Intended for healthcare professionals

  1. Research
  2. Effectiveness of...
  3. Effectiveness of screening older people for impaired vision in community setting: systematic review of evidence from randomised controlled trials
Papers

Effectiveness of screening older people for impaired vision in community setting: systematic review of evidence from randomised controlled trials

BMJ 1998; 316 doi: https://doi.org/10.1136/bmj.316.7132.660 (Published 28 February 1998) Cite this as: BMJ 1998;316:660
  1. Liam Smeeth (l.smeeth{at}ucl.ac.uk), research registrar,
  2. Steve Iliffe, reader
  1. Department of Primary Care and Population Sciences, Royal Free Hospital School of Medicine and University College London Medical School, London NW3 2PF
  1. Correspondence to: Dr L Smeeth
  • Accepted 18 November 1997

Abstract

Objective: To assess whether population screening for impaired vision among older people in the community leads to improvements in vision.

Design: Systematic review of randomised controlled trials of population screening in the community that included any assessment of vision or visual function with at least 6 months' follow up.

Subjects: Adults aged 65 or over.

Main outcome measure: Proportions with visual impairment in intervention and control groups with any method of assessing visual impairment.

Results: There were no trials that primarily assessed visual screening. Outcome data on vision were available for 3494 people in five trials of multiphasic assessment. All the trials used self reported measures for vision impairment, both as screening tools and as outcome measures. The inclusion of a visual screening component in the assessments did not result in improvements in self reported visual problems (pooled odds ratio 1.04: 95% confidence interval 0.89 to 1.22). A small reduction (11%) in the number of older people with self reported visual problems cannot be excluded.

Conclusions: Screening of asymptomatic older people in the community is not justified on present evidence. Visual impairment in this age group can usually be reduced with treatment. It is unclear why no benefit was seen. Further work is needed to clarify what interventions are appropriate for older people with unreported impairment of vision.

Key messages

  • Impaired vision is common among older people and has a variety of adverse associations

  • General practitioners are currently obliged to offer an annual assessment of vision as part of the 75 and over programme

  • Evidence for effectiveness of visual screening is lacking, but a small beneficial effect cannot be excluded

  • The continued inclusion of screening for impaired vision in screening programmes for older people is not supported by the evidence

  • Further work is needed to clarify appropriate interventions for older people with unreported visual impairment

Introduction

The introduction of the sight test fee in 1990 increased concern about undetected visual problems in older people,1 and visual screening for older people in general practice was advocated.2 Renewed concern has been expressed recently by the Royal National Institute for the Blind3 and the Department of Health.4

Since 1990 general practitioners have been required to offer an annual screening assessment to all patients aged 75 and over,5 specifically including an assessment of vision. While multiphasic screening of older people has been shown to be beneficial overall,6 exactly which procedures are effective is uncertain. The 75 and over programme is currently under review.7

Rationale for screening older people for visual problems

Visual impairment is common among older people. In community based surveys of unselected older people undertaken in the United Kingdom, visual acuity of less than 6/12 has been found in around 2% of those aged 65 to 74 and around 20% of those aged 75 and over. 8 9 This level of visual acuity is below the requirements for driving in the United Kingdom.10 Larger surveys have been performed in the United States,1113 and, though the prevalence of reduced visual acuity is lower in one of these,11 similar overall trends are seen. Various adverse factors have been reported in association with visual impairment. These include reduced functional status and quality of life,1416 depression,1618 and falls.1921

Visual problems in older people may go unreported for several reasons, including decreased expectations in old age and a belief that nothing can be done to help,14 failure by the patient to recognise visual loss,22 or the presence of another handicap that dominates the perception of difficulties.23 Other possible inhibiting factors include fears about surgical treatment and costs24 and the stigma of blindness.25

How and why vision should be assessed was not specified in the 1990 general practitioner contract.5 The Royal College of General Practitioners advocates a simple question about visual function to identify unreported problems.26 Specific screening procedures for glaucoma or diabetic retinopathy have not been included in the over 75 programme nor in trials of multiphasic screening.

Methods

The research question was defined as, what is the effectiveness of population screening for visual impairment in improving vision among unselected older people (aged 65 or over) in a community setting, either alone or as part of a multiphasic assessment programme?

