- 1Department of Endocrinology and Diabetes, Perth Children’s Hospital, Nedlands, WA, Australia
- 2Children’s Diabetes Centre, Telethon Kids Institute, The University of Western Australia, Perth, WA, Australia
- 3Centre for Child Health Research, The University of Western Australia, Perth, WA, Australia
- 4Division of Paediatrics within the Medical School, The University of Western Australia, Perth, WA, Australia
- 5School of Public Health and Preventive Medicine, Monash University, Melbourne, VIC, Australia
- 6Diabetes and Vascular Medicine, Baker Heart and Diabetes Institute, Melbourne, VIC, Australia
- 7NHMRC Clinical Trials Centre, The University of Sydney, Sydney, NSW, Australia
- 8Division of Endocrinology, Women’s and Children’s Health Network, North Adelaide, SA, Australia
- 9Faculty of Health and Medical Sciences, The University of Adelaide, Adelaide, SA, Australia
- 10Department of Paediatrics, University of Otago, Christchurch, New Zealand
Background: Technology use, including continuous glucose monitoring (CGM) and insulin pump therapy, is associated with improved outcomes in youth with type 1 diabetes (T1D). In 2017 CGM was universally funded for youth with T1D in Australia. In contrast, pump access is primarily accessed through private health insurance, self-funding or philanthropy. The study aim was to investigate the use of diabetes technology across different socioeconomic groups in Australian youth with T1D, in the setting of two contrasting funding models.
Methods: A cross-sectional evaluation of 4957 youth with T1D aged <18 years in the national registry was performed to determine technology use. The Index of Relative Socio-Economic Disadvantage (IRSD) derived from Australian census data is an area-based measure of socioeconomic status (SES). Lower quintiles represent greater disadvantage. IRSD based on most recent postcode of residence was used as a marker of SES. A multivariable generalised linear model adjusting for age, diabetes duration, sex, remoteness classification, and location within Australia was used to determine the association between SES and device use.
Results: CGM use was lower in IRSD quintile 1 in comparison to quintiles 2 to 5 (p<0.001) where uptake across the quintiles was similar. A higher percentage of pump use was observed in the least disadvantaged IRSD quintiles. Compared to the most disadvantaged quintile 1, pump use progressively increased by 16% (95% CI: 4% to 31%) in quintile 2, 19% (6% to 33%) in quintile 3, 35% (21% to 50%) in quintile 4 and 51% (36% to 67%) in the least disadvantaged quintile 5.
Conclusion: In this large national dataset, use of diabetes technologies was found to differ across socioeconomic groups. For nationally subsidised CGM, use was similar across socioeconomic groups with the exception of the most disadvantaged quintile, an important finding requiring further investigation into barriers to CGM use within a nationally subsidised model. User pays funding models for pump therapy result in lower use with socioeconomic disadvantage, highlighting inequities in this funding approach. For the full benefits of diabetes technology to be realised, equitable access to pump therapy needs to be a health policy priority.
Introduction
Advanced diabetes technologies including the use of pump therapy and continuous glucose monitoring (CGM) are associated with improved glycaemic outcomes in youth with type 1 diabetes (T1D) (1–5). Sustained long-term improvements in glycaemic control and reduction of long-term diabetes associated complications including microvascular complications and cardiovascular mortality, have been demonstrated for youth and adults with T1D on pump therapy in comparison to multiple daily injections (MDI) (6–10). Current consensus guidelines recommend that youth with T1D should be offered the most advanced diabetes technologies that are affordable and available to them, with choice of device based on specific needs to promote personalised diabetes care (11, 12). Accessibility of these devices varies globally; reimbursement models differ and barriers to access persist in many populations (13, 14). A recent review of 29 European countries revealed discrepancies in CGM and pump therapy; overall, CGM was at least partially subsidised in 17 of 29 countries, whereas pump therapy was readily available in 20 of 29 countries, with other countries reporting access and reimbursement issues (15).
