Abstract
Purpose
Childhood cancer survivors (CCS) are at risk for increased morbidity and reduced quality of life associated with treatment-related late effects. In Germany, however, only a few of the more than 40,000 CCS registered in the German Childhood Cancer Registry (GCCR) currently benefit from adequate clinical long-term follow-up (LTFU) structures. To establish a comprehensive knowledge base on CCS’ long-term health in Germany, a database was developed in cooperation with the GCCR. Following a first evaluation phase at two German university centres, this database will be implemented more widely within Germany allowing longitudinal documentation of clinical LTFU data.
Methods
The feasibility study cohort comprised 208 CCS aged 18 or older whose medical, mental and psychosocial health data were collected during routine LTFU or first clinic visits in adult care. CCS were enrolled from 04/2021 to 12/2022, and data entry was completed by 03/2023. Descriptive data analysis was conducted. All CCS were stratified into three risk groups (RG) based on their individual risk for developing late effects resulting from their respective diagnoses and treatments.
Results
Chronic health conditions of various organ systems associated with late and long-term effects of cancer therapy affected CCS in all RG supporting the clinical relevance of risk-adapted LTFU. Enrolment into the database was feasible and broadly accepted amongst CCS.
Conclusion
Implementation of a clinical follow-up care infrastructure and database in Germany will pave the way to collect clinically evaluated and regularly updated health data of potentially over 40,000 German CCS and facilitate future national and international cooperation.
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Introduction
Long-term survival of childhood cancer has steadily increased during the last decades resulting in a growing community of childhood cancer survivors (CCS) worldwide (Robison and Hudson 2014). As many CCS face therapy-related chronic health conditions (“late effects”), adequate and risk-adapted clinical long-term follow-up (LTFU) care that aims at timely diagnosis and treatment of late effects is important to prevent subsequent morbidity and reduced health-related quality of life (Bhakta et al. 2017; Dixon et al. 2018). Most LTFU recommendations are based on experiences from large CCS cohorts that have been followed up regularly as part of regional or nation-wide CCS programmes (Kremer et al. 2013). At the beginning of this century, one of the largest CCS cohorts, the multi-centre North-American Childhood Cancer Survivor Study (CCSS), was established to facilitate research on long-term health outcomes in this patient group (Robison et al. 2002). It started out with a survey of over 20,000 CCS who had been diagnosed prior to the age of 21 between 1970 and 1986 and had survived for 5 years or more (Wang et al. 2022). The CCSS continues to assess various health issues in this expanding cohort of currently over 35,000 CCS. In addition, a clinical follow-up programme (SJLIFE) was set up, initially including over 9000 adult 10-year CCS originally treated at St. Jude Children’s Research Hospital, who periodically return to Memphis for comprehensive clinical evaluations (Hudson et al. 2011). Similar programmes have been set up in several European countries such as the Netherlands (Winther et al. 2015; Feijen et al. 2023).
In Germany, since 1980, childhood cancer-related data of all children and adolescents with cancer have been routinely collected by the German Childhood Cancer Registry (GCCR), embedded in the Division of Childhood Cancer Epidemiology (EpiKiK) at the University Medical Centre of Mainz of Johannes Gutenberg University. The GCCR-based cohort now exceeds 40,000 5-year CCS (Kaatsch et al. 2022). At least every 5 years, the GCCR carries out questionnaire-based follow-up on relapses and subsequent neoplasms as part of mandated duties (Kaatsch et al. 2022; Erdmann et al. 2020; Grabow et al. 2011; Langer et al. 2018). In addition, EpiKiK/GCCR-affiliated investigators have initiated and collaborated on numerous (inter)national studies on long-term health-related outcomes (Kaatsch et al. 2022; Byrne et al. 2022; van den Oever et al. 2023; Kaatsch et al. 2021; Aleshchenko et al. 2022; Botta et al. 2022).
Multidisciplinary LTFU clinics have been established at several university clinics in Germany recently (Gebauer et al. 2018), offering specialised and risk-adapted surveillance in CCS according to current guidelines (Gebauer et al. 2020). During CCS’ routine LTFU clinic visits, data on their current health status is routinely collected. We intend to document this clinically validated and prospectively assessed information comprehensively in a common database. These data can serve as a basis for future cooperation in national and international projects on chronic health conditions in CCS and facilitate joint analysis with CCS cohorts from other countries. We now present this clinical LTFU database including an analysis of the data collected during a first evaluation phase.
