The Risk of Fellow Eye Visual Loss With UnilateralRetinal Pigment Epithelial Tears
Gabrielle Schoeppner, M.D., Elaine L. Chuang, M.D., and Alan C. Bird, M.D.
To identify the magnitude of risk of felloweye visual loss, we reviewed the records of 43patients with unilateral central visual losscaused by a tear of detached retinal pigmentepithelium seen in our institution over a period of one to 13 years. Loss of vision because ofcomplications of age-related macular diseaseoccurred in 16 of 43 patients (37%) in the firstyear, seven of 23 patients (30%) in the secondyear, and eight of 16 patients (50%) in the thirdyear. An additional five patients lost visualacuity between the third and eighth years offollow-up. The cumulative risk of loss of visual acuity was 37% in one year, 59% in twoyears, and 80% in three years. Visual lossoccurred in 29 of the 36 eyes as a result of acomplication of retinal pigment epithelial detachment. The magnitude of risk to the felloweye was greater than has been documented inunselected age-related macular degeneration.
IN AGE-RELATED MACULAR DISEASE, the risk ofdeveloping a lesion in the fellow eye in patientswith visual loss in the first eye has been variously estimated at a cumulative risk of 12%over four to 27 months, I 36% for one to fouryears,234% for 3% years," and as an annual riskof 12% to 15%4,6 and 3% to 7%.6 It has beensuggested that the overall risk in age-relatedmacular degeneration may not be uniform, andthe risk has been correlated with the appearance, density of distribution, and fluorescenceof the drusen. 3,4,6-11
In 1981, a newly recognized complication ofage-related macular disease, tears of detachedretinal pigment epithelium, was described."
Accepted for publication Sept. 14, 1989.From the Department of Clinical Ophthalmology, In
stitute of Ophthalmology, Moorfields Eye Hospital,London, England. This study was supported by theMedical Research Council Grant G 8709312 N.
Reprint requests to Alan C. Bird, M.D., ProfessorialUnit, Moorfields Eye Hospital, City Road, EC1, London,V 2PD United Kingdom.
Since then, it has been determined that peoplewith tears of the pigment epithelium in one eyehave a particularly high risk of sustaining anidentical lesion in the fellow eye." We hadformed a clinical impression that the risk ofvisual loss in the fellow eye in patients with apigment epithelial tear in one eye was muchhigher than in other forms of age-related macular degeneration. We undertook this study totest this observation and to provide data thatwould be directly comparable to previous investigations of fellow-eye visual loss in patientswho had any form of exudative maculopathy inthe affected eye. If the magnitude of risk in thissubset of patients with age-related maculardisease was found to be greater than the groupas a whole, it would allow a more accurateprognosis to be given and support the view thatdifferential risk exists within age-related macular disease. It might also stimulate a search forpotential prophylaxis.
Subjects and Methods
Records, including fluorescein angiograms,of the 84 patients who had tears of the retinalpigment epithelium were reviewed. These patients were seen in our clinic between 1976 and1987. Tears were identified by criteria previously established." The diagnosis was consideredacceptable in the acute stage if the bed of thetear was readily recognizable by biomicroscopyand fluorescein angiography with a welldefined margin between the bed of the tear andthe hyperpigmented residual detachment. Insome patients, the diagnosis was not evidentuntil the second visit if blood obscured the bedof the tear at the time of first examination. Asmall number of patients were seen more thansix months after the initial event with welldefined fibrosis next to hyperpigmented pigment epithelium.
Forty-eight patients had a tear in one eye anda visual acuity of 20/40 or better in the other eye
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684 AMERICAN JOURNAL OF OPHTHALMOLOGY December, 1989
at the time of their first visit. In the good eye,drusen were identified in the fundus, but therewas no evidence of exudative complications ofage-related macular degeneration. Of thisgroup, four patients were not available forfollow-up; two had left the country after theirinitial examination, and two died severalmonths after the initial event. A fifth patientcould not be included because the tear wasprecipitated by photocoagulation to an avascular pigment epithelial detachment in the felloweye within a year of the occurrence of a tear inthe first eye. The 43 remaining patients wereincluded in the study.
