A randomized, placebo-controlled, clinical trial of high-dose supplementation with vitamins C and E, beta carotene, and zinc for age-related macular degeneration and vision loss: AREDS report no. 8

A. Kassoff; J. Kassoff; J. Buehler; M. Eglow; F. Kaufman; M. Mehu; S. Kieval; M. Mairs; B. Graig; A. Quattrocchi; D. Jones; J. Locatelli; A. Ruby; Jr Capon A.; B. Garretson; T. Hassan; M. T. Trese; G. A. Williams; V. Regan; P. Manatrey; P. Streasick; L. Szydlowski; F. McIver; C. Bridges; C. Stanley; K. Cumming; B. Lewis; M. Zajechowski; R. R. Margherio; M. S. Cox; J. C. Werner; R. Falk; P. Siedlak; C. Neubert; M. L. Klein; J. T. Stout; A. O'Malley; A. K. Lauer; J. E. Robertson; D. J. Wilson; C. Beardsley; H. Anderson; P. Wallace; G. Smith; S. Howard; R. F. Dreyer; C. Ma; R. G. Chenoweth; J. D. Zilis; M. Johnson; P. Rice; H. Daniel; H. Crider; S. Parker; K. Sherman; D. F. Martin; Sr Aaberg; Jr Sternberg P.; L. T. Curtis; B. Ju; J. Gilman; B. Myles; S. Strittman; C. Gentry; H. Yi; Jr Capone A.; M. Lambert; T. Meredith; Jr Aaberg; D. Saperstein; J. I. Lim; B. Stribling; D. Armiger; R. Swords; D. H. Orth; T. P. Flood; J. Civantos; S. Debustros; K. H. Packo; P. T. Merrill; J. A. Cohen; C. Figliulo; C. Morrison; D. A. Bryant; D. Doherty; M. McVicker; T. Drefcinski; J. M. Seddon; M. K. Pinnolis; N. Davis; I. Burton; T. Taitsel; D. Walsh; J. Dubois-Moran; C. Callahan; C. Evans; K. K. Snow; D. A. Jones-Devonish; V. D. Crouse

doi:10.1001/archopht.119.10.1417

A randomized, placebo-controlled, clinical trial of high-dose supplementation with vitamins C and E, beta carotene, and zinc for age-related macular degeneration and vision loss: AREDS report no. 8

A. Kassoff, J. Kassoff, J. Buehler, M. Eglow, F. Kaufman, M. Mehu, S. Kieval, M. Mairs, B. Graig, A. Quattrocchi, D. Jones, J. Locatelli, A. Ruby, Jr Capon A., B. Garretson, T. Hassan, M. T. Trese, G. A. Williams, V. Regan, P. ManatreyP. Streasick, L. Szydlowski, F. McIver, C. Bridges, C. Stanley, K. Cumming, B. Lewis, M. Zajechowski, R. R. Margherio, M. S. Cox, J. C. Werner, R. Falk, P. Siedlak, C. Neubert, M. L. Klein, J. T. Stout, A. O'Malley, A. K. Lauer, J. E. Robertson, D. J. Wilson, C. Beardsley, H. Anderson, P. Wallace, G. Smith, S. Howard, R. F. Dreyer, C. Ma, R. G. Chenoweth, J. D. Zilis, M. Johnson, P. Rice, H. Daniel, H. Crider, S. Parker, K. Sherman, D. F. Martin, Sr Aaberg, Jr Sternberg P., L. T. Curtis, B. Ju, J. Gilman, B. Myles, S. Strittman, C. Gentry, H. Yi, Jr Capone A., M. Lambert, T. Meredith, Jr Aaberg, D. Saperstein, J. I. Lim, B. Stribling, D. Armiger, R. Swords, D. H. Orth, T. P. Flood, J. Civantos, S. Debustros, K. H. Packo, P. T. Merrill, J. A. Cohen, C. Figliulo, C. Morrison, D. A. Bryant, D. Doherty, M. McVicker, T. Drefcinski, J. M. Seddon, M. K. Pinnolis, N. Davis, I. Burton, T. Taitsel, D. Walsh, J. Dubois-Moran, C. Callahan, C. Evans, K. K. Snow, D. A. Jones-Devonish, V. D. Crouse

