Your search keyword '"Rosenfeld, P.J."' showing total 4 results

1. Reply

Author

Hibert, M.L., primary, Chen, Y.I., additional, Ohringer, N., additional, Wilbur, L.R., additional, Waheed, N.K., additional, Heier, J.S, additional, Calhoun, M.W., additional, Rosenfeld, P.J., additional, and Polimeni, J.R., additional

Published

2022

2. Altered Blood Flow in the Ophthalmic and Internal Carotid Arteries in Patients with Age-Related Macular Degeneration Measured Using Noncontrast MR Angiography at 7T

Author

Hibert, M.L., primary, Chen, Y.I., additional, Ohringer, N., additional, Feuer, W.J., additional, Waheed, N.K., additional, Heier, J.S., additional, Calhoun, M.W., additional, Rosenfeld, P.J., additional, and Polimeni, J.R., additional

Published

2021

3. Progression of Geographic Atrophy in Age-related Macular Degeneration: AREDS2 Report Number 16

Author

Keenan, T.D., Agron, E., Domalpally, A., Clemons, T.E., Asten, F. van, Wong, W.T., Danis, R.G., Sadda, S., Rosenfeld, P.J., Klein, M.L., Ratnapriya, R., Swaroop, A., Ferris, F.L., 3rd, and Chew, E.Y.

Subjects

genetic structures, Sensory disorders Donders Center for Medical Neuroscience [Radboudumc 12], eye diseases

Abstract

Item does not contain fulltext PURPOSE: To analyze the prevalence, incidence, and clinical characteristics of eyes with geographic atrophy (GA) in age-related macular degeneration (AMD), including clinical and genetic factors affecting enlargement. DESIGN: Prospective cohort study within a controlled clinical trial. PARTICIPANTS: Age-Related Eye Disease Study 2 (AREDS2) participants, aged 50-85 years. METHODS: Baseline and annual stereoscopic color fundus photographs were evaluated for GA presence and area. Analyses included GA prevalence and incidence rates, Kaplan-Meier rates, mixed-model regression, and multivariable analysis of the square root of GA, area adjusted for covariates, including clinical/imaging characteristics and genotype. MAIN OUTCOME MEASURES: (1) Presence or development of GA; (2) change in the square root of GA area over time. RESULTS: At baseline, 517 eyes (6.2%) of 411 participants (9.8%) had pre-existing GA (without neovascular AMD), with the following characteristics: 33% central, 67% noncentral; and the following configurations: 36% small, 26% solid/unifocal, 24% multifocal, 9% horseshoe/ring, and 6% indeterminate. Of the remaining 6530 eyes at risk, 1099 eyes (17.3%) of 883 participants developed incident GA without prior neovascular disease during mean follow-up of 4.4 years. The Kaplan-Meier rate of incident GA was 19% of eyes at 5 years. In eyes with incident GA, 4-year risk of subsequent neovascular AMD was 29%. In eyes with incident noncentral GA, 4-year risk of central involvement was 57%. GA enlargement rate (following square root transformation) was similar in eyes with pre-existing GA (0.29 mm/year; 95% confidence interval 0.27-0.30) and incident GA (0.28 mm/year; 0.27-0.30). In the combined group, GA enlargement was significantly faster with noncentrality, multifocality, intermediate baseline size, and bilateral GA (P < 0.0001 for interaction in each case) but not with AREDS2 treatment assignment (P = 0.33) or smoking status (P = 0.05). Enlargement was significantly faster with ARMS2 risk (P < 0.0001), C3 non-risk (P = 0.0002), and APOE non-risk (P = 0.001) genotypes. CONCLUSIONS: Analyses of AREDS2 data on natural history of GA provide representative data on GA evolution and enlargement. GA enlargement, which was influenced by lesion features, was relentless, resulting in rapid central vision loss. The genetic variants associated with faster enlargement were partially distinct from those associated with risk of incident GA. These findings are relevant to further investigations of GA pathogenesis and clinical trial planning.

Published

2018

4. Imaging Protocols in Clinical Studies in Advanced Age-Related Macular Degeneration: Recommendations from Classification of Atrophy Consensus Meetings

Author

Holz, F.G., Sadda, S.R., Staurenghi, G., Lindner, M., Bird, A.C., Blodi, B.A., Bottoni, F., Chakravarthy, U., Chew, E.Y., Csaky, K., Curcio, C.A., Danis, R., Fleckenstein, M., Freund, K.B., Grunwald, J., Guymer, R., Hoyng, C.B., Jaffe, G.J., Liakopoulos, S., Mones, J.M., Oishi, A., Pauleikhoff, D., Rosenfeld, P.J., Sarraf, D., Spaide, R.F., Tadayoni, R., Tufail, A., Wolf, S., and Schmitz-Valckenberg, S.

Subjects

Indocyanine Green, Male, genetic structures, Optical Imaging, Retinal Pigment Epithelium, Multimodal Imaging, Sensory disorders Donders Center for Medical Neuroscience [Radboudumc 12], eye diseases, Clinical Protocols, Geographic Atrophy, Photography, Wet Macular Degeneration, Humans, Female, sense organs, Fluorescein Angiography, 610 Medicine & health, Tomography, Optical Coherence, Aged

Abstract

Item does not contain fulltext PURPOSE: To summarize the results of 2 consensus meetings (Classification of Atrophy Meeting [CAM]) on conventional and advanced imaging modalities used to detect and quantify atrophy due to late-stage non-neovascular and neovascular age-related macular degeneration (AMD) and to provide recommendations on the use of these modalities in natural history studies and interventional clinical trials. DESIGN: Systematic debate on the relevance of distinct imaging modalities held in 2 consensus meetings. PARTICIPANTS: A panel of retina specialists. METHODS: During the CAM, a consortium of international experts evaluated the advantages and disadvantages of various imaging modalities on the basis of the collective analysis of a large series of clinical cases. A systematic discussion on the role of each modality in future studies in non-neovascular and neovascular AMD was held. MAIN OUTCOME MEASURES: Advantages and disadvantages of current retinal imaging technologies and recommendations for their use in advanced AMD trials. RESULTS: Imaging protocols to detect, quantify, and monitor progression of atrophy should include color fundus photography (CFP), confocal fundus autofluorescence (FAF), confocal near-infrared reflectance (NIR), and high-resolution optical coherence tomography volume scans. These images should be acquired at regular intervals throughout the study. In studies of non-neovascular AMD (without evident signs of active or regressed neovascularization [NV] at baseline), CFP may be sufficient at baseline and end-of-study visit. Fluorescein angiography (FA) may become necessary to evaluate for NV at any visit during the study. Indocyanine-green angiography (ICG-A) may be considered at baseline under certain conditions. For studies in patients with neovascular AMD, increased need for visualization of the vasculature must be taken into account. Accordingly, these studies should include FA (recommended at baseline and selected follow-up visits) and ICG-A under certain conditions. CONCLUSIONS: A multimodal imaging approach is recommended in clinical studies for the optimal detection and measurement of atrophy and its associated features. Specific validation studies will be necessary to determine the best combination of imaging modalities, and these recommendations will need to be updated as new imaging technologies become available in the future.

Published

2017