Prevalence and Associated Factors of Diabetic Retinopathy among Type 2 Diabetes Mellitus Patients in Brunei Darussalam: A Cross-sectional Study

Article information

Korean J Ophthalmol. 2022;36(1):26-35
Publication date (electronic) : 2021 November 8
doi : https://doi.org/10.3341/kjo.2021.0040
1Department of Ophthalmology, Pengiran Muda Mahkota Pengiran Muda Haji Al-Muhtadee Billah, Tutong Hospital, Tutong, Brunei Darussalam
2Department of Medicine, RIPAS and PAPRSB IHS Pengiran Muda Mahkota Pengiran Muda Haji Al-Muhtadee Billah, Tutong Hospital, Tutong, Brunei Darussalam
3Department of Ophthalmology, RIPAS Hospital, Bandar Seri Begawan, Brunei Darussalam
4Department of Community Medicine, Calicut Medical College, Kerala, India
5Pengiran Anak Puteri Rashidah Sa’adatul Bolkiah Institute of Health Sciences, Universiti Brunei Darussalam, Gadong, Brunei Darussalam
Corresponding author: Sajid Adhi Raja, MS, FRCSEd. Department of Ophthalmology, Pengiran Muda Mahkota Pengiran Muda Haji Al-Muhtadee Billah Hospital, Tutong TA1341, Brunei Darussalam. Tel: 673-426-0729, E-mail: sajid.adhiraja@moh.gov.bn
Received 2021 March 19; Revised 2021 October 25; Accepted 2021 October 28.

Abstract

Purpose

To determine the prevalence of diabetic retinopathy (DR) and the factors associated with retinopathy among type 2 diabetes mellitus (DM) patients in Brunei Darussalam.

Methods

Cross-sectional study of all type 2 DM patients who attended diabetic eye screening over a 3-month period at one of four government hospitals. We assessed association between DR with the following variables: age, sex, glycated hemoglobin (HbA1c), duration of DM, hypertension, hyperlipidemia, and microalbuminuria.

Results

There were 341 patients (female, 58.9%; mean age, 55.3 ± 11.9 years) with a mean duration of DM of 9.4 ± 7.4 years and mean serum HbA1c of 8.4% ± 1.9%. The overall prevalence of any DR was 22.6% (95% confidence interval, 18.8–27.1) with prevalence rates of 4.1% (95% confidence interval, 2.1–6.4) for proliferative DR and 9.7% (95% confidence interval, 6.8–13.2) for vision-threatening DR. Multivariate analysis showed that DR was significantly associated with certain age groups (reduced in older age groups), longer duration of DM (11 years or more), poor control (HbA1c >9.0%) and presence of any microalbuminuria.

Conclusions

DR affects one in five patients with DM in Brunei Darussalam, comparable to rates reported for other Asian populations. It is especially worrying that one in ten patients with DM had vision-threatening DR. DR was significantly associated with longer duration of DM, poor control and presence of microalbuminuria but reduced in older age groups. It is important to advocate good control right from the time of diagnosis of DM and institute timely and effective management of retinopathy. DR was significantly associated with longer duration of DM, poor control of diabetes, and presence of microalbuminuria but reduced in older age groups.

Diabetic retinopathy (DR) is a leading cause of blindness among adults worldwide [1]. It progresses in stages from mild to moderate, severe non-proliferative DR (NPDR) and proliferative DR (PDR) [2]. Vitreous hemorrhage in PDR is a cause of severe or sudden loss of vision. Macular oedema can occur in any stages of retinopathy and cause moderate loss of vision. Vision-threatening DR (VTDR) is defined as severe NPDR, PDR, or the presence of diabetic macular oedema [3].

With the increasing prevalence of non-communicable diseases, the number of people with diabetes mellitus (DM) and related complications is expected to increase. A decade ago, the overall global prevalence of DR was reported as 34.6% [4]. A more recent review of articles published between 2015 and 2018 reported a global prevalence of 27% and highlighted considerable heterogeneity in prevalence. The lowest prevalence was reported in Europe (20.6%) and Southeast Asia (12.5%) and highest in Africa (33.8%), Middle East and North Africa (33.8%), North America (34%), and the Western Pacific region (36.2%) [5]. This heterogeneity may be due to varying prevalence of DM and other non-communicable diseases such as obesity, as well as differences in awareness, level of knowledge and available medical facilities in different parts of the world.

