Abstract
Background
Childhood cancer is neglected within global health. Oxford Pediatrics Linking Oncology Research with Electives describes early outcomes following collaboration between low- and high-income paediatric surgery and oncology centres. The aim of this paper is twofold: to describe the development of a medical student-led research collaboration; and to report on the experience of Wilms’ tumour (WT).
Methods
This cross-sectional observational study is reported as per STROBE guidelines. Collaborating centres included three tertiary hospitals in Tanzania, Rwanda and the UK. Data were submitted by medical students following retrospective patient note review of 2 years using a standardised data collection tool. Primary outcome was survival (point of discharge/death).
Results
There were 104 patients with WT reported across all centres over the study period (Tanzania n = 71, Rwanda n = 26, UK n = 7). Survival was higher in the high-income institution [87% in Tanzania, 92% in Rwanda, 100% in the UK (X2 36.19, p < 0.0001)]. Given the short-term follow-up and retrospective study design, this likely underestimates the true discrepancy. Age at presentation was comparable at the two African sites but lower in the UK (one-way ANOVA, F = 0.2997, p = 0.74). Disease was more advanced in Tanzania at presentation (84% stage III–IV cf. 60% and 57% in Rwanda and UK, respectively, X2 7.57, p = 0.02). All patients had pre-operative chemotherapy, and a majority had nephrectomy. Post-operative morbidity was higher in lower resourced settings (X2 33.72, p < 0.0001). Methodology involving medical students and junior doctors proved time- and cost-effective. This collaboration was a valuable learning experience for students about global research networks.
Conclusions
This study demonstrates novel research methodology involving medical students collaborating across the global south and global north. The comparison of outcomes advocates, on an institutional level, for development in access to services and multidisciplinary treatment of WT.
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Introduction
Background
Nephroblastoma [Wilms’ tumour (WT)] is the most common paediatric renal tumour, thought to arise from persistent metanephric cells or nephroblastomatosis [1]. Outcomes have improved significantly in high-income countries (HIC) over the past few decades with the 5-year survival rate increasing from 20% in the 1960s to over 90% in the current decade [2,3,4,5]. This improvement is due to a multidisciplinary approach to treatment, and to a series of clinical trials led by two large study groups: the North American Children’s Oncology Group via The National Wilms Tumour Study (NWTS) group, and the European Société Internationale d’Oncologie Pédiatrique (SIOP) group.
Outcomes are much poorer in low- and middle-income countries (LMIC), with survival in sub-Saharan Africa ranging from 11% in Sudan to 46% in Malawi [6]. The disparity in survival is multi-factorial: access to and availability of treatment; late presentation; limited resources and a paucity of trained staff; malnutrition; limited supportive care; abandonment of treatment; poverty; and perception of incurability [7,8,9,10]. Furthermore, the burden of childhood cancer predominates in LMIC (84%), where 90% of the world’s children live [11].
Oxford Paediatrics Linking Oncology Research with Electives (OxPLORE) is a collaboration founded in 2017 that unites HIC-based medical students with peers and junior doctors in LMIC settings during their elective placements. This novel research methodology of harnessing medical student power in medical research has been described elsewhere [12]. OxPLORE was conceived and developed at Oxford University, UK, by a group of medical students interested in global surgery and a trainee in paediatric surgery (KF), with the support of the senior author (KL).
Objectives
The overall aim of OxPLORE is to foster bidirectional partnerships, enabling robust data collection to guide advancements in paediatric surgical and oncology care globally. In this paper, we report the centres’ experiences of WT.
Materials and methods
Oxford medical students were recruited through advertising events preceding their elective placements. Students were provided with a letter of endorsement from the senior author (KL) to aid obtaining ethical approval; a data collection proforma; and were advised to engage with a local medical student or junior doctor. Electronic messaging and conferences enabled ongoing communication with collaborators after students returned from their electives. Data exchange occurred through security password-encoded excel spreadsheets. Deadlines were set for collation of data by Oxford and were analysed centrally (KF) given unpredictable working demands for collaborators in Tanzania and Rwanda.
Reporting of this study has been verified as per the STROBE (Strengthening the Reporting of Observational Studies in Epidemiology) checklist [13].