Furthermore, lower socioeconomic status (SES) is associated with adverse glycaemic outcomes in youth with T1D (16–19), which may be compounded or partially driven by the association of SES and use of diabetes technologies (18, 20, 21). Given the association between use of diabetes technologies and improved glycaemic outcomes, disparity in access to technology may potentiate disadvantage in low socioeconomic groups.
The association between SES and technology use in youth with T1D has not been previously investigated in the Australian population. The public hospital network and the universal health insurance system provide free or low-cost health care to all Australian citizens (22). However, Australia has two separate models for funding of advanced diabetes technologies. In April 2017, the Australian Government committed to fully subsidising CGM for children and young adults (aged <21 years) living with T1D, dramatically increasing CGM uptake (23). Insulin pump therapy is not publicly subsidised, rather pumps are accessed primarily via private health insurance or self-funding, both of which carry significant financial burden for families. Across the Australian states and territories, there is limited access to compassionate programs for low-income families to access pumps (24) and strict criteria are in place, potentially excluding many from accessing reimbursement via these pathways who would find self-funding a pump financially burdensome or impossible. Furthermore, pump provision beyond young adulthood is not usually available. These disparities in pump access are now of critical importance with the availability of new generation hybrid closed loop (HCL) systems that require insulin pump therapy combined with CGM use, and which have been shown to improve outcomes for people living with T1D (25–27).
These two distinct models for pump therapy and CGM provide the platform to investigate the impact of differing funding models on technology use in Australian youth with T1D. The aim of this study was to evaluate the association between SES and use of diabetes technologies. We hypothesized that socioeconomic disadvantage would be associated with lower use of diabetes technologies.
Methods
Study design and population
This is a cross-sectional population-based study of children aged <18 years with T1D receiving care at paediatric diabetes centres in Australia.
Demographic and clinical information was extracted from the Australasian Diabetes Data Network (ADDN), a prospective, longitudinal database with contributing centres comprising major diabetes clinics across Australia and New Zealand (28). Initiated in 2012, the registry has expanded to include data from 23 paediatric centres, 13 of which are in Australia. The majority of Australian children, in both urban and regional settings, receive care in public paediatric services, of which a majority share data with ADDN. Those who have not consented to share data with ADDN, and those undergoing care in the private system are not represented in this cohort’s analysis.
Data from the 1st of July 2020 to the 1st July 2022 were included in the study. 5913 individuals were aged <18 years and contributing data to ADDN on 1st July 2022. Information recorded at the visit closest to this reference date was used to determine device use and postcode. Where information on device use was missing from this record, device use status at the previous visit was carried forward from a maximum of 2 years prior (median time difference between visit date and device use status = 0.29 years, interquartile range = 0.12 to 0.67 years). CGM and pump use were classified as binary measures (Yes/No) based on whether the device was being used at this visit. Those with missing postcode data (n=145), or who did not have a clinic visit (n=811) were excluded from the analysis, resulting in a dataset from 4957 individuals, which represents approximately 30-40% of youth living with T1D in Australia, with 14,919 individuals aged 0-20 years registered with the National Diabetes Services Scheme as of 30th June 2022 (29), noting difference in age range for this reference and those included in the study.
Consent for data sharing with ADDN is obtained from individuals from their diabetes centre, usually at time of diagnosis.
Area-based measures
Socio-Economic Indexes for Areas (SEIFA) is a tool developed by the Australian Bureau of Statistics, utilising Australian census data to capture aspects of relative socioeconomic advantage and disadvantage (30). Statistical areas can then be ranked regarding SES utilising one of four specific indices. The SEIFA Index of Relative Socio-Economic Disadvantage (IRSD) was implemented in this analysis to provide an area-based indication of disadvantage, as individual-level measures of SES are not collected through ADDN. The IRSD includes 16 variables incorporating income, highest level of education, employment type and status, spoken English ability, family structure, disability needs, housing factors, internet and personal vehicle access (30). Utilisation of socioeconomic deprivation indices has been validated in other studies when individual-level measures of SES have not been prospectively collected (18, 31–33). Most recent primary residential postcode was used to determine an individual’s IRSD quintile.