The International Diabetic Federation estimates the worldwide prevalence of DM is 9.1% with type 2 DM being the most common form [6]. Brunei Darussalam has an estimated prevalence of 13.3% [6]. The National Diabetic Management Programme of Brunei Darussalam mandates annual retinopathy screening for all patients with DM. To date, there have only been three studies published that had reported on prevalence of DR in Brunei Darussalam [79]. A study in 1998 at the Pengiran Muda Mahkota Pengiran Muda Haji Al-Muhtadee Billah Hospital, Tutong looked at DM control and reported a prevalence of DR of 18.0% (background DR, 17.1%; vitreous hemorrhage, 0.6%; and blindness, 0.3%) [7]. Another study between 1997 and 2000 from the tertiary center in Brunei Darussalam reported prevalence of DR of 19% (background DR, 15%; DR with maculopathy, 4%) [8]. The latest study done in 2014 to assess a new screening tool for DR in Brunei Darussalam reported a prevalence of DR at 18.5% including combined prevalence of severe DR and PDR of 3.7% [9]. Since the purpose of that study was to assess a new screening tool, the results obtained may not be a true representation of the epidemiological situation. None of these three studies assessed associations with other factors. The purpose of our study is to assess the current prevalence of DR and associated factors in Brunei Darussalam and to compare with reported rates of other populations.

Materials and Methods

Setting and study design

Brunei Darussalam has a small population of 450,000 people living across its four districts and served by four government hospitals. There is also support from 15 health centers, ten clinics and 22 maternal and child healthcare facilities. All patients with DM are routinely screened for DR at government health facilities. There is currently no private ophthalmic facility that offers DR screening and follow-up. This study was conducted at one of the four district hospitals, serving a population of 52,700 (2019 estimation; Department of Economic Planning and Statistics, Brunei Darussalam). The demographic breakdown resembles the national breakdown [10]. It is the only facility in the district equipped with NW8F (Topcon Health Care, Tokyo, Japan) for fundus digital imaging and fluorescein angiography, and Nidek MC-500 Pascal laser (Nidek, Aichi, Japan) for retina screening and treatment. The Brunei Darussalam Health Information and Management System (Bru-HIMS) electronically links all government health facilities across the country. Patients requiring vitrectomy or intravitreal anti-vascular endothelial growth factor treatment are referred to a tertiary center where these treatments are available.

This is a non-interventional cross-sectional study which retrospectively looked at the prevalence of DR and factors associated with DR. The data was collected as a part of a planned improvement of ophthalmic services audit in the district. During this period, services were provided as per normal departmental protocol and there were no new treatments or interventions provided. Institutional review board approval was not required. Data collected were anonymized. A statistician unfamiliar with the study population then analyzed and curated the data. This study was conducted with adherence to the general principles of the Helsinki declaration 2008. All patients gave verbal consent for their data to be analyzed for the study.

Patients and study participants

Based on the population size and estimated prevalence of DM in Brunei Darussalam, the estimated burden of DM in the district is approximately 4,400 patients. All patients diagnosed with DM within the district are referred to the district hospital for assessment of visual acuity, non-contact intraocular pressure and retinal examination by non-mydriatic camera or by slit-lamp bio-microscopy if photographic images are not of gradable quality. Findings are recorded in the Bru-HIMS electronic database and further review appointments given based on the retinal findings; annually for patients with no retinopathy and 3 to 12 months for patients with DR, depending on severity. Fluorescein angiography is being done less frequently unless the patient has concurrent retinal vessel occlusions, suspected ischemic macular disease, or optic nerve head disease. Laser treatment for DR is offered in the eye clinic and patients requiring anti-vascular endothelial growth factor or vitrectomy are referred to the national referral center for treatment, whilst still maintaining an appointment for routine follow-up in the district hospital.