Materials and methods
The database includes seven categories on CCS’ health and psychosocial status as well as on previous cancer disease(s) and corresponding treatment. The categories are based on common late effects addressed in LTFU guidelines (van Kalsbeek et al. 2021) and allow free text entry for the documentation of rare chronic health conditions. Subcategories include further specifications of diseases according to standard diagnostic procedures and, if applicable, to the International Classification of Diseases (ICD) (Harrison et al. 2021).
Following a pre-test in Luebeck in 2018 (Gebauer et al. 2018), the clinical LTFU database was modified for technical and pragmatic reasons before a first evaluation period. From April 2021 until December 2022, all CCS who survived ≥ 5 years after first cancer diagnosis and attended the LTFU clinics in Luebeck and Berlin were asked to provide their written informed consent for inclusion of their data in the database. This study was approved by the ethics committee of the University to Luebeck (registration number 180-87) and the ethics committee in Berlin waived this requirement.
Depending on the type of information, required data were entered into the database either once or repeatedly during each LTFU clinic visit. Risk-adapted LTFU in the participating clinics was carried out according to published guidelines (Gebauer et al. 2020) and served as the basis for the documentation of clinical data. At inclusion into the database, participants were asked to complete five validated self-report questionnaires and one questionnaire on their living situation via a study tablet to assess mental health, psychosocial burden and fatigue (Table 1). Information from the tablet was automatically transferred to the database following data protection guidelines. Psychologists or social workers specialised in LTFU assessed the psychosocial status of the CCS during the LTFU visit considering the answers to the questionnaires to identify if further support was required.
Risk group (RG) stratification
A previously published definition of RG based on former risk stratification models (Frobisher et al. 2017) and adopted to the German health care system (Gebauer et al. 2020) was used to stratify CCS according to their risk for late effects. RG1 with a low risk for developing late effects comprises CCS who had only required surgical therapy [with exception of CCS with a central nervous system (CNS) tumour] as well as CCS of acute lymphatic leukaemia (ALL) or non-hereditary retinoblastoma who received chemotherapy only. CCS with intermediate risk for late effects (RG2) had received chemotherapy (excluding ALL and non-hereditary retinoblastoma) or, in case of a CNS tumour, had merely undergone surgical therapy. RG3 includes CCS at high(er) risk for late effects, such as after haematopoietic stem cell transplantation and/or irradiation.
Statistical analysis
Statistical analyses were conducted using SPSS IBM Version 29. Descriptive statistics were carried out for CCS whose data were completed in the database until March 22, 2023. All continuous variables are presented as means and standard deviations (SD) and as median values and interquartile ranges (IQR). Comparisons according to RG and for numerical variables were made using Kruskal–Wallis test to compare means of metric variables, such as age and body mass index, for which data were not normally distributed, and chi-square-test for other non-metric variables. Generated asymptotic p values are of purely descriptive nature. Cancer diagnoses were grouped into main categories for analyses (see Table 2). Survivors of a malignancy in adulthood, who, considering the nature of their diagnoses, had required treatment in paediatric oncology (e.g. young adults with medulloblastoma), were included in the analyses.
In case the day of cancer diagnosis was missing, it was replaced by the first day of the month. If the month was missing, it was set as January. Missing years were analysed as missing data.
Additional to describing general patient characteristics, we present the database by assessing data on health conditions in CCS at time of (first) database entry according to organ system and by RG. Late effects are also presented by the number of affected (organ) systems per patient in the respective RG. Further health-related information, e.g. family history, genetic tumour predisposition, cardiovascular risk profile as well as detailed information on mental health and psychosocial status, has also been documented in the database (see Table 1) and will be evaluated in a prospective fashion in the future observational studies and embedded trials. For this first evaluation, we decided to focus on somatic health conditions.
Results
Participant characteristics
Overall, 208 patients out of 212 agreed to participate in the study (response rate: 98.1%). Mean age of patients at enrolment into the study was 26.5 years (range 18.0–60.0), of which the majority were young adults aged 18–24 years (62.5%). On average, 16.4 years (range 5.0–57.7) had passed since cancer diagnosis. Detailed patient characteristics are presented in Table 2. CCS in our cohort were mainly diagnosed with leukaemia (36.5%) or lymphoma (26.4%) in childhood or adolescence, whilst 13.9% had previously suffered from a brain tumour (Table 2). According to RG stratification, 19.2% of participating patients had a low (RG1), 25.0% an intermediate (RG2) and 55.8% a high risk (RG3) for late effects following their cancer treatment (Table 2).