Visual loss was defined as reduction of acuityin the fellow eye to a level of 20/80 or worsebecause of lesions known to complicate agerelated macular disease, namely detachment ofthe retinal pigment epithelium, subretinal neovascularization, and geographic atrophy. Allpatients who had not lost vision were invitedfor follow-up examinations in 1986 and 1988. Atthe initial visit and each subsequent visit, thebest-corrected visual acuity was recorded andophthalmoscopy was undertaken, which included color photography and fluorescein angiography if there were new symptoms. Loss ofvisual acuity was recorded, and any new lesions at the macula were identified.
Results
Of the 43 patients included in the study, twowere seen for only one year, and two more werewithdrawn from analysis at the end of one yearbecause they received prophylactic photocoagulation to Bruch's membrane at that time. Theprophylactic photocoagulation was undertakenin the good eye in an attempt to prevent pigment epithelial detachment. Thus 43 patientswere examined at intervals for one year, and 39patients were followed up thereafter. The average age at the time of the initial tear was 70years; 27 patients were women, and 13 patientswere men.
Thirty-six patients were reexamined untilvisual loss occurred. No patients had visualloss from a cause other than age-related macular disease, and in no patient was a macularlesion identified that was amenable to photocoagulation. The seven patients who retainedgood visual acuity (20/40 or better) included thetwo who received prophylactic laser treatmentand the two who were followed up for only oneyear. The remaining three have been followed
up for seven, eight, and 13 years after the initialevent.
In the first year of follow-up, 16 of 43 patientslost visual acuity (37%) in the fellow eye. Visualacuity was lost in seven of the 23 patients (30%)in the second year, and in eight of the remaining 16 patients (50%) in the third year. Additionally, one patient lost visual acuity in thefourth year, one in the fifth year, two in thesixth year, and one in the seventh year. Thecumulative loss of fellow-eye visual acuity was37% in the first year, 59% in two years, and 80%after three years.
Visual loss in the fellow eye was most frequently precipitated by detachment of the pigment epithelium. In 23 eyes, pigment epithelialdetachments developed. Of these, six had welldefined subpigment epithelial new vessels apparent on angiographic examination, and 11had indirect evidence of neovascularization asshown by subretinal hemorrhage or exudateand notching before visual loss. In 15 of these23 eyes, a tear supervened. An additional sixpatients had tears of detached pigment epithelium at the time of visual loss in the fellow eyewithout our seeing the initial lesion.
Two patients lost vision from primary subretinal neovascularization, and an additional twohad disciform scars, making it impossible todistinguish between detachment of the pigment epithelium and choroidal neovascularization as the initiating event. Three patients developed geographic atrophy; in each patient,we had observed shallow pigment epithelialdetachments associated with soft drusen beforevisual loss.
Discussion
We believe that the high risk in the fellow eyein patients with a tear in the first eye representsthe natural history of the disorder. The ascertainment of patients was complete with theexception of the two who died and the two wholeft the country. The criteria for inclusion inthis study allowed only patients without evidence of exudative maculopathy in the felloweye. Visual loss was defined as reduction ofvisual acuity to 20/80; in some patients, weobserved the lesion that caused visual loss forsome time before the visual acuity deterioratedto this level. It is unlikely, therefore, that therisk has been overestimated compared to otherstudies. There is considerable variability in the
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protocol of previous investigations. One studyestablished loss of visual acuity as the endpoint." whereas others used the developmentof a lesion likely to cause visual loss. 1,2,4-6 Somedata represent a cumulative risk over a setnumber of years, I,;! whereas others represent anannual risk.t" Our data imply a risk of felloweye involvement in this subset of patients thatis greater than twice that in patients with exudative maculopathy in general.
Complications of pigment epithelial detachment accounted for the visual loss in mostpatients, indicating that the lesion in the felloweye mirrored the lesion in the first. Most, butnot all, pigment epithelial detachments eventually tore. This propensity for bilateral tears wasobserved previously."
