Figures
Abstract
The burden of inflammatory bowel disease (IBD) in Australia is increasing but national data about the current prevalence are limited. We aimed to estimate the prevalence of IBD (including Crohn’s disease, ulcerative colitis and unspecified IBD) as well as Crohn’s disease and ulcerative colitis separately in a general practice population in Australia. We also assessed risk factors associated with Crohn’s disease and ulcerative colitis. We conducted a cross-sectional study using data from MedicineInsight, a national database of general practice electronic health records, from 1 July 2017 to 30 June 2019. The prevalence of IBD was calculated and stratified by sociodemographic characteristics. Logistic regression analysis was conducted to assess risk factors associated with Crohn’s disease and ulcerative colitis. The study comprised 2,428,461 regular patients from 481 practices. The estimated crude prevalence of IBD was 653 per 100,000 patients; Crohn’s disease was 306 per 100,000 and ulcerative colitis was 334 per 100,000. Males were independently associated with a lower risk of Crohn’s disease (OR: 0.86; 95% CI: 0.81, 0.90) but a greater risk of ulcerative colitis (OR: 1.12; 95% CI: 1.06, 1.17) than females. Compared to non-smokers, patients who were current smokers were associated with a greater risk of Crohn’s disease (OR: 1.13; 95% CI: 1.04, 1.23) but a lower risk of ulcerative colitis (OR: 0.52; 95% CI: 0.47, 0.57). Other factors positively associated with both Crohn’s disease and ulcerative colitis were age (≥ 25 years), non-Indigenous status and socioeconomic advantage. Our findings provide a current estimate of the prevalence of IBD, Crohn’s disease and ulcerative colitis in a large national general practice population in Australia and an assessment of the factors associated with Crohn’s disease and ulcerative colitis. These data can assist in estimating the health burden and costs, and planning for health services.
Citation: Busingye D, Pollack A, Chidwick K (2021) Prevalence of inflammatory bowel disease in the Australian general practice population: A cross-sectional study. PLoS ONE 16(5): e0252458. https://doi.org/10.1371/journal.pone.0252458
Editor: Louise Emilsson, University of Oslo, NORWAY
Received: February 13, 2021; Accepted: May 14, 2021; Published: May 27, 2021
Copyright: © 2021 Busingye et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
Data Availability: The current study is based on data from MedicineInsight (https://www.nps.org.au/medicine-insight), a national general practice data source developed and managed by NPS MedicineWise. In accordance with the ethical approvals for this study, on-provision of these data is not permitted as it may compromise participants’ privacy. De-identified MedicineInsight data may be requested for research purposes and all requests are carefully considered by the independent MedicineInsight Data Governance Committee. All approvals are made on an individual project basis and all data must be stored in an approved secure environment. Data access enquiries can be directed to NPS MedicineWise via aDataGovernance@nps.org.au.
Funding: NPS MedicineWise receives funding from the Australian Government Department of Health for the MedicineInsight program and the study was also funded by the Australian Government Department of Health. The Australian Government Department of Health did not play a role in the study design, data collection and analysis, decision to publish, or preparation of the manuscript.
Competing interests: I have read the journal’s policy and the authors of this manuscript have the following competing interests: all the authors are employees of NPS MedicineWise, the data custodian of MedicineInsight. NPS MedicineWise receives funding from the Australian Government Department of Health for the MedicineInsight Program.
Introduction
Crohn’s disease (CD) and ulcerative colitis (UC), known collectively as inflammatory bowel disease (IBD), are life-long gastrointestinal disorders [1]. IBD is an important public health challenge globally and is associated with significant morbidity and reduced quality of life [2].
