplastic anemia
- MDS:
-
Myelodysplastic syndrome
- RIC:
-
Reduced intensity conditioning
- MAC:
-
Myeloablative conditioning
- ATG:
-
Anti-thymocyte globulin
- TOI:
-
Total Outcome Index
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Funding
This work was supported by the Basic Science Research Program through the National Research Foundation of Korea (NRF) funded by the Ministry of Education, Science and Technology (NRF-2017R1C1B5015107), and it was also supported by the Ulsan University Hospital Research Grant (UUH-2019-06).
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Yunsuk Choi, Jaekyoung Cheon, Jae-Cheol Jo, SuJin Koh, and Young Ju Min contributed to the study conception and design. Patient management and data collection were performed by Jaekyoung Cheon, Yoo Jin Lee, Jae-Cheol Jo, Kukju Kweon, Sang-Hyuk Park, Sin-hye Lee, and Hyo-jin Kim. Data analysis was performed by Yunsuk Choi and Jaekyoung Cheon. The first draft of the manuscript was written by Yunsuk Choi and Jaekyoung Cheon. All authors reviewed the manuscript and contributed to the editing of the manuscript. All authors read and approved the final manuscript.
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Cheon, J., Lee, Y.J., Jo, JC. et al. Late complications and quality of life assessment for survivors receiving allogeneic hematopoietic stem cell transplantation. Support Care Cancer 29, 975–986 (2021). https://doi.org/10.1007/s00520-020-05572-0
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DOI: https://doi.org/10.1007/s00520-020-05572-0