Research output: Contribution to journal › Article › peer-review

2752 Scopus citations

Abstract

Background: Observational and experimental data suggest that antioxidant and/or zinc supplements may delay progression of age-related macular degeneration (AMD) and vision loss. Objective: To evaluate the effect of high-dose vitamins C and E, beta carotene, and zinc supplements on AMD progression and visual acuity. Design: The Age-Related Eye Disease Study, an 11-center double-masked clinical trial, enrolled participants in an AMD trial if they had extensive small drusen, intermediate drusen, large drusen, noncentral geographic atrophy, or pigment abnormalities in 1 or both eyes, or advanced AMD or vision loss due to AMD in 1 eye. At least 1 eye had best-corrected visual acuity of 20/32 or better. Participants were randomly assigned to receive daily oral tablets containing: (1) antioxidants (vitamin C, 500 mg; vitamin E, 400 IU; and beta carotene, 15 mg); (2) zinc, 80 mg, as zinc oxide and copper, 2 mg, as cupric oxide; (3) antioxidants plus zinc; or (4) placebo. Main Outcome Measures: (1)Photographic assessment of progression to or treatment for advanced AMD and (2) at least moderate visual acuity loss from baseline (??≥15 letters). Primary analyses used repeated-measures logistic regression with a significance level of .01, unadjusted for covariates. Serum level measurements, medical histories, and mortality rates were used for safety monitoring. Results: Average follow-up of the 3640 enrolled study participants, aged 55-80 years, was 6.3 years, with 2.4% lost to follow-up. Comparison with placebo demonstrated a statistically significant odds reduction for the development of advanced AMD with antioxidants plus zinc (odds ratio [OR], 0.72; 99% confidence interval [CI], 0.52-0.98). The ORs for zinc alone and antioxidants alone are 0.75 (99% CI, 0.55-1.03) and 0.80 (99% CI, 0.59-1.09), respectively. Participants with extensive small drusen, nonextensive intermediate size drusen, or pigment abnormalities had only a 1.3% 5-year probability of progression to advanced AMD. Odds reduction estimates increased when these 1063 participants were excluded (antioxidants plus zinc: OR, 0.66; 99% CI, 0.47-0.91; zinc: OR, 0.71; 99% CI, 0.52-0.99; antioxidants: OR, 0.76; 99% CI, 0.55-1.05). Both zinc and antioxidants plus zinc significantly reduced the odds of developing advanced AMD in this higher-risk group. The only statistically significant reduction in rates of at least moderate visual acuity loss occurred in persons assigned to receive antioxidants plus zinc (OR, 0.73; 99% CI, 0.54-0.99). No statistically significant serious adverse effect was associated with any of the formulations. Conclusions: Persons older than 55 years should have dilated eye examinations to determine their risk of developing advanced AMD. Those with extensive intermediate size drusen, at least 1 large druse, noncentral geographic atrophy in 1 or both eyes, or advanced AMD or vision loss due to AMD in 1 eye, and without contraindications such as smoking, should consider taking a supplement of antioxidants plus zinc such as that used in this study.

Original language	English (US)
Pages (from-to)	1417-1436
Number of pages	20
Journal	Archives of ophthalmology
Volume	119
Issue number	10
DOIs	https://doi.org/10.1001/archopht.119.10.1417
State	Published - 2001
Externally published	Yes

ASJC Scopus subject areas

Ophthalmology

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10.1001/archopht.119.10.1417

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Kassoff, A., Kassoff, J., Buehler, J., Eglow, M., Kaufman, F., Mehu, M., Kieval, S., Mairs, M., Graig, B., Quattrocchi, A., Jones, D., Locatelli, J., Ruby, A., Capon A., J., Garretson, B., Hassan, T., Trese, M. T., Williams, G. A., Regan, V., ... Crouse, V. D. (2001). A randomized, placebo-controlled, clinical trial of high-dose supplementation with vitamins C and E, beta carotene, and zinc for age-related macular degeneration and vision loss: AREDS report no. 8. Archives of ophthalmology, 119(10), 1417-1436. https://doi.org/10.1001/archopht.119.10.1417

A randomized, placebo-controlled, clinical trial of high-dose supplementation with vitamins C and E, beta carotene, and zinc for age-related macular degeneration and vision loss: AREDS report no. 8. / Kassoff, A.; Kassoff, J.; Buehler, J. et al.
In: Archives of ophthalmology, Vol. 119, No. 10, 2001, p. 1417-1436.