In addition, the Remoteness Areas Structure within the Australian Statistical Geography Standard was used to classify, based on residential postcode, an individual’s location within Australia as being urban (major city), inner and outer regional, remote or very remote (34).
Statistical analysis
Standard descriptive statistics were used to summarise demographic and clinical characteristics of the study population; medians and interquartile ranges for continuous measures, counts, proportions and percentages for categorical measures.
Pump and CGM use in each IRSD quintile were summarised as percentages (with 95% Wilson score confidence intervals) and chi-square tests conducted. Multivariable generalised linear models (Poisson family with log link and robust sandwich errors) were used to determine the association between SES and device use following adjustment for relevant confounders. These models included terms for IRSD quintile, remoteness classification, age, diabetes duration, sex, and individual’s location within Australia. The overall significance of IRSD quintile in predicting device use was assessed using a chi-square test of the difference in residual deviance when IRSD quintile was added to the model. Adjusted risk ratios with 95% confidence intervals, were calculated for pairwise comparisons of IRSD quintiles 2 to 5 to quintile 1.
Sensitivity models including and excluding Remoteness Area Structure were conducted to explore any model bias due to potential over-adjustment when determining the relationship between SES and device use.
Results
Data for 4957 Australian youth living with T1D with a mean (SD) age of 12.3 (3.7) years and mean (SD) duration of diabetes of 4.8 (3.7) years were analysed (Table 1). Mean (SD) HbA1c for all individuals was 8.1% (1.6%)/65 (17.5) mmol/mol, reflecting previous analyses of the ADDN cohort (35). The distribution of individuals varied across the quintiles, with the majority living in postcodes associated with IRSD quintiles 4 and 5 (49.8%), the areas associated with lower relative socioeconomic disadvantage (Table 1).
Pump use differed significantly by IRSD quintile (χ2 (4, 4957) = 80.17, p<0.001). Figure 1A provides the percentages [with 95% Wilson score confidence intervals (CI’s)] of individuals using pumps across IRSD quintiles. Increased pump use was associated with increasing IRSD quintile, with the lowest use in the most disadvantaged quintile (38.9%) and highest use in the least disadvantaged quintile (52%). The pattern of increasing pump use with higher IRSD quintile was still observed after adjusting for age, duration of diabetes, sex, remoteness and individual’s location within Australia (see Table 2 for adjusted risk ratios (RRadj) with CI’s). Compared to the most disadvantaged IRSD quintile 1, pump use was 16% more likely in quintile 2 (RRadj = 1.16 [95% CI: 1.04, 1.31]), 19% more likely in quintile 3 (RRadj = 1.19 [1.06, 1.33]), 35% more likely in quintile 4 (RRadj = 1.35 [1.21, 1.50], and 51% more likely in the least disadvantaged quintile 5 (RRadj = 1.51[1.36, 1.67]).
Figure 1 (A) Unadjusted percentage of pump use by IRSD quintile (with Wilson score CI’s). (B) Unadjusted percentage of CGM use by IRSD quintile (with Wilson score CI’s).
CGM use also differed significantly by IRSD quintile (χ2 (4, 4957) = 45.48, p<0.001). Figure 1B displays percentages (with 95% confidence intervals) of CGM use across IRSD quintiles. The lowest use was seen in quintile 1 at 56.4%, with higher but similar use across quintiles 2 to 5 (76.7% in quintile 2, 70.9% in quintile 3, 72.9% in quintile 4 and 69.2% in quintile 5). After adjusting for available sociodemographic and clinical characteristics, IRSD quintile 1 remained a predictor of less CGM use (see Table 2 for adjusted risk ratios). Compared to the most disadvantaged quintile 1, CGM use was 35% more likely in quintile 2 (RRadj = 1.35 [1.26, 1.44]), 28% more likely in quintile 3 (RRadj = 1.28 [1.19, 1.37]), 35% more likely in quintile 4 (RRadj = 1.35 [1.26, 1.45]), and 34% more likely in the least disadvantaged quintile 5 (RRadj = 1.34 [1.25, 1.44]).
Model results were similar with or without inclusion of Remoteness Area Structure (see Supplementary Material).
