Papers

Cost effectiveness analysis of screening for sight threatening diabetic eye disease

Marilyn James, head of health economics (research and development) unit ^a,  David A Turner, research fellow ^a,  Deborah M Broadbent, clinical assistant ^b,  Jiten Vora, consultant diabetologist ^c,  Simon P Harding, consultant ophthalmologist ^b. 

^a Centre for Health Planning and Management, University of Keele, Keele, Staffordshire ST5 5BG, ^b St Paul's Eye Unit, Royal Liverpool University Hospitals, Liverpool L7 8XP, ^c Department of Diabetes and Endocrinology, Royal Liverpool University Hospitals

Correspondence to: M James m.james{at}keele.ac.uk

	Abstract

Top Abstract Introduction Methods Results Discussion References

Objective: To measure the cost effectiveness of systematic photographic screening for sight threatening diabetic eye disease compared with existing practice.
Design: Cost effectiveness analysis
Setting: Liverpool.
Subjects: A target population of 5000 diabetic patients invited for screening.
Main outcome measures: Cost effectiveness (cost per true positive) of systematic and opportunistic programmes; incremental cost effectiveness of replacing opportunistic with systematic screening.
Results: Baseline prevalence of sight threatening eye disease was 14.1%. The cost effectiveness of the systematic programme was £209 (sensitivity 89%, specificity 86%, compliance 80%, annual cost £104 996) and of the opportunistic programme was £289 (combined sensitivity 63%, specificity 92%, compliance 78%, annual cost £99 981). The incremental cost effectiveness of completely replacing the opportunistic programme was £32. Absolute values of cost effectiveness were highly sensitive to varying prevalence, sensitivity and specificity, compliance, and programme size.
Conclusion: Replacing existing programmes with systematic screening for diabetic eye disease is justified.

	Introduction

Top Abstract Introduction Methods Results Discussion References

Various methods of screening for diabetic eye disease have been tested in recent years,^1-12 but few studies have produced meaningful cost effectiveness data. A three centre study commissioned by the Department of Health reported relatively high costs per case of diabetic eye disease detected. ^{1 2} Similar data are also available from the United States.⁵ The Department of Health study was undermined by suboptimal screening methods, and both studies disregarded the effect of pre-existing opportunistic screening on cost effectiveness. Foulds et al studied the potential savings of systematic screening, but the cost effectiveness data are difficult to verify in the absence of sensitivity data.¹³ Mathematical modelling has also been used to study the potential economic benefits of screening. ^{4 6 14}

Nationally coordinated screening of diabetic patients for sight threatening eye disease is being considered as part of the national service framework on diabetes, which is due to be published in spring 2001, and an economic evaluation of a programme with high sensitivity and specificity and known prevalence and compliance is therefore urgently needed.¹⁵ The Liverpool diabetic eye study was established in 1991 to investigate the efficacy of primary care based photographic screening for sight threatening eye disease and to set up a systematic service replacing the existing opportunistic programme. We present a detailed cost effectiveness analysis of the systematic and opportunistic programmes and the effect of varying disease prevalence, compliance, and sensitivity and specificity to allow generalisation of our results throughout the NHS.

	Methods

Top Abstract Introduction Methods Results Discussion References

The systematic screening programme uses a mobile screening unit that visits inner city general practices together with a dedicated hospital assessment clinic.¹⁶ Screening comprises three-field, non-stereoscopic photography using mydriasis; 35 mm transparencies; and validated grading. The pre-existing opportunistic service used direct ophthalmoscopy and was performed by general practitioners, optometrists, and diabetologists. There was no systematic training, central coordination, or audit, and patients with positive results were assessed in general hospital eye service clinics.

The outcome measure was the detection of sight threatening eye disease, defined as any of the following: moderate preproliferative retinopathy or worse; circinate exudates within the macula; any exudate within 1 disc diameter of the foveola; other diabetes related disease such as vascular occlusion.

Source data
Data for this analysis were taken from two studies within the Liverpool diabetic eye study. The first was a cross sectional observational study of 320 diabetic patients registered with four general practices who were examined by a consultant ophthalmologist specialising in medical retinal diseases using slit-lamp biomicroscopy (an accepted reference standard for determining need for treatment). ^{8 16} The second study comprised an analysis of the implementation of systematic screening in Liverpool and included a structured, closed response questionnaire administered by trained observers to the first 1363 diabetic patients recruited.¹⁷ These two studies provided all data except the specificity of the opportunistic programme, which was calculated from a previous study.¹ We adopted a health service perspective for measurement of costs and benefits.

Costs
We used an ingredient approach because the costs in screening programmes are largely fixed or semifixed; recording individual patient based costings is not helpful in this situation. Capital was given a seven year life and discounted at the test discount rate of 6%. Overhead costs for hospital based activitiesgrading, administration, and follow upwere set at 10% (Royal Liverpool University Hospitals Trust finance data).