Sample size calculation was conducted prior to the study based on prevalence of DR in the Western Pacific region (36.2%) and the estimated DM population (4,400) in the district. A sample of 329 patients was required to provide a 95% confidence interval (CI) and 5% margin of error. Patients with DM who attended the diabetic eye clinic for DR screening and monitoring over a 3-month period (October 7, 2019 to January 7, 2020) were recruited consecutively until sample size was achieved. In total, data of all patients (n = 341) who attended screening or follow-up during the 3-month study was collected. The extracted data included age, sex, duration of DM, glycated hemoglobin (HbA1c) levels, presence of hypertension, hyperlipidemia, and microalbuminuria.

DR screening outcome

DR screening was done using the Topcon NW8F non-mydriatic camera. Retinal images for each patient are captured and stored in the patient database linked to the Bru-HIMS electronic record system. For patients with non-gradable quality digital images, a dilated fundus examination was conducted using a slit-lamp biomicroscope. DR was classified into five groups based on a simplified version of the Early Treatment of Diabetic Retinopathy Study classification. The five groups are no DR; mild NPDR, if there are only microaneurysms less than 20 in four quadrants; severe NPDR, if there are four quadrant intraretinal bleeding, venous beading in at least two quadrants, or intraretinal microvascular abnormality in at least one quadrant; moderate NPDR, which has features more than mild but less than severe NPDR; and lastly, presence of new vessels at the disc or elsewhere on the retina with or without vitreous hemorrhage classify as PDR.

Statistics

Descriptive and statistical analyses were carried out using IBM SPSS ver. 22.0 (IBM Corp., Armonk, NY, USA). Data of all patients (n = 341) were used for the descriptive analyses and data are presented as mean and standard deviations for continuous variables and absolute number and percentages for categorical variables including 95% CI. Ten patients with anemia were excluded as serum HbA1c is affected by this condition and hence may not reflect true DM control, leaving 331 patients for analyses. Age groups were categorized into under 40, 41 to 50, 51 to 60, 61 to 70, and over 70 years, with duration of DM in years into under 5, 6 to 10, 11 to 15, 15 to 20, and over 20 years. DM control was categorized based on HbA1c level into good control (≤7.5%), suboptimal (7.6% to 8.9%) and poor control (≥9.0%). Univariate analyses were conducted using the chi-square test and any variables found to be significant (p < 0.05) were entered into multivariate analysis.

Results

The largest age group was in the 51 to 60 years old range, with more females than males (58.9%) and the population was predominantly Malay (consistent with the district and national population breakdown). Most patients had DM of less than 10 years (61.9%), and the mean duration of DM was 9.4 ± 7.4 years. Thirty patients (8.8%) had DM of less than one year. The mean serum HbA1c level was 8.5% ± 1.9% with 150 patients (44.0%; 95% CI, 38.9%–49.4%) categorized as having good control (HbA1c ≤7.5%). Hypertension (86.8%) and dyslipidemia (84.5%) were common and 22.6% had microalbuminuria or worst. Patients’ demographics and profiles are shown in Table 1.

The patients’ demographic and profiles (n = 341)

The prevalence of DR was 22.6% (95% CI, 18.8–27.1). Among patients with DR, 14 patients (18.2%; 95% CI, 9.8–28.4) had PDR with overall prevalence of PDR being 4.1% (95% CI, 2.1%–6.5%). Macular oedema occurred in 17 patients (5.0%; 95% CI, 2.9–7.7) and VTDR occurred in 9.7% (95% CI, 6.8%–13.3%) of all patients. The breakdown is shown in Table 2.

The breakdown of retina screening outcome (n = 341)

In univariate analysis, age groups (p = 0.030 for trend), longer duration of DM (p = 0.002 for trend), DM control (p < 0.0001 for trend) and presence of any microalbuminuria (p < 0.05) were significantly associated with DR (Table 3). Sex, hypertension, and dyslipidemia did not show significant associations (all p > 0.05). When these variables were entered into multivariate analysis, duration of DM, poor control of DM, and presence of microalbuminuria remained significantly associated with presence of any DR (Table 4). Duration of DM for 11 years or more, having poor DM control, and microalbuminuria were associated with any DR. Compared to the youngest age group (<40 years), the 61 to 70 and over 70 age groups had 80% to 90% lower risk for DR (p = 0.006).