Study design and setting
The Phase One OxPLORE study is a cross-sectional observational study. Three collaborating centres were included in the study:
-
(1)
Muhumbili National Hospital (MNH), Dar es Salaam, Tanzania
-
(2)
Centre Hospitalier Universitaire de Kigali (CHUK), Kigali, Rwanda
-
(3)
Oxford University Hospital (OUH), UK.
A retrospective medical record review was performed by collaborating centres of all children (< 16 years) presenting with WT between January 2016 and December 2017.
OUH uses an electronic patient registration system, allowing identification of children diagnosed with WT. There was no electronic system in MHN or CHUK, and patients were identified via inpatient ward registries, clinician notes and theatre logbooks.
Participants
There were no patient exclusion criteria other than age. Criteria for inclusion as a study site were close collaboration and transfer of research knowledge and skills between H- and LMIC medical students/junior doctors, senior clinician support from collaborating centre and local ethical approval.
Variables and outcomes
The primary outcome was survival to the point of discharge or death, whichever came first. Secondary outcomes included: patient demographics; stage of tumour at presentation; management (surgical and adjuvant medical); and post-operative morbidity. Post-operative morbidity was categorised as per the Clavien–Dindo classification: stage 1 (deviation from normal post-operative course without need for intervention); stage 2 (requiring pharmacological treatment); stage 3 (requiring surgical, radiological or endoscopic intervention); stage 4 (life-threatening events needing intensive care or involving organ failure) [14].
Data collection, management and analysis
Data were retrospectively taken from patient files using a paper version of a standardised data collection tool. The tool was agreed by all three participating sites, allowing reliable comparison, before commencing data collection. Anonymised data were recorded electronically at each centre and analysed centrally using Graphpad Prism® version 8 (KF). Data are presented as median (range) unless otherwise stated and p values of < 0.05 considered statistically significant. One-way ANOVA was used to compare continuous variables, and Chi-squared tests to compare categorical variables. Missing data are acknowledged, but no statistical methods employed to account for them.
Ethics/study oversight
Regarding individual patients, there was no perceived risk or incentives, and consent was not required. Confidentiality was ensured and all data anonymised. Institutional endorsement was sought at each participating centre’s review board, where the research protocol was reviewed and approved by the ethics board of CHUK (Ref: EC/CHUK/680/2018), MNH (Ref: MNH/TRC/III/2018/018) and OUH (Ref: 4741).
Results
Collaboration development
The educational value of this collaboration for the junior researchers is evidenced through the presentation of results by medical students from the UK (SG) and Rwanda (EM), and surgical trainee (KF) at international conferences in 2019. Moreover, students benefited from early experience in the challenges of international research, namely varying local protocols for ethical approval, time differences for communication, and limited time spent abroad. The costs of running phase one of the OxPLORE collaboration itself were by design minimal, and subsequent funding for attending presentations was sourced and applied for by students, which served as further experience in medical research. The collaboration also served as an experience of communication, on a peer–peer basis, junior-senior basis and low–high resource basis. The benefits to all parties on an educational and personal level were anecdotally commented on by all positively.
Outcomes
Further details and background of participating centres are shown in Table 1. There were 104 patients with WT treated in the three centres over the 2-year study period, with a larger patient volume in MNH (n = 71 cf. n = 26 in CHUK and n = 7 in OUH). Table 2 describes the core outcome set. Survival over the 2-year study period was 87% in MNH, 92% in CHUK and 100% in OUH at time of data closing (December 2018).
Presentation
More females with WT presented to the OUH cohort (86% cf. 41% and 42% in MNH and CHUK, respectively). Age at presentation is shown in Fig. 1. There was no significant difference overall in age at presentation (one-way ANOVA, F = 0.2997, p = 0.74); however, the violin plots demonstrate a trend of younger age of presentation in the HIC setting [majority cluster of patients around the median in all three sites (40 months in MNH, 37 months in CHUK and 24 months in OUH)].
Stage of disease at presentation was varied across the centres (Fig. 2). Stage in CHUK and OUH was widespread, whereas disease was more advanced in MNH. This was a significant finding when the data were categorised into stages I–II and compared with stages III–V (X2 7.57, p = 0.02).