Research output: Contribution to journal › Article › peer-review

Kassoff, A, Kassoff, J, Buehler, J, Eglow, M, Kaufman, F, Mehu, M, Kieval, S, Mairs, M, Graig, B, Quattrocchi, A, Jones, D, Locatelli, J, Ruby, A, Capon A., J, Garretson, B, Hassan, T, Trese, MT, Williams, GA, Regan, V, Manatrey, P, Streasick, P, Szydlowski, L, McIver, F, Bridges, C, Stanley, C, Cumming, K, Lewis, B, Zajechowski, M, Margherio, RR, Cox, MS, Werner, JC, Falk, R, Siedlak, P, Neubert, C, Klein, ML, Stout, JT, O'Malley, A, Lauer, AK, Robertson, JE, Wilson, DJ, Beardsley, C, Anderson, H, Wallace, P, Smith, G, Howard, S, Dreyer, RF, Ma, C, Chenoweth, RG, Zilis, JD, Johnson, M, Rice, P, Daniel, H, Crider, H, Parker, S, Sherman, K, Martin, DF, Aaberg, S, Sternberg P., J, Curtis, LT, Ju, B, Gilman, J, Myles, B, Strittman, S, Gentry, C, Yi, H, Capone A., J, Lambert, M, Meredith, T, Aaberg, J, Saperstein, D, Lim, JI, Stribling, B, Armiger, D, Swords, R, Orth, DH, Flood, TP, Civantos, J, Debustros, S, Packo, KH, Merrill, PT, Cohen, JA, Figliulo, C, Morrison, C, Bryant, DA, Doherty, D, McVicker, M, Drefcinski, T, Seddon, JM, Pinnolis, MK, Davis, N, Burton, I, Taitsel, T, Walsh, D, Dubois-Moran, J, Callahan, C, Evans, C, Snow, KK, Jones-Devonish, DA & Crouse, VD 2001, 'A randomized, placebo-controlled, clinical trial of high-dose supplementation with vitamins C and E, beta carotene, and zinc for age-related macular degeneration and vision loss: AREDS report no. 8', Archives of ophthalmology, vol. 119, no. 10, pp. 1417-1436. https://doi.org/10.1001/archopht.119.10.1417

@article{7f7f044298cd4819bb1f1ae3e8aecd1c,

title = "A randomized, placebo-controlled, clinical trial of high-dose supplementation with vitamins C and E, beta carotene, and zinc for age-related macular degeneration and vision loss: AREDS report no. 8",

abstract = "Background: Observational and experimental data suggest that antioxidant and/or zinc supplements may delay progression of age-related macular degeneration (AMD) and vision loss. Objective: To evaluate the effect of high-dose vitamins C and E, beta carotene, and zinc supplements on AMD progression and visual acuity. Design: The Age-Related Eye Disease Study, an 11-center double-masked clinical trial, enrolled participants in an AMD trial if they had extensive small drusen, intermediate drusen, large drusen, noncentral geographic atrophy, or pigment abnormalities in 1 or both eyes, or advanced AMD or vision loss due to AMD in 1 eye. At least 1 eye had best-corrected visual acuity of 20/32 or better. Participants were randomly assigned to receive daily oral tablets containing: (1) antioxidants (vitamin C, 500 mg; vitamin E, 400 IU; and beta carotene, 15 mg); (2) zinc, 80 mg, as zinc oxide and copper, 2 mg, as cupric oxide; (3) antioxidants plus zinc; or (4) placebo. Main Outcome Measures: (1)Photographic assessment of progression to or treatment for advanced AMD and (2) at least moderate visual acuity loss from baseline (??≥15 letters). Primary analyses used repeated-measures logistic regression with a significance level of .01, unadjusted for covariates. Serum level measurements, medical histories, and mortality rates were used for safety monitoring. Results: Average follow-up of the 3640 enrolled study participants, aged 55-80 years, was 6.3 years, with 2.4% lost to follow-up. Comparison with placebo demonstrated a statistically significant odds reduction for the development of advanced AMD with antioxidants plus zinc (odds ratio [OR], 0.72; 99% confidence interval [CI], 0.52-0.98). The ORs for zinc alone and antioxidants alone are 0.75 (99% CI, 0.55-1.03) and 0.80 (99% CI, 0.59-1.09), respectively. Participants with extensive small drusen, nonextensive intermediate size drusen, or pigment abnormalities had only a 1.3% 5-year probability of progression to advanced AMD. Odds reduction estimates increased when these 1063 participants were excluded (antioxidants plus zinc: OR, 0.66; 99% CI, 0.47-0.91; zinc: OR, 0.71; 99% CI, 0.52-0.99; antioxidants: OR, 0.76; 99% CI, 0.55-1.05). Both zinc and antioxidants plus zinc significantly reduced the odds of developing advanced AMD in this higher-risk group. The only statistically significant reduction in rates of at least moderate visual acuity loss occurred in persons assigned to receive antioxidants plus zinc (OR, 0.73; 99% CI, 0.54-0.99). No statistically significant serious adverse effect was associated with any of the formulations. Conclusions: Persons older than 55 years should have dilated eye examinations to determine their risk of developing advanced AMD. Those with extensive intermediate size drusen, at least 1 large druse, noncentral geographic atrophy in 1 or both eyes, or advanced AMD or vision loss due to AMD in 1 eye, and without contraindications such as smoking, should consider taking a supplement of antioxidants plus zinc such as that used in this study.",