Univariate analyses between variables and presence or absence of any DR (n = 331)

Multivariate analyses of association with any diabetic retinopathy (n = 331)

Discussion

Our study showed that DR is common among patients with type 2 DM in Brunei Darussalam with one in five affected and that certain variables were associated with the presence of DR. The prevalence of DR at 22.6% in our study is within the range reported across continents in the literature as shown in Table 5 [79,1125]. Globally, reported rates range from those in Spain (12.3%) [15], India (15.4%) [18], and Korea (15.8%) [24] to high rates reported in Indonesia (43.1%) [23], Malaysia (39.3%) [20], and Saudi Arabia (36.4%) [17]. Studies from China, UK, and US all reported rates of above 30% [11,14,19]. Overall, there seems to be no definite correlations with the relative development of the countries. These variations can be accounted by several factors especially the patient population studied in these publications. Generally, studies tend to be done in academic or large centers and this can result in over representations of more severe cases. Milder or controlled cases are usually followed up in peripheral clinics and such patients may not be included in the population samples. Availability of healthcare and its’ infrastructure are also important. With greater accessibility, the proportion of patients diagnosed with DM early is higher and the proportion of undiagnosed cases is expected to be lower. On the other hand, in less developed countries where prevalence of obesity is low or just beginning to increase, the prevalence of DM may similarly be low or just increasing. Therefore, the true prevalence of complications related to diabetes such as DR is likely to be lower in less developed countries when compared to developed countries. Despite this, reported figures represent major universal public health concern with one in eight to almost one in two having DR [1126]. This is particularly important given that DR is the main cause of visual impairment and blindness in adults and that the prevalence of DM is increasing [1].

Comparison of prevalence of diabetic retinopathy among diabetes patients in Brunei Darussalam with some recently published data from countries around the world

Similarly, there is also heterogeneity in the reported prevalence of VTDR globally (Table 5) [79,1125]. Interestingly, the prevalence of VTDR is generally low in developed nations and high in developing countries. This may be related to better control of DM and timely treatment of DR in the more developed world. On the other hand, changing food habits, increasing prevalence of non-communicable diseases such as obesity, hypertension, and dyslipidemia, and non-availability of timely and appropriate treatment of retinopathy may be reasons for increased rates of VTDR in developing countries. Further research is required to ascertain the reasons.

The current rate of 22.9% for any DR in Brunei Darussalam is slightly higher than the rates (18.0%–19.0%) reported in the previous local studies from nearly two decades ago [79]. The combined rate of severe DR and PDR (6.3%) in the current study is also higher than the last study of 3.7% carried out more than 5 years ago [9]. The study by Da and Nyunt [7] which was conducted in the same institution as the current study provided a unique opportunity for comparison. The proportion of patients with good control of DM (HbA1c <8.0%) has declined from 48.6% in the year 2003 to 60.1% at present. In contrast, the proportion of patients with hypertension has increased from 61.7% to 86.8% and likewise dyslipidemia has increased, reflecting changes to the patient demographic over time [7]. Retinopathy has increased from 18.0% to 22.9%. These differences may be a true reflection of increasing prevalence of DR in Brunei Darussalam. Perhaps the prevalence of non-communicable diseases including DM has been increasing with greater awareness and understanding, contributing to the increasing number of patients being diagnosed with DM.

Our study showed several factors to be significantly associated with DR. Among the known risk factors for development of DR, duration of DM is the most important non-modifiable factor. According to large epidemiological studies, the risk of developing DR increased several folds after a latent period of 8 to 10 years’ duration of DM [4,25]. We showed that patients who had DM of more than 10 years were significantly associated with DR: 11 to 15 years (odds ratio [OR], 3.88), 16 to 20 years (OR, 3.39) and over 20 years (OR, 5.43). Among the patients in this study, 61.9% have DM of less than 10 years duration. This indicates a likely increase in the prevalence of DR in the population in the coming years.