MD missing data, SD standard deviation, IQR interquartile range
aReferring to age at time of first clinical follow-up examination
bOthers: extracranial germ cell tumour, neuroendocrine tumour, adrenal cortex tumour, colon cancer, Langerhans cell histiocytosis
cDespite missing year of diagnosis, this patient is still evaluable as part of the study as per the inclusion criteria considering their date of clinical/oncological examination was documented as 2016, presupposing cancer diagnosis prior to that (> 5 years since diagnosis)
dTimespan between dates of primary oncological diagnosis and first clinical follow-up examination. Percentages may not add up to 100% due to rounding; percentages of same absolute numbers might differ as only valid values were analysed per variable
Health conditions in CCS according to RG and organ system
Chronic health conditions were documented in a considerable number of CCS (Table 3). Endocrinological disorders were found in half of all CCS documented in the database (113/208, 54.3%). For a third of our cohort (75/207, 36.2%), at least one cardiovascular health condition was documented, and about a fifth of CCS had a degree of disability (20/95, 21.1%).
Occurrence of health conditions in CCS differed amongst RG. In most categories, disorders consistently affected more CCS allocated to RG3 than CCS of RG1 or RG2 (Table 3). Overall, the number of affected organ systems increased with each RG (Fig. 1).
Information from the database also allows a breakdown of single conditions within one organ system, e.g. specification of 11 different endocrinological conditions (Fig. 2).
Number of endocrinological conditions ranged from 0 to 5 per CCS, with the majority having at least one specific condition (Fig. 3). Whilst two-third of CCS of RG1 had no endocrinological disorders and none had more than two, CCS of RG2 and RG3 suffered from up to three and five endocrinological conditions, respectively, with a lower proportion of CCS having none.
Furthermore, each subcategory was divided into several specifications providing detailed information on CCS’ health status. As an example, bone status comprised “unremarkable” (114/206, 55.3%), “vitamin D deficiency” (81/206, 39.3%), “osteopenia” (9/206, 4.4%), “osteoporosis” (3/206, 1.5%), “osteonecrosis” (3/206, 1.5%) and “not examined” (3/206, 1.5%). Percentages add up to more than 100% due to multiple selections (conditions) being possible per patient.
Discussion
Long-term health consequences of cancer and its therapy affect most CCS, resulting in a reduced health-related quality of life and life expectancy in this growing cohort (Byrne et al. 2022; van Erp et al. 2021). Comprehensive risk-based care facilitates timely diagnosis and treatment of late effects and is recommended in numerous guidelines (Frobisher et al. 2017; Kremer et al. 2013). These recommendations are based on regularly updated, extensive analyses of CCS’ health status during LTFU. For some late effects, specific surveillance strategies are lacking as reliable data on occurrence and complications of some chronic health conditions are not available yet (Bowers et al. 2021). Recommendations in favour of or against surveillance modalities, however, require careful balancing of potential benefits and harms (Clement et al. 2018; Heinzel et al. 2022). Prospectively documented and evaluated late effects in nation-wide CCS cohorts can fill these knowledge gaps (Yeh et al. 2022) and serve as a basis for future joint projects. In several countries, national cohorts of CCS, who are regularly followed up by questionnaire surveys or clinically in specialised LTFU clinics, have been established (Winther et al. 2015). To provide comprehensive information on CCS’ health status in Germany, which goes beyond the current regular follow-up on subsequent neoplasms and relapses conducted by the GCCR, a database was created to support standardised prospective and longitudinal clinical data collection from routine LTFU assessments. Generally, acceptance of the database was successful in both participating clinics with almost all eligible CCS participating in this feasibility study.
Nationwide implementation of this database over the following years will provide clinically evaluated and regularly updated health data of potentially over 40,000 German CCS. These prospectively collected data can contribute to larger international analyses of CCS data, thus creating the basis for better tailored and individualised, risk-adapted LTFU recommendations.
According to the risk stratification approach (Frobisher et al. 2017) which was applied to our cohort, a considerable larger proportion of CCS allocated to RG3 (high risk for late effects) suffered from chronic health conditions than CCS of RG1 (low risk) and RG2 (intermediate risk). This difference is most pronounced for occurrence of endocrinological and cardiovascular disorders, as well as ear–nose–throat disorders, degree of disability and occurrence of subsequent neoplasms thus supporting the clinical relevance of the proposed risk stratification. Yet, it also needs to be considered that CCS in RG3 were generally older, so time since treatment was longest in this group. This limitation in this first data analysis will potentially be diminished once the cohort documented in the database exceeds a higher number of CCS. Number of health conditions with time increased in our cohort has also been previously described (Suh et al. 2020), emphasising the necessity of LTFU, potentially life-long. However, our findings also demonstrate an already high number of chronic health conditions in a cohort of young adult CCS, illustrated e.g. by a high occurrence of endocrinological disorders, which is in line with previous work and underlines the need for regular, life-long surveillance from the beginning of survivorship on Bhakta et al. (2017), Brignardello et al. (2013).