Search methods

A systematic Medline search for randomised controlled trials evaluating screening in older people was performed for the period 1966 to December 1996 by using a published optimally sensitive search strategy.27 The exploded (that is, including all sub-branches) MeSH terms “mass screening,” “preventive health services,” “eye diseases,” and “diagnosis, eye,” and the non-exploded MeSH terms “health promotion” and “geriatric assessment” were used. Titles and abstracts were searched for the words “geriatric” or “elderly” combined with any of “screening,” “assessment,” “health,” “function,” or “surveillance.” Other textword searches used the words “macular degeneration,” “cataract,” and “presbyopia.” Wild card characters were used to ensure all forms of words were included. At all stages articles about animals and children were excluded. The October 1997 Cochrane Library (which includes the Cochrane Controlled Trials Register and the Database of Abstracts of Reviews of Effectiveness) was also searched for both trials and relevant reviews.28 Other review articles and books were consulted. Bibliographies of all relevant articles were scanned. Experts in screening for older people and in ophthalmology were consulted.

Inclusion criteria

The inclusion criteria were in two stages. In the first stage, articles were included only if they were randomised controlled trials of either visual or multiphasic screening of unselected subjects in a community setting that included patients aged 65 and over. Trials of screening undertaken on selected groups of patients were excluded on the grounds that the results would not answer the question under review. Studies including adults aged under 65 only were also excluded. Because visual screening may have been only one small part of a multiphasic screening programme and data about visual outcomes may not have been included in published reports of trials, therefore, the named author for correspondence for all trials identified in the first stage was contacted (at their current addresses verified by telephone) to ask for any further unpublished data about visual screening tests used and visual outcomes. Non-responders were sent two reminders and were telephoned.

The second stage inclusion criteria were then applied to all the trials included from the first stage: the availability of any visual outcome data, whether formally tested or self reported; and a follow up of at least six months to allow intervention for detected visual problems.

Study selection and data extraction

The full texts of articles selected for retrieval and review from the abstracts and citations were obtained. A checklist of the first stage inclusion criteria was then applied by both authors independently. All criteria had to be met. After contact with the trial authors a structured data extraction form was used, again by both authors independently. Data was extracted as follows: setting; subjects; overall intervention; visual screening test(s) used; duration of follow up; and visual outcome measures and visual outcome data. Data about randomisation process, the degree of allocation concealment, and blinding of outcome assessors was also extracted. Authors were contacted for clarification if required. Disagreements between reviewers were discussed and a consensus reached on all articles.

Critical appraisal

There is empirical evidence that inadequate randomisation to intervention and control groups can affect the outcome of a trial.29 In particular, it is important that the treatment assignment is known only after the decision has been taken for the patient to enter the trial. This is known as concealed allocation. Studies were therefore classified for allocation concealment by using previously developed categories: A=trials in which allocation appeared to be adequately concealed (for example, a central randomisation procedure); B=trials in which allocation concealment was unclear, either because the approach was not reported or in which the randomisation process did not match categories A or C; and C=trials in which allocation concealment was inadequate (such as alphabetical use of surname).30 In addition, data were extracted about the degree of blinding of outcome assessors in the trials.

Outcome measures

The aims of multiphasic screening of older people are broad—for example, to improve quality of life and reduce admission to hospital. Any benefit arising from the inclusion of a visual assessment, however, will necessarily be dependent on improved vision, which was therefore used as the outcome measure for this review. Any method of visual assessment (such as acuity chart, questions about vision, or measures of visual function) was accepted as an outcome measure. We felt that stricter inclusion would excessively limit the data included in the review.

Analysis

We used RevMan software.31 Heterogeneity between trials was tested for with χ2 test. Odds ratios were combined with the fixed effects Mantel-Haenszel method. The relative risk is presented as well as the odds ratio because it is more easily understood by some.32

Results

In total 2246 citations and abstracts were screened, and 147 full text articles were reviewed in detail. Seventeen trials met the first stage inclusion criteria, all of which were trials of multiphasic screening. The reference details are given on the web.w1-17 There were no trials that primarily assessed visual screening. Requests for further information led to replies from authors of 16 of the 17 trials. Five trials met the final inclusion criteria—that is, visual outcome data with follow up of at least 6 months.w3 w9 w13 w14 w16 These trials are summarised in table 1.