Discussion
This large, cross-sectional national study demonstrated an association between socioeconomic deprivation and the use of advanced diabetes technologies in youth with T1D in Australia. The differential funding models for advanced diabetes technologies in Australia provided the opportunity to explore the association between SES and technology use, which has not previously been investigated in the Australian context.
This study demonstrated that pump therapy use was higher in the least socioeconomically deprived quintiles. The pattern of pump use across quintiles is more likely to represent the ability of families living in higher quintiles to afford private health insurance or self-funding of pumps, potentially reflecting the inadequacy of the current funding model for pump therapy in Australia. The finding of increased pump use in higher quintiles may also represent other social determinants of health in higher quintiles, such as higher levels of parental education increasing understanding and acceptability of pump therapy, reduced financial barriers impacting access to health care or better English language skills, given that delivery of pump therapy education is primarily in English.
Conversely, CGM use was lowest in the most disadvantaged quintile despite fully subsidised access to this technology for all Australian youth. Similar use across quintiles 2 to 5 was observed. In 2017, the Australian government subsidised CGM use for Australian youth living with T1D. CGM uptake increased from less than 5% to 79% two years post-subsidy of CGM (23). The important but unexplained finding in our study of significantly lower CGM use in quintile 1 compared to other quintiles, in the context of a population with overall high CGM use given national subsidy, warrants further investigation. Delineating the specific barriers to accessing CGM technology in the most disadvantaged quintile has the potential to inform policy change and impact models of care in T1D. We hypothesise that factors including clinician bias in technology initiation, access to relevant mobile devices, technology acceptability and understanding which could be impacted by English language proficiency or parental level of education, could be driving this finding in the Australian population. Prospective quantitative analysis of socioeconomic factors influencing CGM use in this group compared to other quintiles, specifically investigating the impact of ethnicity, parental level of education, technology understanding, access and burden, and other potential factors, will be essential to explain the findings. Longitudinal studies rather than cross-sectional analysis will also aid in our understanding of this issue. Qualitative investigation of groups with lower technology uptake will help identify the barriers limiting the uptake of CGM in a fully subsidised funding model. This will inform Australian care providers in regard to addressing these factors as well as assist other countries with their technology funding models and implementation strategies.
IRSD quintiles 4 and 5 represent approximately half of the study cohort (combined 49.8%). Higher socioeconomic status has previously been reported to be an independent risk factor for T1D in Australia, potentially explaining this finding (36). As discussed in detail below, SEIFA statistical areas do not precisely align with Australian postcodes, and it is possible that IRSD quintile based on postcode rather than SEIFA statistical area skews a portion of the population into higher IRSD quintiles. Despite the relatively large sample size, results could also reflect a non-representative sample of the T1D paediatric population within ADDN given 4957 individuals represent approximately 30-40% of youth living with T1D in Australia as previously mentioned, and that individuals lacking postcode data or visit history were unable to be included in the analysis.
This is the first analysis of diabetes technology use in relation to SES in the Australian paediatric context. A key strength of the study design is that a large number of individuals with T1D were able to be included in the analysis. Given Australia's unique global position with differential diabetes technology funding models, the results of this study contribute evidence that further advocacy efforts for improved pump therapy access are required. The results have the potential to support advocacy and inform Australian healthcare policy in regard to technology access. This study highlights the importance of investigating if this association also exists in the Australian adult population, as funding models for diabetes technologies evolve in this cohort.
There are several limitations to this study. SEIFA IRSD quintiles represent the area-based deprivation in which an individual lives and provide an indication of socioeconomic deprivation only. Furthermore, SEIFA statistical areas do not precisely align with Australian postcode areas, which can have a wide variation of socioeconomic deprivation within them. IRSD based on an individual’s postcode should be interpreted with care. Collection of the individual-level factors influencing the SES of youth with T1D would be required to further delineate specific barriers in accessing technology. These factors include but are not limited to; parental occupation, income and level of education, ethnicity, private health insurance status, family structure and supports, however this type of data are not collected through ADDN.