In recent decades, there has been a dramatic epidemiological change in the incidence of IBD in the Asia-Pacific region [3, 4]. Australia has not been spared from the increasing burden of IBD [5–7]. The few epidemiological studies from Australia show a significant incidence and prevalence of the disease [6, 7], but are limited by geographical coverage, sample size and the characteristics of the populations studied. Moreover, incidence or prevalence statistics extrapolated from limited locales and historical or international data, as done previously [5, 8], may not be reliable. To the best of our knowledge, there is no current Australian national prevalence estimate for IBD, which is important for planning health services and assessing economic costs.
The aim of this study was to estimate the prevalence of IBD (comprising CD, UC and unspecified IBD) as well as CD and UC separately in the Australian primary care setting using MedicineInsight, a large-scale national general practice database. We also assessed the sociodemographic and behavioral factors associated with CD and UC.
Material and methods
Study design and period
A cross-sectional study was conducted using MedicineInsight data from 1 July 2017 to 30 June 2019. Historical records outside this study period were included when identifying IBD.
Data source
MedicineInsight is a large-scale, national general practice data program developed and managed by NPS MedicineWise with funding from the Australian Government Department of Health. The MedicineInsight programme has been described elsewhere [9]. Briefly, MedicineInsight extracts and collates longitudinal, de-identified patient health records from clinical information systems (CIS; ‘Best Practice’ or ‘MedicalDirector’) of general practices that have consented to participate in the program [10]. The data collected include patient demographics, encounters (but not progress notes), diagnoses, prescriptions and pathology tests. Progress notes, data recorded by providers about patient care in the unstructured area of the medical record, are not collected because they may contain identifiable information. The sociodemographic characteristics of regularly attending MedicineInsight patients are broadly comparable to patients who visited a GP in 2016–17 in the Medicare Benefits Schedule (MBS, a listing of services in Australia’s universal health insurance scheme) data [9].
Study population
We included regular patients who had valid information for age and sex. We defined ‘regular’ patients as those who met the Royal Australian College of General Practitioners’ (RACGP’s) definition of an ‘active’ patient (at least three consultations with a GP at the same general practice within a two-year period). MedicineInsight data from 481 practices that met the standard data quality criteria (described elsewhere) [9] were included.
Ascertainment of patients with IBD
A diagnosis of IBD was identified from one or more of three CIS diagnosis fields including diagnosis and medical history, the reason for encounter and the reason for prescription, using relevant free-text terms or CIS-specific codes (‘Docle’ or ‘Pyefinch’ from Best Practice or MedicalDirector).
Patients were defined as having IBD if relevant terms and synonyms of CD, UC or IBD (not specified by clinician, hereafter IBD-unspecified) were recorded in one of the three diagnosis fields, at any time in their medical records up to the end of the study (S1 Table). We further identified patients with either CD or UC only as those with relevant terms and synonyms of CD or UC recorded in one of the three diagnosis fields, at any time in their medical records up to the end of the study. For patients who had both UC and CD or IBD-unspecified recorded in their medical records, the most recent recorded diagnosis was considered as the final diagnosis [11]. Patients with a record of IBD-unspecified were only included in the overall IBD population but not the CD or UC sub-populations because it was not clear whether they had CD or UC.
Outcome
Prevalence was defined as the proportion of the study population who had a diagnosis of IBD, CD and UC recorded up to 30 June 2019.
Covariates
Sociodemographic characteristics comprised age (at 1 July 2019, based on year of birth), sex, Aboriginal and Torres Strait Islander status, state/territory, remoteness, Socio-Economic Indexes for Areas (SEIFA) and most recently recorded smoking status up to 30 June 2019. Information on patients’ Aboriginal or Torres Strait Islander status is recorded within the CIS and extracted into MedicineInsight using the Australian Bureau of Statistics (ABS) standard classification [12]. State/territory, remoteness and SEIFA are based on the patients’ most recently recorded residential postcodes. Remoteness was determined by the ABS geographical framework ‘Remoteness Areas’ [13], and SEIFA quintiles (1 to 5, least to most advantaged) by the ABS Index of Relative Socio-Economic Advantage and Disadvantage [14].