author = "A. Kassoff and J. Kassoff and J. Buehler and M. Eglow and F. Kaufman and M. Mehu and S. Kieval and M. Mairs and B. Graig and A. Quattrocchi and D. Jones and J. Locatelli and A. Ruby and {Capon A.}, Jr and B. Garretson and T. Hassan and Trese, {M. T.} and Williams, {G. A.} and V. Regan and P. Manatrey and P. Streasick and L. Szydlowski and F. McIver and C. Bridges and C. Stanley and K. Cumming and B. Lewis and M. Zajechowski and Margherio, {R. R.} and Cox, {M. S.} and Werner, {J. C.} and R. Falk and P. Siedlak and C. Neubert and Klein, {M. L.} and Stout, {J. T.} and A. O'Malley and Lauer, {A. K.} and Robertson, {J. E.} and Wilson, {D. J.} and C. Beardsley and H. Anderson and P. Wallace and G. Smith and S. Howard and Dreyer, {R. F.} and C. Ma and Chenoweth, {R. G.} and Zilis, {J. D.} and M. Johnson and P. Rice and H. Daniel and H. Crider and S. Parker and K. Sherman and Martin, {D. F.} and Sr Aaberg and {Sternberg P.}, Jr and Curtis, {L. T.} and B. Ju and J. Gilman and B. Myles and S. Strittman and C. Gentry and H. Yi and {Capone A.}, Jr and M. Lambert and T. Meredith and Jr Aaberg and D. Saperstein and Lim, {J. I.} and B. Stribling and D. Armiger and R. Swords and Orth, {D. H.} and Flood, {T. P.} and J. Civantos and S. Debustros and Packo, {K. H.} and Merrill, {P. T.} and Cohen, {J. A.} and C. Figliulo and C. Morrison and Bryant, {D. A.} and D. Doherty and M. McVicker and T. Drefcinski and Seddon, {J. M.} and Pinnolis, {M. K.} and N. Davis and I. Burton and T. Taitsel and D. Walsh and J. Dubois-Moran and C. Callahan and C. Evans and Snow, {K. K.} and Jones-Devonish, {D. A.} and Crouse, {V. D.}",

year = "2001",

doi = "10.1001/archopht.119.10.1417",

language = "English (US)",

volume = "119",

pages = "1417--1436",

journal = "Archives of ophthalmology",

issn = "0003-9950",

publisher = "American Medical Association",

number = "10",

}

TY - JOUR

T1 - A randomized, placebo-controlled, clinical trial of high-dose supplementation with vitamins C and E, beta carotene, and zinc for age-related macular degeneration and vision loss

T2 - AREDS report no. 8

AU - Kassoff, A.

AU - Kassoff, J.

AU - Buehler, J.

AU - Eglow, M.

AU - Kaufman, F.

AU - Mehu, M.

AU - Kieval, S.

AU - Mairs, M.

AU - Graig, B.

AU - Quattrocchi, A.

AU - Jones, D.

AU - Locatelli, J.

AU - Ruby, A.

AU - Capon A., Jr

AU - Garretson, B.

AU - Hassan, T.

AU - Trese, M. T.

AU - Williams, G. A.

AU - Regan, V.

AU - Manatrey, P.

AU - Streasick, P.

AU - Szydlowski, L.

AU - McIver, F.

AU - Bridges, C.

AU - Stanley, C.

AU - Cumming, K.

AU - Lewis, B.