LTFU aims at holistic health assessment. The database correspondingly includes data on physical and mental health conditions, assessment of general health information, such as vaccination record, medical history and substance use as well as psychosocial and socioeconomic parameters. Analyses of this data provide an overview of the CCS’ characteristics as well as overall and in-depth assessment of their health status, e.g. alongside the documentation of organ systems affected by health conditions, also their type and extent are documented. Specific information on health care provision derived from data analyses can be directly transferred back into LTFU care and support its improvement by adapting to CCS’ needs.
To optimise data quality for future projects, careful consideration of possible imprecisions and errors in data assessment and documentation was conducted. In this context, some limitations were detected, e.g. some variables generating high numbers of missing data due to a missing “no” option. Interpretation of such missings as negation might distort results. For this first analysis within the feasibility study, we regard our approach as justifiable, seeing as findings in the affected variables would have likely been entered into the database had they been clear and available. For example, we argue that a relapse, had it occurred, would have been documented. For future use and implementation, a “no” option was added to these variables; for “infertility”, the variable “no clinical and laboratory evidence of infertility” will be added to the assessment. In addition, occurrence of hypogonadism could not be evaluated in women taking contraceptives if no further medical history was available. That is why our numbers might differ from expected prevalences from former studies (Mostoufi-Moab et al. 2016). Careful documentation of medical history and medications is essential to generate plausible data. A checklist will be forwarded to all participating LTFU centres to ensure complete data acquisition and to minimise missing data (Online Resource 1). Furthermore, to prevent systematic errors in data entry, a database manual containing background information on respective variables was provided and will be adapted for all future study centres. All identified limitations will be addressed in a database update to optimise future analyses.
Conclusion and outlook
Risk-adapted clinical LTFU is crucial for CCS to ensure early detection of late effects of cancer treatment. However, in Germany, not all CCS benefit from such LTFU. Current structures need to be expanded to guarantee optimal health monitoring in all CCS. Our database enables a comprehensive assessment of health status in German CCS, including both general and detailed analyses of health aspects. Following a feasibility study in two LTFU clinics, data of further CCS that receive LTFU in German LTFU centres will be documented. Additionally, our database will be implemented in over ten centres in Germany as part of the prospective LE-Na trial (Evaluation and implementation of multidisciplinary, standardised, guideline-based long-term follow-up care for adult survivors of childhood cancer in Germany) which started in January 2023. During the study period of 5 years, over 5000 CCS who have not received standardised LTFU yet, will be invited to attend LTFU care in participating centres and asked for their data to be documented in the database. This comprehensive base on validated and prospectively collected CCS LTFU data will improve ongoing LTFU care and facilitate future national and international collaboration and research.
Data availability
The anonymised data that support the findings of this study are available from the corresponding author upon reasonable request.
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Acknowledgements
We thank Stefanie Braun, Lea Hildebrand, Anne-Kathrin Jahnke, Wiebke Stritter and Jana Vachek for their assistance with recruitment and documentation of study participants in the database as well as Samuel Hahn for his assistance with our list of references for psychosocial questionnaires and Cécile Ronckers for her assistance with manuscript preparation and revisions.
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Open Access funding enabled and organized by Projekt DEAL. This work was supported by the “Lübeck-Hilfe für krebskranke Kinder e.V.”.
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Conceptualisation: JG, TL. Methodology: MS, MB, JG. Software: A-KK-S, AN. Formal analysis: MS, MB, LLK. Investigation: MS, FR. Resources: A-K-KS, AN. Data curation: MS. Writing—original draft: MS, MB, JG. Writing—review & editing: MS, MB, CC, FR, AB-S, BW, LLK, GC, A-KK-S, DG, KB, AN, TL, JG. Visualisation: MS. Supervision: TL, JG. Project administration: CC. Funding acquisition: TL, JG.
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This study was performed in line with the principles of the Declaration of Helsinki. Approval was granted by the Ethics Committee of University to Luebeck (registration number 180-87) and the Ethics Committee in Berlin waived this requirement.
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Sleimann, M., Balcerek, M., Cytera, C. et al. Implementation of a clinical long-term follow-up database for adult childhood cancer survivors in Germany: a feasibility study at two specialised late effects clinics. J Cancer Res Clin Oncol 149, 12855–12866 (2023). https://doi.org/10.1007/s00432-023-05145-8
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DOI: https://doi.org/10.1007/s00432-023-05145-8