The use of advanced diabetes technologies has been demonstrated to improve glycaemic outcomes in T1D (1, 2, 5), however there are barriers in accessing these technologies. Various studies have identified specific barriers including funding models (13, 37) and individual-level factors of socioeconomic deprivation including ethnicity, access to private health insurance, higher parental level of income and education (38–41). Clinician selection bias when selecting individuals to initiate diabetes technologies has also been demonstrated (42, 43) and acceptability of technology to individuals and their families, including in decision making regarding technology use, is also an important barrier to consider in the context of our findings. As glycaemic control is further impacted by socioeconomic status (19, 44, 45), non-inclusive funding models may potentiate disparities in glycaemic outcomes for youth with T1D. Considering the improvement in glycaemic control and reduction in diabetes related complications demonstrated with pump therapy and CGM, addressing barriers and improving funding models are critical goals in creating equitable access to diabetes technology in Australia.
This cross-sectional analysis of national data shows that despite universal subsidy, those in the most disadvantaged quintile utilised CGM less than those in other quintiles, where use was similar. This indicates that while subsidy is an essential first step, it is insufficient to prevent socioeconomic-based inequities in technology use. Conversely, for pump therapy, where a user pays model operates, an increase in pump use was associated with decreasing socioeconomic disadvantage. A health system that supports all youth living with T1D to access and use diabetes technologies is likely to result in improved glycaemic outcomes, with the consequent cost benefit of reduced complications, improved mental health and increased productivity. Future models of care should evolve to address barriers to accessing diabetes technology, particularly with the rapidly accumulating evidence from both research and real-world settings that advanced HCL systems improve glucose control for youth with T1D.
Data availability statement
The raw data supporting the conclusions of this article will be made available by the authors, without undue reservation.
Ethics statement
The studies were conducted in accordance with the local legislation and institutional requirements. All centres contributing data had Human Research or Health and Disability Ethics Committee approval for participation in ADDN. Patients provided written informed consent for data upload to ADDN. The current analysis was approved by Monash University Human Research Ethics Committee (MUHREC), Project ID 38039.
Author contributions
All authors contributed to the development of this project and editing of the manuscript as well as the Australasian Diabetes Data Network (ADDN) study group.
Group members of Australasian Diabetes Data Network (ADDN)
The authors drafted this manuscript on behalf of the ADDN Study Group members (18th June 2023; authors have been removed from the list): Professor Maria Craig (The Children’s Hospital at Westmead, Sydney), Dr Kym Anderson (University Hospital Geelong, Geelong), Associate Professor Sof Andrikopoulos (Australian Diabetes Society), Clinical Professor Geoff Ambler (The Children’s Hospital at Westmead, Sydney), Dr Helen Barrett (The Mater Private Hospital, Brisbane), Professor Jenny Batch (Queensland Children’s Hospital, Brisbane), Associate Professor Philip Bergman (Monash Children’s Hospital, Melbourne), Professor Fergus Cameron (Royal Children’s Hospital, Melbourne), Professor Peter Colman (The Royal Melbourne Hospital, Melbourne), Associate Professor Louise Conwell (Queensland Children’s Hospital, Brisbane), Associate Professor Andrew Cotterill (Queensland Children’s Hospital, Brisbane), Dr Chris Cooper (University Hospital Geelong, Geelong), Professor Jennifer Couper (Women’s and Children’s Hospital, Adelaide), Professor Kim Donaghue (The Children’s Hospital at Westmead, Sydney), Dr Jan Fairchild (Women’s and Children’s Hospital, Adelaide), Dr Gerry Fegan (Fiona Stanley Hospital, Perth), Dr Spiros