AU - Zajechowski, M.

AU - Margherio, R. R.

AU - Cox, M. S.

AU - Werner, J. C.

AU - Falk, R.

AU - Siedlak, P.

AU - Neubert, C.

AU - Klein, M. L.

AU - Stout, J. T.

AU - O'Malley, A.

AU - Lauer, A. K.

AU - Robertson, J. E.

AU - Wilson, D. J.

AU - Beardsley, C.

AU - Anderson, H.

AU - Wallace, P.

AU - Smith, G.

AU - Howard, S.

AU - Dreyer, R. F.

AU - Ma, C.

AU - Chenoweth, R. G.

AU - Zilis, J. D.

AU - Johnson, M.

AU - Rice, P.

AU - Daniel, H.

AU - Crider, H.

AU - Parker, S.

AU - Sherman, K.

AU - Martin, D. F.

AU - Aaberg, Sr

AU - Sternberg P., Jr

AU - Curtis, L. T.

AU - Ju, B.

AU - Gilman, J.

AU - Myles, B.

AU - Strittman, S.

AU - Gentry, C.

AU - Yi, H.

AU - Capone A., Jr

AU - Lambert, M.

AU - Meredith, T.

AU - Aaberg, Jr

AU - Saperstein, D.

AU - Lim, J. I.

AU - Stribling, B.

AU - Armiger, D.

AU - Swords, R.

AU - Orth, D. H.

AU - Flood, T. P.

AU - Civantos, J.

AU - Debustros, S.

AU - Packo, K. H.

AU - Merrill, P. T.

AU - Cohen, J. A.

AU - Figliulo, C.

AU - Morrison, C.

AU - Bryant, D. A.

AU - Doherty, D.

AU - McVicker, M.

AU - Drefcinski, T.

AU - Seddon, J. M.

AU - Pinnolis, M. K.

AU - Davis, N.

AU - Burton, I.

AU - Taitsel, T.

AU - Walsh, D.

AU - Dubois-Moran, J.

AU - Callahan, C.

AU - Evans, C.

AU - Snow, K. K.

AU - Jones-Devonish, D. A.

AU - Crouse, V. D.

PY - 2001

Y1 - 2001

N2 - Background: Observational and experimental data suggest that antioxidant and/or zinc supplements may delay progression of age-related macular degeneration (AMD) and vision loss. Objective: To evaluate the effect of high-dose vitamins C and E, beta carotene, and zinc supplements on AMD progression and visual acuity. Design: The Age-Related Eye Disease Study, an 11-center double-masked clinical trial, enrolled participants in an AMD trial if they had extensive small drusen, intermediate drusen, large drusen, noncentral geographic atrophy, or pigment abnormalities in 1 or both eyes, or advanced AMD or vision loss due to AMD in 1 eye. At least 1 eye had best-corrected visual acuity of 20/32 or better. Participants were randomly assigned to receive daily oral tablets containing: (1) antioxidants (vitamin C, 500 mg; vitamin E, 400 IU; and beta carotene, 15 mg); (2) zinc, 80 mg, as zinc oxide and copper, 2 mg, as cupric oxide; (3) antioxidants plus zinc; or (4) placebo. Main Outcome Measures: (1)Photographic assessment of progression to or treatment for advanced AMD and (2) at least moderate visual acuity loss from baseline (??≥15 letters). Primary analyses used repeated-measures logistic regression with a significance level of .01, unadjusted for covariates. Serum level measurements, medical histories, and mortality rates were used for safety monitoring. Results: Average follow-up of the 3640 enrolled study participants, aged 55-80 years, was 6.3 years, with 2.4% lost to follow-up. Comparison with placebo demonstrated a statistically significant odds reduction for the development of advanced AMD with antioxidants plus zinc (odds ratio [OR], 0.72; 99% confidence interval [CI], 0.52-0.98). The ORs for zinc alone and antioxidants alone are 0.75 (99% CI, 0.55-1.03) and 0.80 (99% CI, 0.59-1.09), respectively. Participants with extensive small drusen, nonextensive intermediate size drusen, or pigment abnormalities had only a 1.3% 5-year probability of progression to advanced AMD. Odds reduction estimates increased when these 1063 participants were excluded (antioxidants plus zinc: OR, 0.66; 99% CI, 0.47-0.91; zinc: OR, 0.71; 99% CI, 0.52-0.99; antioxidants: OR, 0.76; 99% CI, 0.55-1.05). Both zinc and antioxidants plus zinc significantly reduced the odds of developing advanced AMD in this higher-risk group. The only statistically significant reduction in rates of at least moderate visual acuity loss occurred in persons assigned to receive antioxidants plus zinc (OR, 0.73; 99% CI, 0.54-0.99). No statistically significant serious adverse effect was associated with any of the formulations. Conclusions: Persons older than 55 years should have dilated eye examinations to determine their risk of developing advanced AMD. Those with extensive intermediate size drusen, at least 1 large druse, noncentral geographic atrophy in 1 or both eyes, or advanced AMD or vision loss due to AMD in 1 eye, and without contraindications such as smoking, should consider taking a supplement of antioxidants plus zinc such as that used in this study.