Data analysis
Descriptive statistics were used to present the study outcomes, including use of percentages and associated 95% confidence intervals (CI), and means and standard deviations (SDs). Robust standard errors were used in the calculation of 95% CIs to adjust for clustering by practice. The crude prevalence of IBD was calculated and stratified by sociodemographic characteristics. Logistic regression analysis was conducted to determine risk factors associated with CD and UC. All relevant variables such as age, sex, Indigenous status, state/territory, remoteness, socioeconomic and smoking status were introduced into multivariable regression analysis in a backward stepwise elimination method and variables with a p ≤ 0.1 were retained in the final models.
A difference between groups was considered statistically significant if p < 0.05, or there was non-overlap of 95% CIs [15], where appropriate. Data management and analyses were conducted with SAS Enterprise Guide 7.1 (Cary, NC USA, 2015) and Stata 16 (College campus, TX, USA).
Ethics
Approval to conduct this study was received on June 17, 2020 from the MedicineInsight independent external Data Governance Committee (reference number: 2020–017). The Royal Australian College of General Practitioners (RACGP) National Research and Evaluation Ethics Committee (NREEC) granted ethics approval for the standard operation and use of the MedicineInsight database by NPS MedicineWise (NREEC 17–017).
Results
Characteristics of the study population
There were 2,428,461 patients eligible for inclusion, representing approximately 9.7% of the Australian population [16], with a mean (SD) age of 42 (24) years and 56.1% were female (S2 Table). The demographic profiles of the study population and the national MBS data for patients in Australia who visited a GP during 2018–19 [17] are largely similar in terms of age, gender and socioeconomic status, but females are slightly overrepresented compared with the MBS patient population (52.3%) (S2 Table).
Characteristics of patients with IBD, Crohn’s disease and ulcerative colitis
Table 1 shows the sociodemographic characteristics of patients with IBD, CD and UC. The mean age (SD) of all patients with IBD was 52 (18) years and patients with UC were on average older than those with CD (55 vs 50 years). For CD, 45.9% of patients were ex-smokers, and for UC, 51.7% (Table 1).
Prevalence of IBD, Crohn’s disease and ulcerative colitis
Among the study population, 15,859 patients (653 per 100,000) were identified as having IBD (including CD, UC and IBD-unspecified). The overall crude prevalence per 100,000 of CD, UC and IBD-unspecified was 306 (n = 7,442), 334 (n = 8,121) and 12 (n = 296), respectively (Table 2). Prevalence of IBD, CD and UC was significantly greater in patients aged ≥ 20 than those aged < 20 years and in non-Indigenous than Aboriginal and/or Torres Strait Islander patients. Prevalence of CD was significantly greater for females (331) than males (275) but prevalence of UC was similar for both sexes (Table 2). Compared with the overall IBD prevalence for the study population (653), the IBD prevalence was significantly greater for patients resident in South Australia (908) and Tasmania (831), and lower in the Northern Territory (330). Similar findings were observed for CD and UC.
There were significant differences in the prevalence of IBD between males and females among patients aged 10–29 and 50–59 years (Fig 1 and S3 Table). For patients aged 10–29 years, the prevalence of CD was greater in males than females but was greater in females than males for patients aged 40–79 years (Fig 1 and S3 Table). In contrast to CD, there was no significant difference between males and females in the prevalence of UC for most age groups, except for the 70–79 years where the prevalence was greater among males than females (Fig 1 and S3 Table).
Non-overlap of 95% CIs indicates significant differences between males and females for each age group. IBD: Inflammatory bowel disease; CD: Crohn’s disease; UC: Ulcerative colitis.