The presenting haemoglobin was similar in patients in the different centres, and no significant difference was found on one-way ANOVA (F = 1.144, p = 0.32). Figure 3 shows the data distribution, where the range is noted to be more varied in the MNH cohort [median 9.88 g/dl (range 5.4–15.3 g/dl)], compared with CHUK [median 10.1 g/dl (range 6–10.4 g/dl)] and OUH [median 9.2 g/dl (range 7.5–9.5 g/dl)].
Treatment
All patients had pre-operative chemotherapy (SIOP regimen). Most patients had nephrectomy (80% MNH, 81% CHUK and 86% in OUH). Those who did not were deemed inoperable.
Post-operative morbidity (Clavien–Dindo scale) varied widely between the centres (Fig. 4), with more morbidity in the lower resourced settings when categories I–II were compared with III–IV (X2 33.72, p < 0.0001).
Discussion
The aim of this OxPLORE study was twofold: firstly, to establish and trial a medical student-facilitated research collaboration, using medical electives and existing links between the global north and south; and secondly to describe phase one results following the collaboration of three centres interested in comparing their experience of WT.
Student-led research collaborations have been shown to enable students to engage in high-quality studies with great impact, while gaining fundamental skills in study design and delivery [15]. Further, the bidirectional advantages of HIC-LMIC research partnerships are well described [16]. Worldwide, the highest burden of disease is in LMIC; however, medical research originating from these countries is limited. Collaboration between the different resourced settings can help overcome the challenges LMIC researchers face, including: few qualified researchers, less funding, limited infrastructure and lack of protected research time [17, 18]. The utilisation of medical students to undertake research bypasses the issue of limited research time for overburdened doctors.
Validation of the success of this collaboration has not formally been conducted. Manifestation of valuable learning to individuals is demonstrated through formal presentations by collaborating medical students and contributions to this paper. This confers a ‘result’ impact of training, as per the Kirkpatrick model of evaluation [19]. Moreover, the personal relationships that have evolved from the first phase of the OxPLORE collaboration will continue to be nourished in the long-term and will provide the foundation for career-long collaboration between students in training and research. This contrasts with large global research collaborations, which can be faceless and do little to support or develop low- and middle-income partners.
OxPLORE has strived to address the power imbalance which can manifest in relationships between LMIC and HIC researchers by developing its research agenda collaboratively. Further, the collaboration with MNH was born from a longstanding partnership with OUH, the Oxford Tanzania Link [20], which shares experiences, supports medical learning and encourages adoption of the best medical practice.
Survival
Survival was higher in the HIC than the two LIC centres in the OxPLORE study. In this study, inadequate treatment does not seem to be a key contributor to disparities in mortality rate as comparative treatment options were available in all three centres. The lower chance of cure in less developed countries has been attributed to access to care, late diagnosis, inadequate resources for treatment, poor organisation and high rates of abandonment [21, 22]. Further, political instability also has negative effects on the reliable delivery of sustainable health programs in the African continent [23]. WT is a difficult cancer to cure in LMIC due to the multidisciplinary nature of the treatment involving surgery, imaging, pathology and oncology services. Although MNH and CHUK both have multidisciplinary paediatric oncology teams, this study could provide the evidence to initiate audit and analysis of the team efficacy and aid the departments in the advocacy of their needs.
Interestingly, OxPLORE reported survival rates in MNH (87%) and CHUK (92%) were higher than other studies in sub-Saharan Africa. Survival rates of 41% and 46% were reported in a similar retrospective study performed over a 2-year period at a single Kenyan centre [24] and Malawian centre, respectively [25]. The Malawian authors have further reported an associated haematological toxicity and treatment-related mortality in malnourished children following the initiation of SIOP pre-operative chemotherapy regimen [26]. Other outcomes in terms of 2-year event-free survival in North Africa [27] (73–87%) and sub-Saharan Africa [7] (47%) have been attributed to the studies analysing patients with low- or intermediate-risk tumours, without metastatic disease or progression post-operatively. Survival rates reported at 2–3 years follow-up from a population-based registry study in Eastern Africa were 38.7% in Harare, Zimbabwe; 15.8% in Kampala, Uganda; and 22.9% in Nairobi, Kenya [28]. Our higher survival rate could be accounted for by the short-term follow-up of the OxPLORE study, and our definition of ‘survival’, as this will inevitably include patients who are palliative at the time of analysis. Unpublished survival data from MNH over a 2-year period report an ‘alive and well’ group of 47% at 12 months and 45% at 18 months.