AB - Background: Observational and experimental data suggest that antioxidant and/or zinc supplements may delay progression of age-related macular degeneration (AMD) and vision loss. Objective: To evaluate the effect of high-dose vitamins C and E, beta carotene, and zinc supplements on AMD progression and visual acuity. Design: The Age-Related Eye Disease Study, an 11-center double-masked clinical trial, enrolled participants in an AMD trial if they had extensive small drusen, intermediate drusen, large drusen, noncentral geographic atrophy, or pigment abnormalities in 1 or both eyes, or advanced AMD or vision loss due to AMD in 1 eye. At least 1 eye had best-corrected visual acuity of 20/32 or better. Participants were randomly assigned to receive daily oral tablets containing: (1) antioxidants (vitamin C, 500 mg; vitamin E, 400 IU; and beta carotene, 15 mg); (2) zinc, 80 mg, as zinc oxide and copper, 2 mg, as cupric oxide; (3) antioxidants plus zinc; or (4) placebo. Main Outcome Measures: (1)Photographic assessment of progression to or treatment for advanced AMD and (2) at least moderate visual acuity loss from baseline (??≥15 letters). Primary analyses used repeated-measures logistic regression with a significance level of .01, unadjusted for covariates. Serum level measurements, medical histories, and mortality rates were used for safety monitoring. Results: Average follow-up of the 3640 enrolled study participants, aged 55-80 years, was 6.3 years, with 2.4% lost to follow-up. Comparison with placebo demonstrated a statistically significant odds reduction for the development of advanced AMD with antioxidants plus zinc (odds ratio [OR], 0.72; 99% confidence interval [CI], 0.52-0.98). The ORs for zinc alone and antioxidants alone are 0.75 (99% CI, 0.55-1.03) and 0.80 (99% CI, 0.59-1.09), respectively. Participants with extensive small drusen, nonextensive intermediate size drusen, or pigment abnormalities had only a 1.3% 5-year probability of progression to advanced AMD. Odds reduction estimates increased when these 1063 participants were excluded (antioxidants plus zinc: OR, 0.66; 99% CI, 0.47-0.91; zinc: OR, 0.71; 99% CI, 0.52-0.99; antioxidants: OR, 0.76; 99% CI, 0.55-1.05). Both zinc and antioxidants plus zinc significantly reduced the odds of developing advanced AMD in this higher-risk group. The only statistically significant reduction in rates of at least moderate visual acuity loss occurred in persons assigned to receive antioxidants plus zinc (OR, 0.73; 99% CI, 0.54-0.99). No statistically significant serious adverse effect was associated with any of the formulations. Conclusions: Persons older than 55 years should have dilated eye examinations to determine their risk of developing advanced AMD. Those with extensive intermediate size drusen, at least 1 large druse, noncentral geographic atrophy in 1 or both eyes, or advanced AMD or vision loss due to AMD in 1 eye, and without contraindications such as smoking, should consider taking a supplement of antioxidants plus zinc such as that used in this study.

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UR - http://www.scopus.com/inward/citedby.url?scp=0034800655&partnerID=8YFLogxK

U2 - 10.1001/archopht.119.10.1417

DO - 10.1001/archopht.119.10.1417

M3 - Article

C2 - 11594942

AN - SCOPUS:0034800655

SN - 0003-9950

VL - 119

SP - 1417

EP - 1436

JO - Archives of ophthalmology

JF - Archives of ophthalmology

IS - 10

ER -

A randomized, placebo-controlled, clinical trial of high-dose supplementation with vitamins C and E, beta carotene, and zinc for age-related macular degeneration and vision loss: AREDS report no. 8

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