	Results

Top Abstract Introduction Methods Results Discussion References

A baseline prevalence of 14.1% and a cohort of 5000 patients yield an assumed 705 (14.1/100×5000) true cases of sight threatening eye disease in the target population. Table 1 shows the number of true and false positive and negative results calculated for each programme. Table 2 shows the costs for the components of systematic screening, and table 3 presents costs for opportunistic screening based on the percentage of the sample seen by each type of screener. Total costs were £104 996 for systematic screening and £99 981 for opportunistic screening. The cost effectiveness was £209 and £289 respectively, and incremental cost effectiveness was £32 (table 4).

Sensitivity analysis
Figure 1 shows the effect of varying the prevalence of sight threatening eye disease on cost effectiveness. If the prevalence falls the cost effectiveness of both programmes falls. At all prevalences the opportunistic programme is less expensive, but the systematic programme is more cost effective than the opportunistic programme.

View larger version (25K): [in this window] [in a new window]   Fig 1.   Effect of changing prevalence of sight threatening diabetic eye disease on cost effectiveness of systematic and opportunistic screening programmes

View larger version (16K): [in this window] [in a new window]   Fig 2.    Effect of varying sensitivity of opportunistic screening on cost effectiveness. Cost effectiveness of systematic screening is shown as horizontal line

	Discussion

Top Abstract Introduction Methods Results Discussion References

We directly compared the costs of pre-existing opportunistic screening with a newly introduced systematic programme. The systematic programme is slightly more expensive than the opportunistic programme but yields 157 extra cases at only £32 per case.

In an earlier cost effectiveness assessment, Buxton et al studied 3318 screen events in three UK centres using two methods: direct ophthalmoscopy by optometrists, physicians, and general practitioners and single field non-mydriatic polaroid photography. ^{1 2} If their figures are adjusted to 1996-7 prices the cost effectiveness of direct ophthalmoscopy by optometrists is £1057, hospital physicians £1392, and general practitioners £853-£1454; the costs of hospital and community photographic screening ranged from £670 to £2084. Their disappointing results were largely due to suboptimal screening methods and a low prevalence (5.8%).²

Lairson et al studied the cost effectiveness of four screening methods in the United States.⁵ They also found a large difference between a photographic protocol similar to ours ($295 (£184)) and direct ophthalmoscopy by a technician ($794), with direct ophthalmoscopy over 2.5 times more expensive than photography.

Applicability
Our results can be generalised to other British photographic screening programmes. The baseline prevalence is likely to be similar throughout the country,¹⁹ as is the effectiveness of opportunistic screening. However, accurate data on sensitivity, specificity, and compliance are required to complete an analysis based on our model. Such an analysis would be valuable when applied to other current techniques including dual modality screening,^20-22 optometry based programmes,²³ digital photography, ^{24 25} and automated neural net systems.²⁶

Outcome measures
We have used the number of detected cases as our measure of effectiveness. The use of this proxy measure depends on the inference that correctly and appropriately identified cases can be treated and blindness prevented. Although useful, this kind of measure does not necessarily show the full effectiveness of a programme as it reflects process rather than final outcome. Further work is required to measure cost effectiveness against long term end points such as numbers of patients treated, years of sight saved, quality of life, or numbers of blind registrations.⁵

	Acknowledgments

We thank Mr P Kingham of Royal Liverpool University Hospitals Trust finance department for help with costs.

Contributors: SPH, DMB, MJ, and JV conceived the study and wrote the protocol. DAT and MJ performed cost modelling and sensitivity analysis. DMB performed prevalence and compliance analysis and contributed to cost modelling. SPH wrote the manuscript with contributions from MJ, DAT, DMB, and JV. MJ is the guarantor of the study.

	Footnotes

Funding: This study was funded by North West Regional grant DIF1.

Competing interests: None declared.