In the management of DM, good control of diabetes is very important to reduce the risk of future complications. However, even with good control, complications do occur due to the chronic nature of the disease. Our study showed a linear correlation between DR and levels of control: good control (14.3%), suboptimal control (20.3%) and poor control (35.9%). Poor control was significantly associated with development of DR (OR, 2.01). The American Diabetes Association recommends 7% as target of HbA1c level for good control [26]. The Diabetes Control and Complications Trial and the United Kingdom Prospective Diabetes Study showed that increasing levels of HbA1c correlated well with occurrence and progression of DR [27,28]. However, later studies demonstrated that strict control of DM does not give clear benefits in controlling macro-vascular diseases, unlike in microvascular diseases [2931]. The Action to Control Cardiovascular Risk in Diabetes study showed that intensive control of DM increased the risk of mortality especially in type 2 DM [32]. In our setting, we use HbA1c ≤7.5% as a target value for good control. Later analysis of the above mentioned and similar studies suggest that HbA1c targets should be individualized based on the duration of the DM and existing comorbidities [33]. Generally, younger individuals with DM who are otherwise healthy should aim for a lower target value whereas older individuals with cardiovascular comorbidities should have a higher target level of HbA1c.

Albuminuria in DM is a wide spectrum ranging from micro to macroalbuminuria, which usually correlates with duration and severity of the disease. It is an important predictor of DM nephropathy. Not unexpectedly, our study showed a positive association between microalbuminuria and DR (OR, 2.00). Therefore, it is important that interval screening for microalbuminuria be carried out.

Interestingly, we found that among the age groups, the older patients had a lower risk for DR, (61–70 years group with OR 0.22, p = 0.006 and >70 years group with OR 0.09, p = 0.007) when compared to the over 40 years group. This probably indicates for uncertain reason that the younger age groups were at higher risk for DR. At first sight, this may seem contradictory to our finding that a longer duration of DM was significantly associated with DR. We found that the older groups (61–70 and >70), despite having a longer duration of DM, had better mean HbA1c levels and good DM control when compared to the younger age groups. Furthermore, factors that were not considered in our study may contribute, such as genetic predisposition and lifestyle. The phenomenon of young DM patients having more complications is probably a reflection of the changing demographic in DM, with more young people developing DM, corresponding with the increasing prevalence of obesity and metabolic syndromes.

Among the factors assessed, hypertension and hyperlipidemia were not associated with DR. Hypertension can cause retinopathy and nephropathy and is often correlated with severe and chronic hypertension. In DM, the management of hypertension is more aggressive with lower target levels making contribution of hypertension less important than DM itself [34,35]. There have been several studies examining the effect of hypertension and hyperlipidemia in relation to diabetic complications. A meta-analytic review published in Cochrane patients concluded that there is only weak evidence for beneficial effects of reduction in blood pressure with respect to preventing DR [36]. The Action to Control Cardiovascular Risk in Diabetes Eye Study showed that intensive glycemic control together with control of dyslipidemia using fenofibrate and simvastatin reduced the proportion of eyes that had progression of DR by one-third [37]. However, the beneficial effect may be due to the intensive management of DM rather than lipid control. Similar to the management of hypertension, the recommendation for initiating treatment for dyslipidemia in patients with DM is also more aggressive. All our patients with diagnosis of hypertension and hyperlipidemia were receiving treatment.

There are several limitations to our study that need to be considered when interpreting the study findings. First, our study was a retrospective study and there are inherent limitations with retrospective studies such as incomplete data and selection bias. Our study looked into already known risk factors for DR in the context of Brunei Darussalam. Second, this study was conducted in a single hospital and might not accurately represent the whole country. However, the patient population breakdown in our study is consistent with that of the national breakdown and previous studies from different districts have reported comparable results [7,8]. Third, we only included patients over a 3-month period, and it is possible that more patients with significant DR would be included, given their shorter follow-up intervals. This may inflate the prevalence of DR. However, the total number of patients with significant PDR who will have shorter follow-up interval of 3 months is small. Fourth, our study population excluded patients with complicated diseases such as diabetic foot disease, cardiac, or renal disease, as they typically received treatment and are followed up in the tertiary hospital. Such patients are likely to have DR and not captured in our study. Hence, the prevalence of DR could be higher than our estimate. However, the proportion of such patients is estimated to be small.