Although not observed in this dataset, a key barrier to effective cancer treatment in children in sub-Saharan Africa is the abandonment of treatment. Regarding WT specifically, the period after surgical removal is the highest risk period [29], with misunderstanding of treatment plans and financial difficulty being identified as key causes for treatment abandonment in a Kenyan survey [30]. Loss to follow-up has been reported at 50% in Kenya, and countrywide efforts have been employed to enhance compliance. Introduction of a National Hospital Insurance Fund (NHIF) enrolment has been effective at increasing the numbers of patients completing successive phases of therapy and decreasing the risk of death [31].
Presentation and treatment
We reported differences in presentation between the three collaborating centres, including larger patient volume in MNH compared with CHUK and OUH. Patients tended to be younger in OUH which likely reflects their earlier presentation and the more advanced disease observed in the sub-Saharan African centres.
A further key difference between centres was post-operative morbidity. MNH had a much higher burden of severe post-operative complications (84% with a Clavien–Dindo score III–V). Varying levels of intra- and post-operative facilities, resources and expertise to manage complications might account for this discrepancy. Furthermore, complex tumours of more advanced stage confer riskier and more challenging operations. Pre-operative morbidity status also influences subsequent outcome. Indeed, malnutrition at diagnosis results in increased treatment-related morbidity and treatment abandonment rate, and inferior event-free survival [32].
Limitations of study
There are several limitations in this study. Regarding study design and methodology, it was decided that a limited number of outcome measures would be recorded. This was due to predicted limitations of information in patient records and the fact that OxPLORE’s inaugural study was also intended as a proof of concept of this multinational collaboration, so a simple study design is required. Furthermore, there were only a small number of patients in the OUH cohort, which limited the power of statistical analysis. The referral basin for OUH is a smaller (regional) population, compared to MNH and CHUK which serve as national referral centres for paediatric oncology in Tanzania and Rwanda, respectively. Finally, long-term follow-up of identified patients was not possible in this retrospective study which limits the interpretation of survival rates and ability of conclusions to be drawn regarding treatment abandonment and causation of morbidity and mortality.
Challenges faced, particularly in the LMIC setting, included missing data, access to data and obtaining ethical approval. As phase one methodology was retrospective, data quality is difficult to assess, so the generalisability and reliability of results may be affected.
Recommendations
Childhood cancer is a public health problem in developing countries. The majority of African children with cancer die without access to healthcare resources [23]. These same childhood cancers have excellent curative potential given the ideal treatment programmes, thus presenting an opportunity for improvement [33]. We recommend interventions at all stages of the child cancer journey, with focus on: early access to diagnosis; treatment in a multidisciplinary setting (involving surgical expertise, histology services, specialised nursing, pharmacy, laboratories, radiology, palliative care, infectious diseases, critical care and nutrition) via a standardised protocol and measures to address abandonment of treatment and loss to follow-up (Fig. 5).
Conclusion
Phase one of OxPLORE has proven the feasibility of medical student partnerships between HIC and LMIC to undertake collaboration, data collection and research outcome dissemination. This global collaboration and comparison describes the disparity in global outcomes of WT and advocates for the public health dilemma to be addressed as a global health priority.
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Acknowledgements
We thank all members of staff in MNH, CHUK and JRH and contributors to OxPLORE who have supported this project.
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Ford, K., Gunawardana, S., Manirambona, E. et al. Investigating Wilms’ Tumours Worldwide: A Report of the OxPLORE Collaboration—A Cross-Sectional Observational Study. World J Surg 44, 295–302 (2020). https://doi.org/10.1007/s00268-019-05213-6
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DOI: https://doi.org/10.1007/s00268-019-05213-6