Table 1

Randomised controlled trials of screening older people that included data on visual outcome: subjects, settings, and interventions. In all trials concealment of allocation was adequate (see text for details)

View this table:

All five trials adequately concealed randomisation. Regarding blinding of outcome assessors, the trial participants were aware of whether they had received a screening assessment. Thus, despite attempts to blind the outcome assessors, which arm of the trial subjects were in could clearly emerge during the face to face assessments of outcome. This phenomenon was noted by Vetter in two trialsw3 w13 and led McEwan to consider such blinding impossible.w9

Individuals in the trial by Wagner and colleagues were recruited from a health maintenance organisation and may have differed in their overall baseline health from the general population.w16 This trial had three arms. For the purposes of our review subjects in the two arms who did not receive any form of visual screening assessment were analysed together as control patients.

Table 2 shows the visual assessment methods and outcome measures. All the trials used self reported measures to assess impaired vision, both as the screening assessment and as the outcome measure.

Table 2

Visual screening methods and outcome measures

View this table:

Effects of screening on visual impairment

Statistical testing showed no evidence of heterogeneity of effect in the five trials (χ2=0.96, df=4, P=0.92). When odds ratios were pooled there was no reduction in the proportion of individuals with visual impairment as a result of screening (pooled odds ratio 1.04; 95% confidence interval 0.89 to 1.22). The figure shows the outcome data, and individual and pooled odds ratios. The pooled relative risk for visual impairment was 1.03 (0.92 to 1.15).

Figure1

Outcome data: individual and pooled odds ratios for visual screening as part of multiphasic screening package versus standard care. Outcome was not seeing well, as defined by each trial

Discussion

The evidence from randomised controlled trials does not support the inclusion of an assessment of vision in regular multiphasic assessment programmes for unselected older people in a community setting or visual screening in primary care.2 Although a reduction of 11% in the number of older people with visual impairment cannot be excluded, even this figure is disappointingly low.

Results from community surveys in the over 75 age group suggest that over half the visual impairment in this age group could potentially be reduced with treatment, notably by cataract surgery or refractive correction. 8 13 In light of this the lack of improvement seen in these trials is somewhat surprising and cannot be explained from the data presented. Several factors, however, may have contributed. Firstly, the visual assessment was only one component of the screening package in all five trials, and visual screening performed in isolation may have produced a greater effect. This hypothesis was previously suggested as an explanation of the lack of effectiveness of screening for visual impairment seen in a trial of a multiphasic screening assessment among middle aged men. 33 34 In clinical practice, however, screening for visual impairment is highly likely to be one part of a broader screening package, and therefore an assessment of effectiveness within a broader package is the most pragmatically useful measure. Secondly, the people who reported visual problems when prompted to do so in a screening programme may not have perceived their previously unreported visual impairment as a “need” for intervention. Lastly, there is evidence that considerable obstacles exist to improving visual impairment among older people. In the United Kingdom fear of costs has been repeatedly cited by a proportion of older people as a barrier to attending an optometrist and obtaining glasses. 3 14 24 35 In addition, ophthalmic services are unable to meet current demands for treatment, with long waiting lists for cataract surgery in many areas.36

The aim of population screening of older people for visual impairment is presumably to discover visual impairment in those who are not presenting to the health services and to offer them interventions to improve their vision. Further work is required, however, to determine the needs of older people with unreported visual problems. Before population screening can be effective, existing obstacles to the reduction of visual impairment among older people must be overcome.

Figure2

Full details of references w1-17 appear on our website at www.bmj.com

Acknowledgments

We thank all the study authors who responded to requests for additional information. R McEwan, N Vetter, E van Rossum, and E Wagner provided unpublished data used in this review.

Contributors: LS developed the original idea, searched the literature, and undertook the analysis. SI had the original idea and provided supervision throughout. Both authors critically appraised the trials, extracted data, wrote the paper, and approved the final manuscript. LS is the guarantor of the paper.

Funding: LS was a research registrar on the London Academic Training Scheme (LATS), 1996-7.

Conflict of interest: None.