We showed that DR in Brunei Darussalam is common with a rate of 22.6%, which is comparable to what has been reported in the literature. DR affects one in five patients with type 2 DM in Brunei Darussalam, comparable to rates reported for other Asian populations. A third of those with DR had either PDR or VTDR. Longer duration of DM, poor control of diabetes, and presence of microalbuminuria are significantly associated with DR. Interestingly, age groups were not linearly associated with DR, and this requires further study. Since a large percentage of DR occurs in young and middle-aged patients, it is worthwhile to advocate strict control of DM from the outset. Public and targeted awareness programs are needed, especially in countries with young and growing population, like Brunei Darussalam.

Notes

Conflicts of Interest

No potential conflict of interest relevant to this article was reported.

Funding

The authors received no financial support for this article.

Acknowledgements

None.

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Article information Continued

Table 1

The patients’ demographic and profiles (n = 341)

Variable Value 95% confidence interval
Age (yr) 55.3 ± 11.9 54.0–56.6
 ≤30 12 (3.5) 1.8–5.5
 31–40 29 (8.5) 5.6–11.7
 41–50 65 (19.1) 15.1–23.5
 51–60 118 (34.0) 29.2–40.0
 61–70 92 (27.10) 22.1–31.5
 >70 25 (7.43) 4.7–10.4
Sex
 Male 140 (41.1) 35.7–46.3
 Female 201 (58.9) 53.7–64.3
Ethnicity
 Malays 254 (74.5) 69.5–79.0
 Chinese 21 (6.1) 3.9–9.3
 Indigenous 66 (19.4) 15.3–24.0
Duration of diabetes mellitus (yr) 9.4 ± 7.4 8.6–10.2
 ≤5 136 (39.9) 34.7–45.1
 6–10 75 (22.0) 17.5–26.6
 11–15 63 (18.5) 14.1–22.6
 16–20 33 (9.7) 6.7–12.9
 >20 34 (10.0) 7.0–13.2
Glycated hemoglobin (%) 8.4 ± 1.9 8.2–8.6
 ≤6.9 82 (24.0) 19.5–28.4
 7.0–7.9 84 (24.6) 20.1–29.4
 8.0–8.9 58 (17.0) 13.3–21.3
 9.0–9.9 53 (15.5) 11.7–19.5
 10.0–10.9 21 (6.2) 3.8–8.8
 11.0–11.9 24 (7.0) 4.7–9.9
 ≥12.0 19 (5.6) 3.2–8.2
Comorbidities
 Hypertension (yes) 296 (86.8) 82.9–90.1
 Dyslipidemia (yes) 288 (84.5) 80.5–88.3
 Albuminuria (yes) 77 (22.6) 18.8–27.1

Values are presented as mean ± standard deviation or number (%).

Table 2

The breakdown of retina screening outcome (n = 341)

Type of retinopathy Value 95% confidence interval
No DR 263 (77.1) 72.7–81.9
Any DR 78 (22.9) 18.8–27.1
 Mild NPDR 24 (7.0) 4.4–9.9
 Moderate NPDR 34 (10.0) 7.0–13.2
 Severe NPDR 6 (1.8) 0.6–3.2
 PDR 14 (4.1) 2.1–6.5

Values are presented as number (%).

DR = diabetic retinopathy; NPDR = non-proliferative DR; PDR = proliferative DR.

Table 3

Univariate analyses between variables and presence or absence of any DR (n = 331)

