Phenotypic Characterization of Complement Factor H R1210C Rare Genetic Variant in Age-Related Macular Degeneration

Ferrara, Daniela; Seddon, Johanna M.

doi:10.1001/jamaophthalmol.2015.0814

Cited by 42 publications

(54 citation statements)

References 46 publications

(58 reference statements)

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“…In addition to these variants being associated with more advanced AMD within these families, carriers also had earlier age of onset of advanced disease (mean age = 59.2) compared to individuals with advanced AMD without rare CFH variants (mean age at diagnosis in our AMD database = 69.6, n = 1,627)26. We also explored disease symmetry, and among affected individuals carrying a rare CFH variant in these families, 75% (n = 9 of 12 carriers) exhibited a symmetric fundus phenotype.…”

Section: Resultsmentioning

confidence: 86%

Mapping rare, deleterious mutations in Factor H: Association with early onset, drusen burden and lower antigenic levels in familial AMD

Wagner

Raychaudhuri

Villalonga

et al. 2016

Sci Rep

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The genetic architecture of age-related macular degeneration (AMD) involves numerous genetic variants, both common and rare, in the coding region of complement factor H (CFH). While these variants explain high disease burden in some families, they fail to explain the pathology in all. We selected families whose AMD was unexplained by known variants and performed whole exome sequencing to probe for other rare, highly penetrant variants. We identified four rare loss-of-function variants in CFH associated with AMD. Missense variant CFH 1:196646753 (C192F) segregated perfectly within a family characterized by advanced AMD and drusen temporal to the macula. Two families, each comprising a pair of affected siblings with extensive extramacular drusen, carried essential splice site variant CFH 1:196648924 (IVS6+1G>A) or missense variant rs139360826 (R175P). In a fourth family, missense variant rs121913058 (R127H) was associated with AMD. Most carriers had early onset bilateral advanced AMD and extramacular drusen. Carriers tended to have low serum Factor H levels, especially carriers of the splice variant. One missense variant (R127H) has been previously shown not to be secreted. The two other missense variants were produced recombinantly: compared to wild type, one (R175P) had no functional activity and the other (C192F) had decreased secretion.

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Section: Resultsmentioning

confidence: 86%

Mapping rare, deleterious mutations in Factor H: Association with early onset, drusen burden and lower antigenic levels in familial AMD

Wagner

Raychaudhuri

Villalonga

et al. 2016

Sci Rep

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“…R1210C is also associated with atypical hemolytic uremic syndrome (OMIM 134371). The drusen phenotype associated with the R1210C risk allele has recently been described (Ferrara and Seddon, 2015). The authors identified widespread soft drusen, both at the macular and outside the arcades, an unusual combination as such drusen are rarely observed in the peripheral retina.…”

Section: Complement and Drusenmentioning

confidence: 93%

Differentiating drusen: Drusen and drusen-like appearances associated with ageing, age-related macular degeneration, inherited eye disease and other pathological processes

Khan

Mahroo

Khan

et al. 2016

Progress in Retinal and Eye Research

170

159

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Drusen are discussed frequently in the context of their association with age-related macular degeneration (AMD). Some types may, however, be regarded as a normal consequence of ageing; others may be observed in young age groups. They also occur in a number of inherited disorders and some systemic conditions. Whilst drusen are classically located external (sclerad) to the retinal pigment epithelium, accumulations of material internal (vitread to) this layer can display a drusen-like appearance, having been variously termed pseudodrusen or subretinal drusenoid deposits. This review first briefly presents an overview of drusen biogenesis and subclinical deposit. The (frequently overlapping) subtypes of clinically detectable deposit, seen usually in the context of ageing or AMD, are then described in more detail, together with appearance on imaging modalities: these include hard and soft drusen, cuticular drusen, reticular pseudodrusen and "ghost drusen". Eye disorders other than AMD which may exhibit drusen or drusen-like features are subsequently discussed: these include monogenic conditions as well as conditions with undefined inheritance, the latter including some types of early onset drusen such as large colloid drusen. A number of systemic conditions in which drusen-like deposits may be seen are also considered. Throughout this review, high resolution images are presented for most of the conditions discussed, particularly the rarer ones, providing a useful reference library for images of the range of conditions associated with drusen-like appearances. In the final section, some common themes are highlighted, as well as a brief discussion of some future avenues for research.

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“…Carriers of rare variants appear to have differing phenotypes compared with non-carriers. A number of studies have shown rare variants to be associated with earlier onset of advanced AMD [48,58,59,62,63]. Carriers of rare CFH variants have increased drusen load, are more likely to have extramacular drusen, drusen nasal to the optic disc, and crystalline or calcified drusen [62,63,64].…”

Section: Rare Variantsmentioning

confidence: 99%

“…A number of studies have shown rare variants to be associated with earlier onset of advanced AMD [48,58,59,62,63]. Carriers of rare CFH variants have increased drusen load, are more likely to have extramacular drusen, drusen nasal to the optic disc, and crystalline or calcified drusen [62,63,64]. In addition, rare variants in CFH, CFI, C9, and C3 have been more frequently observed in patients with GA than those with nvAMD [58,63].…”

Section: Rare Variantsmentioning

confidence: 99%

Genetics and genetic testing for age-related macular degeneration

Warwick

Lotery

2017

Eye

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Considerable advances have been made in our understanding of age-related macular degeneration (AMD) genetics over the past decade. The genetic associations discovered to date are estimated to account for approximately half of AMD heritability, and functional studies of these variants have revealed new insights into disease pathogenesis, leading to the development of potential novel therapies. There is furthermore growing interest in genetic testing for predicting an individual's risk of AMD and offering personalised preventive or therapeutic treatments. We review the progress made so far in AMD genetics and discuss the possible applications for genetic testing.

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Phenotypic Characterization of Complement Factor H R1210C Rare Genetic Variant in Age-Related Macular Degeneration

Cited by 42 publications

References 46 publications

Mapping rare, deleterious mutations in Factor H: Association with early onset, drusen burden and lower antigenic levels in familial AMD

Mapping rare, deleterious mutations in Factor H: Association with early onset, drusen burden and lower antigenic levels in familial AMD

Differentiating drusen: Drusen and drusen-like appearances associated with ageing, age-related macular degeneration, inherited eye disease and other pathological processes

Genetics and genetic testing for age-related macular degeneration

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