	References

Top Abstract Introduction Methods Results Discussion References

1.	Buxton MJ, Sculpher MJ, Ferguson BA, Humphreys JE, Altman JF, Spiegelhalter DJ, et al. Screening for treatable diabetic retinopathy: a comparison of different methods. Diabet Med 1991; 8: 371-377[Medline].
2.	Sculpher MJ, Buxton MJ, Ferguson BA, Humphreys JE, Altman JFB, Spiegelhalter DJ, et al. A relative cost-effectiveness analysis of different methods of screening for diabeticretinopathy. Diabetic Med 1991; 8: 644-650[Medline].
3.	Fendrick AM, Javitt JC, Chiang YP. Cost-effectiveness of the screening and treatment of diabetic retinopathy. What are the costs of underutilization? Int J Technol Assess Health Care 1992; 8: 694-707[Medline].
4.	Javitt JC, Canner JK, Sommer A. Cost-effectiveness of current approaches to the control of retinopathy in type I diabetics. Ophthalmology 1989; 96: 255-264[Medline].
5.	Lairson DR, Pugh JA, Kapadia AS, Lorimor RJ, Jacobson J, Velez R. Cost-effectiveness of alternative methods for diabetic retinopathy screening. Diabetes Care 1992; 15: 1369-1377[Abstract].
6.	Dasbach EJ, Frybach DG, Newcomb PA, Klein R, Klein BEK. Cost-effectiveness of strategies for detecting diabetic retinopathy. Med Care 1991; 29: 20-39[CrossRef][Medline].
7.	Sculpher MJ, Buxton MJ, Ferguson BA, Spiegelhalter DJ, Kirby AJ. Screening for diabetic retinopathy: a relative cost-effectiveness analysis of alternative modalities and strategies. Health Econ 1992; 1: 39-51[Medline].
8.	Scott JA, Harding SP, Broadbent DM, Vora J. Detecting sight threatening diabetic eye disease in an inner city setting in the UKthe Liverpool diabetic eye study. Invest Ophthalmol Vis Sci 1996; 37: S105.
9.	Finlay R, Griffiths J, Jackson G, Law D. Can general practitioners screen their own patients for diabetic retinopathy? Health Trends 1991; 23: 104-105.
10.	Awh CC, Javitt JC, Chong LP, Gehrs KM, Gusman GI, Street DA, et al. Ophthalmoscopic diagnosis and referral of diabetic eye disease by Primary Care Physicians. ARVO abstract. Invest Ophthalmol Vis Sci 1993; 34: 713.
11.	Forrest RD, Jackson CA, Yudkin JS. Screening for diabetic retinopathy. Comparison of a nurse and doctor with retinal photography. Diabetes Res 1987; 5: 39-42[Medline].
12.	Kinyoun JL, Martin DC, Fujimoto WY, Leonetti DL. Ophthalmoscopy versus fundus photography for detecting and grading diabetic retinopathy. Invest Ophthalmol Vis Sci 1992; 33: 1888-1893[Abstract/Free Full Text].
13.	Foulds W, McCuish A, Barrie T, Green F, Scobie IN, Ghafour IM, et al. Diabetic retinopathy in the west of Scotland: its detection and prevalence, and cost-effectiveness of a proposed screening programme. Health Bull 1983; 41: 318-326.
14.	Rohan TE, Frost CD, Wald NJ. Prevention of blindness by screening for diabetic retinopathy: a quantitative assessment. BMJ 1989; 299: 1198-1201.
15.	Davies R, Sullivan P, Canning C. Simulation of eye disease to compare screening policies. Br J Ophthalmol 1996; 80: 945-950[Abstract/Free Full Text].
16.	Harding SP, Broadbent DM, Neoh C, White MC, Vora J. Sensitivity and specificity of photography and direct ophthalmoscopy in screening for sight threatening eye disease: the Liverpool diabetic eye study. BMJ 1995; 311: 1131-1135[Abstract/Free Full Text].
17.	Briggs MC, Broadbent DM, Harding SP, Vora JP. Primary screening in an inner citythe Liverpool diabetic eye study. Diabet Med 1995; 12(suppl 2): S44.
18.	Netten A, Dennett J. Unit costs of community care. Canterbury: Personal Social Services Research Unit, University of Kent, 1996.
19.	Owens DR, Gibbins RL, Lewis PA, Wall S, Allen JC, Morton R. Screening for diabetic retinopathy by general practitioners: ophthalmoscopy or retinal photography as 35 mm transparencies? Diabet Med 1998; 15: 170-175[CrossRef][Medline].
20.	Ryder B. Screening for diabetic retinopathy. BMJ 1995; 311: 207-208[Free Full Text].
21.	O'Hare JP, Hopper A, Madhaven C, Charny M, Purewal TS, Harney B, et al. Adding retinal photography to screening for diabetic retinopathy: a prospective study in primary care. BMJ 1996; 312: 679-682[Abstract/Free Full Text].
22.	Jacob J, Stead J, Sykes J, Taylor D, Tooke JE. A report on the use of technician ophthalmoscopy combined with the use of the Canon non-mydriatic camera in screening for diabetic retinopathy in the community. Diabet Med 1995; 12: 419-425[Medline].
23.	Leese GP, Tesfaye S, Dengler-Harles M, Laws F, Clark DI, Gill GV, et al. Screening for diabetic eye disease by optometrists using the slit-lamp. J R Coll Physicians 1997; 31: 65-69.
24.	George LD, Halliwell M, Hill R, Aldington SJ, Lusty J, Dunstan F, et al. A comparison of digital and 35 mm colour transparencies in detecting and grading diabetic retinopathy. Diabetic Med 1998; 15: 250-253[CrossRef][Medline].
25.	Ryder REJ, Kong N, Bates AS, Sim J, Welch J, Kritzinger EE. Instant electronic imaging systems are superior to polaroid at detecting sight threatening diabetic retinopathy. Diabet Med 1998; 15: 254-258[CrossRef][Medline].
26.	Gardner GG, Keating D, Williamson TH, Elliott AT. Automatic detection of diabetic retinopathy using an artificial neural network: a screening tool. Br J Ophthalmol 1996; 80: 940-944[Abstract/Free Full Text].
27.	Sussman EJ, Tsurias WG, Sarper KA. Diagnosis of diabetic eye disease JAMA 1982; 247: 3231-3234[Abstract/Free Full Text].
28.	Gehrs KM, Chong LP, Gusman G, Street DA, Awh C, Cupples H, et al. Can we educate primary care physicians about diabetic retinopathy after graduation? Preliminary results of the diabetic retinopathy education study. Invest Ophthalmol Vis Sci 1993; 34: S1182.

(Accepted 13 March 2000)