References

  1. 1.
    1. Rosenthal A
    . High street eye tests. BMJ 1990;300:695-696.
  2. 2.
    1. Hitchings RA
    . Visual disability and the elderly. BMJ 1989;298:1126-1127.
  3. 3.
    1. Grindey S,
    2. Winyard S
    . Losing sight of blindness. London: RNIB, 1997.
  4. 4.
    1. Department of Health
    . The National Health Service: a service with ambitions. London: HMSO, 1996
  5. 5.
    1. Department of Health and the Welsh Office
    . General practice in the National Health Service. A new contract. London: Department of Health, 1989
  6. 6.
    1. Stuck AK,
    2. Siu AL,
    3. Wieland GD,
    4. Adams J,
    5. Rubenstein LZ
    . Comprehensive geriatric assessment: a meta-analysis of controlled trials. Lancet 1993;342:1032-1036.
    OpenUrlCrossRefPubMedWeb of Science
  7. 7.
    1. Iliffe S,
    2. Gould M,
    3. Wallace P
    . Evaluation of the over 75 checks in general practice. Report to the NHS Executive. London: Department of Primary Care and Population Sciences, University College London Medical School and the Royal Free Hospital School of Medicine, 1997.
  8. 8.
    1. Wormald RP,
    2. Wright LA,
    3. Courtney P,
    4. Beaumont B,
    5. Haines AP
    . Visual problems in the elderly population and implications for services. BMJ 1992;304:1226-1229.
  9. 9.
    1. Lavery JR,
    2. Gibson JM,
    3. Shaw DE,
    4. Rosenthal AR
    . Vision and visual acuity in an elderly population. Ophthalmic Physiol Opt 1988;8:390-393.
    OpenUrlPubMedWeb of Science
  10. 10.
    1. Drivers Medical Group
    . At a glance guide to current medical standards of fitness to drive. Swansea: DVLA, 1996.
  11. 11.
    1. Leibowitz HM,
    2. Krueger DE,
    3. Maunder LR,
    4. Milton RC,
    5. Kini MM,
    6. Kahn HA,
    7. et al
    . The Framingham eye study monograph. Surv Ophthalmol 1980; 24(suppl): 335-335.
  12. 12.
    1. Tielsch JM,
    2. Sommer A,
    3. Witt K,
    4. Katz J,
    5. Royall RM
    . Blindness and visual impairment in an American urban population. The Baltimore eye survey. Arch Ophthalmol 1990;108:286-290.
    OpenUrlCrossRefPubMedWeb of Science
  13. 13.
    1. Klein R,
    2. Klein BE,
    3. Linton KL,
    4. De MD
    . The Beaver Dam eye study: visual acuity. Ophthalmology 1991;98:1310-1315.
    OpenUrlPubMedWeb of Science
  14. 14.
    1. Landes R,
    2. Popay J
    . “My sight is poor but I'm getting on now”: The health and social care needs of older people with visual problems. Health Soc Care 1993;1:325-335.
  15. 15.
    1. Scott IU,
    2. Schein OD,
    3. West S,
    4. Bandeen-Roche K,
    5. Enger C,
    6. Folstein MF
    . Functional status and quality of life measurement among ophthalmic patients. Arch Ophthalmol 1994;112:329-335.
    OpenUrlCrossRefPubMedWeb of Science
  16. 16.
    1. Carabellese C,
    2. Appollonio I,
    3. Rozzini R,
    4. Bianchetti A,
    5. Frisoni GB,
    6. Frattola L,
    7. et al
    . Sensory impairment and quality of life in a community elderly population. J Am Geriatr Soc 1993;41:401-407.
    OpenUrlPubMedWeb of Science
  17. 17.
    1. Rovner BW,
    2. Zisselman PM,
    3. Shmuely-Dulitzki Y
    . Depression and disability in older people with impaired vision: a follow-up study. J Am Geriatr Soc 1996;44:181-184
    OpenUrlPubMedWeb of Science
  18. 18.
    1. Jones DA,
    2. Vetter NJ,
    3. Victor CV
    . Visual disability and associated factors in the elderly. Health Visitor 1987;60:256-257
    OpenUrlPubMed
  19. 19.
    1. Brocklehurst JC,
    2. Exton-Smith AN,
    3. Lempert-Barber SM,
    4. Hunt LP,
    5. Palmer MK
