J Savige1,2, L Amos1, Frank Ierino3, H G Mack4, R C Andrew Symons5,6, P Hughes2, K Nicholls2, D Colville1. 1. a University of Melbourne Department of Medicine , Melbourne Health and Northern Health, Royal Melbourne Hospital , Parkville , Victoria , Australia. 2. b Department of Nephrology , Royal Melbourne Hospital , Parkville , Victoria , Australia. 3. c Department of Nephrology , Austin Health , Heidelberg , Victoria , Australia. 4. d University of Melbourne Department of Ophthalmology , Royal Victorian Eye and Ear Hospital , East Melbourne , Victoria , Australia. 5. e Department of Ophthalmology , Royal Melbourne Hospital , Parkville Victoria , Australia. 6. f University of Melbourne Department of Surgery , Royal Melbourne Hospital , Parkville Victoria , Australia.
Abstract
BACKGROUND: Dense deposit disease and atypical hemolytic uremic syndrome are often caused by Complement Factor H (CFH) mutations. This study describes the retinal abnormalities in dense deposit disease and, for the first time, atypical haemolytic uremic syndrome. It also reviews our understanding of drusen pathogenesis and their relevance for glomerular disease. METHODS: Six individuals with dense deposit disease and one with atypical haemolytic uremic syndrome were studied from 2 to 40 years after presentation. Five had renal transplants. All four who had genetic testing had CFH mutations. Individuals underwent ophthalmological review and retinal photography, and in some cases, optical coherence tomography, and further tests of retinal function. RESULTS: All subjects with dense deposit disease had impaired night vision and retinal drusen or whitish-yellow deposits. Retinal atrophy, pigmentation, and hemorrhage were common. In late disease, peripheral vision was restricted, central vision was distorted, and there were scotoma from sub-retinal choroidal neovascular membranes and atypical serous retinopathy. Drusen were present but less prominent in the young person with atypical uremic syndrome due to a heterozygous CFH mutation. CONCLUSIONS: Drusen are common in forms of C3 glomerulopathy caused by compound heterozygous or heterozygous CFH mutations. They are useful diagnostically but also impair vision. Drusen have an identical composition to glomerular deposits. They are also identical to the drusen of age-related macular degeneration, and may respond to the same treatments. Individuals with a C3 glomerulopathy should be assessed ophthalmologically at diagnosis, and monitored regularly for vision-threatening complications.
BACKGROUND: Dense deposit disease and atypical hemolytic uremic syndrome are often caused by Complement Factor H (CFH) mutations. This study describes the retinal abnormalities in dense deposit disease and, for the first time, atypical haemolytic uremic syndrome. It also reviews our understanding of drusen pathogenesis and their relevance for glomerular disease. METHODS: Six individuals with dense deposit disease and one with atypical haemolytic uremic syndrome were studied from 2 to 40 years after presentation. Five had renal transplants. All four who had genetic testing had CFH mutations. Individuals underwent ophthalmological review and retinal photography, and in some cases, optical coherence tomography, and further tests of retinal function. RESULTS: All subjects with dense deposit disease had impaired night vision and retinal drusen or whitish-yellow deposits. Retinal atrophy, pigmentation, and hemorrhage were common. In late disease, peripheral vision was restricted, central vision was distorted, and there were scotoma from sub-retinal choroidal neovascular membranes and atypical serous retinopathy. Drusen were present but less prominent in the young person with atypical uremic syndrome due to a heterozygous CFH mutation. CONCLUSIONS: Drusen are common in forms of C3 glomerulopathy caused by compound heterozygous or heterozygous CFH mutations. They are useful diagnostically but also impair vision. Drusen have an identical composition to glomerular deposits. They are also identical to the drusen of age-related macular degeneration, and may respond to the same treatments. Individuals with a C3 glomerulopathy should be assessed ophthalmologically at diagnosis, and monitored regularly for vision-threatening complications.
Entities:
Keywords:
C3 glomerulopathy; complement alternative pathway; complement factor H; dense deposit disease; drusen; membranoproliferative glomerulonephritis type II
Authors: Ahmad M Mansour; Luiz H Lima; J Fernando Arevalo; Miguel Hage Amaro; Virginia Lozano; Alaa Bou Ghannam; Errol W Chan Journal: Am J Ophthalmol Case Rep Date: 2017-06-22
Authors: Ye Ji Ham; Eleanor Nicklason; Tony Wightman; Sarah Akom; Kieran Sandhu; Philip Harraka; Deb Colville; Andrew Catran; David Barit; David Langsford; Tim Pianta; Andrew Foote; Russell Buchanan; Heather Mack; Judy Savige Journal: Kidney Int Rep Date: 2022-02-02
Authors: Sarah de Jong; Elena B Volokhina; Anita de Breuk; Sara C Nilsson; Eiko K de Jong; Nicole C A J van der Kar; Bjorn Bakker; Carel B Hoyng; Lambert P van den Heuvel; Anna M Blom; Anneke I den Hollander Journal: Hum Mol Genet Date: 2020-08-11 Impact factor: 6.150