Variable Any DR No DR p-value
Age group (yr)
 ≤40 11 (27.5) 29 (76.7) 0.030 for trend
 41–50 15 (24.2) 47 (75.8)
 51–60 36 (30.8) 81 (69.2)
 61–70 13 (14.8) 75 (85.2)
 >70 2 (8.3) 22 (91.7)
Sex
 Male 31 (23.0) 104 (77.0) 0.915
 Female 46 (23.5) 150 (76.5)
Duration of diabetes mellitus (yr)
 ≤5 19 (14.7) 110 (85.3) 0.002 for trend
 6–10 13 (17.6) 61 (82.4)
 11–15 22 (36.1) 39 (63.9)
 16–20 11 (33.3) 22 (66.7)
 >20 12 (35.3) 22 (64.7)
Diabetes mellitus control
 Good control 20 (14.3) 120 (85.7) <0.0001 for trend
 Suboptimal 15 (20.3) 59 (79.7)
 Poor 42 (35.9) 75 (64.1)
Hypertension (yes) 67 (87.0) 222 (87.4) 0.928
Dyslipidemia (yes) 68 (88.3) 215 (84.6) 0.424
Microalbuminuria (yes) 48 (62.3) 106 (41.7) 0.001

Values are presented as number (%).

DR = diabetic retinopathy.

Table 4

Multivariate analyses of association with any diabetic retinopathy (n = 331)

Variable Number Odds ratio p-value 95% confidence interval
Age group (yr)
 ≤40 40 Reference
 41–50 62 0.63 0.348 0.230–1.67
 51–60 117 0.76 0.545 0.320–1.84
 61–70 88 0.22 0.006 0.076–0.65
 ≥71 24 0.09 0.007 0.020–0.52
Duration of diabetes mellitus (yr)
 ≤5 129 Reference
 6–10 74 1.53 0.301 0.68–3.47
 11–15 61 3.88 0.001 1.78–8.46
 16–20 33 3.39 0.014 1.23–8.98
 >20 34 5.43 0.002 1.89–15.59
Diabetes mellitus control
 Good 140 Reference
 Suboptimal 74 1.14 0.753 0.51–2.51
 Poor 117 2.01 0.039 1.03–3.90
Microalbuminuria
 No 177 Reference
 Yes 154 2.00 0.019 1.12–3.59

Table 5

Comparison of prevalence of diabetic retinopathy among diabetes patients in Brunei Darussalam with some recently published data from countries around the world

Study Country Sample size Mean age (yr) DR (%) Vision-threatening DR (%)

Severe NPDR PDR DME
Naik et al. (2018) [11] USA 5,242 NR 34.0 1.6 1.2 4.3
Kanjee et al. (2016) [12] Canada 4,338 53.0 25.1 NR 6.5 0.2
Vujosevic et al. (2017) [13] Italy 8,596 NR 27.5 2.9 0.9 5.7
Thomas et al. (2015) [14] UK 8,6390 65.3 30.3 NR 0.31 NR
Rodriguez-Poncelas et al. (2015) [15] Spain 10,8723 66.9 12.3 0.86 0.36 0.18
Dehghan et al. (2015) [16] Iran 529 44.0 29.6 3.9 3.9 4.9
Ahmed et al. (2016) [17] Saudi Arabia 401 54.5 36.4 11.0 11.6 7.2
Sunita et al. (2018) [18] India 592 51.0 15.4 NR 6.7 6.6*
Liu et al. (2017) [19] China 13,473 62.5 34.1 0.89 11.5 NR
Abougalambou SS and Abougalambou AS (2014) [20] Malaysia 1,077 NR 39.3 NR NR NR
Tan et al. (2018) [21] Singapore 2,862 61.6 33.9 0.71 3.75 7.6
Jongsareejit et al. (2013) [22] Thailand 1,120 NR 24.0 NR 2.8 NR
Sasongko et al. (2017) [23] Indonesia 1,138 59.0 43.1 11.1 12.1 17.1
Jee et al. (2013) [24] Korea 1,678 63.0 15.8 0.8 2.8 4.5
Current study (2020) Brunei Darussalam 341 55.3 22.9 1.5 4.7 5.0
Da and Nyunt (2003) [7] Brunei Darussalam 358 NR 18.0 NR NR NR
Joshi et al. (2003) [8] Brunei Darussalam 5,365 NR 19.0 NR NR 4.0
Ali et al. (2015) [9] Brunei Darussalam 1,184 NR 18.5 3.7 NR 6.4

Values are presented as number.

DR = diabetic retinopathy; NPDR = non-proliferative DR; PDR = proliferative DR; DME = diabetic macular oedema; NR = not recorded.

*

Clinically significant DME.

Includes PDR.