    . Fracture of the femur in old age: a two centre study of associated clinical factors and the cause of the fall. Age Ageing 1978;7:7-15.
    OpenUrlAbstract/FREE Full Text
  20. 20.
    1. Felson DT,
    2. Anderson JJ,
    3. Hannan MT,
    4. Milton RC,
    5. Wilson MC,
    6. Kiel DP
    . Impaired vision and hip fracture, the Framingham study. J Am Geriatr Soc 1989;37:495-500.
    OpenUrlPubMedWeb of Science
  21. 21.
    1. Grisso JA,
    2. Kelsey JL,
    3. Strom BL,
    4. Chiu GY,
    5. Maislin G,
    6. O'Brien LA,
    7. et al
    . Risk factors for falls as a cause of hip fracture in women. The Northeast Hip Fracture Study Group. N Engl J Med 1991;324:1326-1331.
    OpenUrlPubMedWeb of Science
  22. 22.
    1. Long CA,
    2. Holden R,
    3. Mulkerrin E,
    4. Sykes D
    . Opportunistic screening of visual acuity of elderly patients attending outpatient clinics. Age Ageing 1991;20:392-395.
    OpenUrlAbstract/FREE Full Text
  23. 23.
    1. Cullinan TR
    . The epidemiology of visual disability. Studies of visually disabled people in the community. Canterbury: University of Kent, 1977 (Health Services Research Unit Report No 28.)
  24. 24.
    1. Reinstein DZ,
    2. Dorward NL,
    3. Wormald RP,
    4. Graham A,
    5. O'Connor I,
    6. Charlton RM,
    7. et al
    . “Correctable undetected visual acuity deficit” in patients aged 65 and over attending an accident and emergency department. Br J Ophthalmol 1993;77:293-296.
    OpenUrlAbstract/FREE Full Text
  25. 25.
    1. Cullinan TR
    . Visual disability in the elderly. London: Croom Helm, 1986.
  26. 26.
    1. Williams EI,
    2. Wallace P
    . Health checks for people aged 75 and over. London: Royal College of General Practitioners, 1993.
  27. 27.
    1. Dickersin K,
    2. Scherer E,
    3. Lefebvre C
    . Identification of relevant studies for systematic reviews. BMJ 1994;309:1286-1291.
    OpenUrlAbstract/FREE Full Text
  28. 28.
    The Cochrane Library [database on disk and CD-ROM]. Cochrane Collaboration, 1997, Issue 4. Oxford: Update Software, 1997. Updated quarterly.
  29. 29.
    1. Schulz KF,
    2. Chalmers I,
    3. Hayes RJ,
    4. Altman DG
    . Empirical evidence of bias. Dimensions of methodological quality associated with estimates of treatment effects in controlled trials. JAMA 1995;273:408-412.
    OpenUrlCrossRefPubMedWeb of Science
  30. 30.
    1. Mulrow CD,
    2. Oxman AD
    eds. Critical appraisal of studies. Cochrane Collaboration Handbook [updated 1 March 1997]; Section 6. The Cochrane Library [database on disk and CD ROM]. Cochrane Collaboration. Oxford: Update Software, 1997. Updated quarterly.
  31. 31.
    1. Update Software
    . RevMan. Version 3.0 for Windows. Oxford: Update Software, 1996.
  32. 32.
    1. Sackett DL,
    2. Deeks JJ,
    3. Altman DG
    . Down with odds ratios! [EBM note.] Evidence Based Med 1996;1:164-6.
  33. 33.
    1. The South-East London Screening Study Group
    . A controlled trial of multiphasic screening in middle-age: results of the south-east London screening study. Int J Epidemiol 1977;6:357-363
    OpenUrlAbstract/FREE Full Text
  34. 34.
    1. Stone DH,
    2. Shannon DJ
    . Screening for impaired visual acuity in middle age in general practice. BMJ 1978;2:859-861.
  35. 35.
    1. Webster E WA, Barnes G
    . Eye tests in the elderly: factors associated with attendance and diagnostic yield in non-attenders. J R Soc Med 1992;85:614-6
  36. 36.
    1. NHS Centre for Reviews and Dissemination, University of York
    . Management of cataract. Effective Health Care 1996;2(3).
View Abstract
Back to top