Factors associated with Crohn’s disease and ulcerative colitis
Table 3 shows factors associated with CD and UC after adjustment using multivariable logistic regression. Patients who were aged ≥ 25 years, ex-smokers, and the socioeconomically advantaged had a greater risk of having CD or UC compared to those aged ≤ 24 years, non-smokers and the socioeconomically disadvantaged, respectively. Aboriginal and/or Torres Strait Islander patients had a lower risk of both CD (OR: 0.62; 95% CI: 0.52, 0.76) and UC (OR: 0.74; 95% CI: 0.62, 0.90). Compared to females, being male was associated with a lower risk of CD (OR: 0.86; 95% CI: 0.81, 0.90) but a greater risk of UC (OR: 1.12; 95% CI: 1.06, 1.17). Interestingly, compared to non-smokers, patients who were current smokers were associated with a greater risk of CD (OR: 1.13; 95% CI: 1.04, 1.23) but a lower risk of UC (OR: 0.52; 95% CI: 0.47, 0.57). Ex-smokers had a greater risk of both CD and UC than non-smokers. Variations in the risk of CD and UC were observed by state/territory.
Discussion
We have demonstrated the prevalence of IBD overall (including CD, UC and IBD- unspecified), and of CD and UC separately, in a large national Australian general practice population. The unadjusted prevalence of IBD, CD and UC at the end of the 2-year study period was estimated to be 653 per 100,000, 306 and 334, respectively. Our findings suggest higher rates than previously reported in regional population-based studies from Australia [6, 7]. Investigators of a 2010–11 study from Victoria showed the crude prevalence of IBD to be 344.6 per 100,000 (197.3 for CD and 136.0 per 100,000 for UC) [7]. In a 2013–14 population-based study from Tasmania, the crude prevalence per 100,000 of IBD, CD and UC was 335.0, 170.3, and 156.5, respectively [6]. Estimates observed in our study are similar to those reported in some European countries [11, 18]. A recent study conducted in primary care patients in the UK showed that the prevalence of IBD, CD and UC in 2018 was 725, 276 and 397 per 100,000, respectively [11]. A German study, utilizing administrative data, found that the prevalence of IBD in 2010 was 744 per 100,000 with 322 for CD and 412 for UC [18].
The higher prevalence in our study may reflect the increasing incidence of IBD [6, 7]; improved life expectancies of patients with IBD; variations in the source population (e.g., general practice patient population versus general population); and differences in data collection. As IBD is a chronic relapsing condition, and some clinicians might not routinely record a diagnosis of an existing chronic condition at every clinical encounter, we assessed lifetime prevalence where patients who ever had a record of IBD, CD and UC in their clinical record were included. Lifetime prevalence estimates might be higher than cross-sectional point (current) prevalence estimates if patients who are in long term remission are included.
While some Australian reports have shown higher rates of CD than UC [6, 7], our study shows slightly higher rates of UC than CD. This finding aligns with data presented in a 2006 report commissioned by the Australian Crohn’s and Colitis Association [8], and is consistent with some reports from Europe [18, 19] and USA [20].
Our findings also indicate variations in prevalence regarding sex, age group, Indigenous status, smoking status, socioeconomic status and state/territory. Consistent with other Australian studies [6], we found that the prevalence of CD is greater among females than males but the prevalence of UC is similar for both sexes. While data about sex-based differences in IBD are conflicting [21], our findings show that being male is independently associated with a lower risk of CD but a greater risk of UC.
The finding that Aboriginal and/or Torres Strait Islanders have a lower risk for developing IBD is consistent with other reports that have demonstrated lower risk of IBD in Indigenous populations [22–24]. Data from the Australian Paediatric and Adolescent IBD Database indicate lower rates of IBD in children of Aboriginal and Torres Strait Islander descent compared to non-Indigenous children [24]. Evidence from New Zealand demonstrates a lower risk of IBD among the Maori and Pacific Island people compared to Caucasians [22, 23]. The differences in prevalence and risk of IBD between ethnic groups may be attributable to genetic susceptibilities and environmental factors [25, 26].