Fourlanos (The Royal Melbourne Hospital, Melbourne), Associate Professor Sarah Glastras (Royal North Shore Hospital, Sydney), Dr Leonie Gray (Mater Medical Centre, Rockhampton), Associate Professor Shane Hamblin (Western Health, Melbourne), Professor Paul Hofman (University of Auckland, New Zealand), Associate Professor Dianne Jane Holmes-Walker (Westmead Hospital, Sydney), Dr Neville Howard (The Children’s Hospital at Westmead, Sydney), Dr Michelle Jack (Royal North Shore Hospital, Sydney), Dr Steven James (University of the Sunshine Coast, Caboolture), Dr Craig Jefferies (Starship Children’s Health, New Zealand), Dr Stephanie Johnson (Queensland Children’s Hospital, Brisbane), Dr Jeff Kao (Royal Children’s Hospital, Melbourne), Associate Professor Bruce R King (John Hunter Children’s Hospital, Newcastle), Dr Antony Lafferty (The Canberra Hospital, Canberra), Ms Michelle Martin (Illawarra Shoalhaven Diabetes Service, Wollongong), Dr Robert McCrossin (Gladstone Hospital, Gladstone), Dr Mark Pascoe (Royal Hobart Hospital, Hobart), Dr Ryan Paul (Waikato Hospital, New Zealand), Dr Alexia Peña (The University of Adelaide, Adelaide), Associate Professor Darrell Price (Pacific Private Clinic, Gold Coast), Associate Professor Christine Rodda (Sunshine Hospital, Melbourne), Professor David Simmons (Campbelltown Hospital, Sydney), Professor Richard Sinnott (eResearch, University of Melbourne), Dr Alan Sive (Townsville Hospital, Townsville), Dr Carmel Smart (John Hunter Children’s Hospital, Newcastle), Dr Monique Stone (Royal Darwin Hospital, Darwin), Associate Professor Steve Stranks (Australian Diabetes Society), Dr Elaine Tham (Women’s and Children’s Hospital, Adelaide), Dr Charles Verge (Sydney Children’s Hospital, Sydney), Professor Jerry Wales (Queensland Children’s Hospital, Brisbane), Associate Professor Glenn Ward (St. Vincent’s Hospital, Melbourne), Associate Professor Ben Wheeler (Dunedin School of Medicine, New Zealand), Dr Judy Williams (Bundaberg Diabetes Centre, Bundaberg), Dr Helen Woodhead (Australia and New Zealand Society for Paediatric Endocrinology and Diabetes), Dr Nick Woolfield (Caboolture Hospital, Caboolture), Dr Anthony Zimmermann (Lyell McEwin Hospital, Elizabeth Vale).
Acknowledgments
This research was conducted as part of the Australasian Diabetes Data Network. We are grateful to JDRF Australia, the Australian Research Council and to the children and young people with diabetes and their families who provided the data. This research was supported by JDRF Australia (5-SRA-2021-1088-M-X).
Conflict of interest
The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.
Publisher’s note
All claims expressed in this article are solely those of the authors and do not necessarily represent those of their affiliated organizations, or those of the publisher, the editors and the reviewers. Any product that may be evaluated in this article, or claim that may be made by its manufacturer, is not guaranteed or endorsed by the publisher.
Supplementary material
The Supplementary Material for this article can be found online at: https://www.frontiersin.org/articles/10.3389/fendo.2023.1178958/full#supplementary-material
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Keywords: type 1 diabetes (T1D), paediatrics, socioeconomics, equity, model of care, technology
Citation: Lomax KE, Taplin CE, Abraham MB, Smith GJ, Haynes A, Zomer E, Ellis KL, Clapin H, Zoungas S, Jenkins AJ, Harrington J, de Bock MI, Jones TW and Davis EA (2023) Socioeconomic status and diabetes technology use in youth with type 1 diabetes: a comparison of two funding models. Front. Endocrinol. 14:1178958. doi: 10.3389/fendo.2023.1178958
Received: 03 March 2023; Accepted: 31 July 2023;
Published: 21 August 2023.
Edited by:
Joseph Isidore Wolfsdorf, Boston Children’s Hospital and Harvard Medical School, United StatesReviewed by:
Pascal Barat, Université de Bordeaux, FranceIsmaeel Yunusa, University of South Carolina, United States
Copyright © 2023 Lomax, Taplin, Abraham, Smith, Haynes, Zomer, Ellis, Clapin, Zoungas, Jenkins, Harrington, de Bock, Jones and Davis. This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
*Correspondence: Kate E. Lomax, Kate.Lomax3@health.wa.gov.au