The findings of this study are in accord withthe concept of differential risk in patients withage-related macular degeneration, which is determined by variation in the density, site, andchemical composition of drusen. 4,6-11 It has beenproposed that the characteristics of drusen determine the form of lesion that may occur inresponse to Bruch's membrane change. It hasalso been recognized that symmetry exists between the two eyes in clinically detectableBruch's membrane changes3,4,6,7 despite the considerable variation that exists between theeyes. Thus it is not surprising that a correlationexists between the form of the lesion in oneeye, and the form and magnitude of risk in theother.
If the magnitude of risk for visual loss in thesubset of patients with pigment epithelial tearsis so high, there is a need to seek a logicalapproach to prophylactic therapy. It would bevaluable to ascertain the risk factors. An analysis of drusen in the fellow eye of patients withtears of the retinal pigment epithelium showedthem to be confluent and hypofluorescent onfluorescein angiography." It has been suggested that the hypofluorescence implies extensivelipid deposition in Bruch's membrane, whichwould impede water flow and predispose thepigment epithelium to detach." These findingsimply that attempts at prophylaxis should bedirected toward reducing the volume of waterpumped by the pigment epithelium, or increasing the hydraulic conductivity of Bruch's membrane.
References
1. Teeters, V. W., and Bird, A. c.. The development of neovascularization of senile disciform macular degeneration. Am. J. Ophthalmol. 76:1, 1973.
2. Chandra, S. R., Gragoudas, E. 5., Friedman,E., Van Buskirk, E. M., and Klein, M. L.: Naturalhistory of disciform degeneration of the macula. Am.I. Ophthalmol. 78:579, 1974.
3. Gass, J. D M.: Drusen and disciform maculardetachment and degeneration. Arch. Ophthalmol.90:206, 1973.
4. Gregor, A., Bird, A. c., and Chisholm, 1. H.:Senile disciform macular degeneration in the secondeye. Br. J. Ophthalmol. 61:141, 1977.
5. Bressler,S, B., Bressler, N. M., Fine, S. L.,Hillis, A., Murphy, R. P., Olk, R. J., and Patz, A.:Natural course of choroidal neovascular membraneswithin the foveal avascular zone in senile maculardegeneration. Am. J. Ophthalmol. 93:157, 1982.
6. Strahlman, E., Fine, S. L., and Hillis, A.: Thesecond eye of patients with senile macular degeneration. Arch. Ophthalmol. 101:1191, 1983.
7. Gragoudas, E. 5., Chandra, S. R., Freidman,E., Klein, M, L., and Van Buskirk, M.: Disciformdegeneration of the macula. II. Pathogenesis. Arch.Ophthalmol. 94:755, 1976.
8. Siddy, W. E., and Fine, S. L.: Prognosis of patients with bilateral macular drusen. Ophthalmology91:271, 1984.
9. Bressler, N. M., Bressler, S. B., Seddon, I. M.,Gragoudas, E. 5., and Jacobson, L.: Clinicalcharacteristics of drusen in patients with exudativeversus non-exudative age-related macular degeneration. Retina 8:109, 1988.
10. Pauleikhoff, D., Marshall, J., and Bird, A. c..Histochemical and morphological correlation of aging changes in Bruch's membrane. ARVO abstracts.Supplement to Invest. Ophthalmol. Vis. Sci. Philadelphia, J. B. Lippincott, 1989, p. 153.
11. Bird, A. C,; and Marshall, J.: Retinal pigmentepithelial detachments in the elderly. Trans. Ophthalmol. Soc. U.K. 105:674, 1986.
12. Hoskin, A., Bird, A. c., and Sehrni, K.: Tearsof detached retinal pigment epithelium. Br. J. Ophthalmol. 65:417, 1981.
13. Chuang, E. L., and Bird, A. c.. Bilaterality oftears of the retinal pigment epithelium. Br. J. Ophthalmol. 72:417, 1988.
14. --:Repair after tears of the retinal pigmentepithelium. Eye 2:106, 1988.
15. --:The pathogenesis of tears of the retinalpigment epithelium. Am. J. Ophthalmol. 105:285,1988.