This analysis further confirms the well-established paradoxical association between current smoking with CD and UC. As has been documented previously [23, 27, 28], our results indicate that current smoking is independently associated with a greater risk of CD but a lower risk of UC. Investigators of another Australian study found that smoking was positively associated with CD and negatively associated with UC among Caucasian Australians [28]. The reasons for the opposing effects of smoking on CD and UC are not clear, but several mechanisms through which smoking is said to influence the aetiology of IBD have been suggested, including epigenetic alterations, disruption in intestinal microbiota, integrity of the intestinal epithelium and the immune system [27].
The finding that socioeconomic advantage is associated with an increased risk of IBD is consistent with observations from other investigators [23]. This finding is not surprising as IBD has traditionally been regarded as a disease of high-income countries because of a higher prevalence observed in these countries compared to developing countries. Data from the global burden of disease study show that locations with high sociodemographic index (SDI) have the highest age-standardized prevalence of IBD, while those with low SDI have the lowest prevalence [4].
Regional variations in the risk of CD and UC may reflect differences in population characteristics (e.g., genetic and demographic factors, and environmental exposures) and area characteristics (e.g., remoteness and socioeconomic factors), across states/territories. Nevertheless, the high prevalence of IBD in Tasmania and South Australia compared with some other states/territories may require further investigation.
The strengths of this analysis include the size and national coverage of the MedicineInsight data. To the best of our knowledge, this is the first large national epidemiological study to present prevalence estimates for IBD in Australia. Because MedicineInsight is an open cohort and patients in Australia can visit multiple general practices, we used a cohort of regularly attending patients, likely to be receiving most of their care at a MedicineInsight practice, to help improve data quality. The use of MedicineInsight records containing GP-identified diagnoses is likely to be more accurate than self-reported health surveys.
This study is subject to a number of limitations, in addition to those inherent in routinely collected data, described elsewhere [9]. First, for privacy reasons, MedicineInsight does not include data from progress notes, which may contain further clinical information. Second, because data used are from general practice patients, this limits generalizability of the results to the general population. However, this MedicineInsight cohort of regularly attending patients is largely representative of the national MBS patient population, although minor demographic differences may have impacted our estimates, with female patients slightly overrepresented compared with MBS data. As the prevalence of CD is greater among females this could lead to a slight overestimate of the true CD (and IBD) patient prevalence. Third, as IBD is a chronic relapsing condition, we defined patients as those who have ever had a record of IBD in their clinical record. This may overestimate the current prevalence of IBD where patients are in long term remission. Fourth, because this was an observational study, this precludes us from drawing firm conclusions about temporal and causal relationships. Finally, although the prevalence estimates of several conditions derived from MedicineInsight are comparable with other studies and national estimates [17, 29], MedicineInsight data may be further refined by ongoing validation studies.
Conclusions
Our findings provide a current estimate of the prevalence of IBD, CD and UC in a large national general practice population in Australia and an assessment of the factors associated with CD and UC. These data can assist in estimating the health burden and costs, and planning for health services as well as strategies to reduce the burden of IBD.
Supporting information
S1 Table. Relevant search terms and synonyms for Crohn’s disease, ulcerative colitis and unspecified IBD.
https://doi.org/10.1371/journal.pone.0252458.s001
(DOCX)
S2 Table. Sociodemographic characteristics of patients in the main study cohort (2017–2019) compared to MBS national data (2018–2019).
https://doi.org/10.1371/journal.pone.0252458.s002
(DOCX)
S3 Table. Age-sex specific prevalence (per 100,000) of IBD, Crohn’s disease and ulcerative colitis.
https://doi.org/10.1371/journal.pone.0252458.s003
(DOCX)
Acknowledgments
We are grateful to the general practices, general practitioners and patients who allow the use of de-identified information for MedicineInsight. We thank NPS MedicineWise staff and John Stubbs, the consumer representative, who have provided valuable input.
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