Genetics and genetic testing for age-related macular degeneration

Warwick, Alasdair; Lotery, Andrew

doi:10.1038/eye.2017.245

Cited by 54 publications

(47 citation statements)

References 102 publications

(120 reference statements)

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“…C3 has been shown to result in reduced binding to CFH and reduced complement regulation leading to increased membrane attack complex (MAC) deposition at the choriocapillaris [37,38]. The association of AMD pathogenesis with chromosome 10q26, which surrounds ARMS2 and HTRA1, has also been demonstrated in many studies although the debate is ongoing as to the causal allele and underlying pathogenic mechanism [39].…”

Section: Amd Pathogenic Mechanisms and Interaction Of Genetic/environmentioning

confidence: 99%

Epigenetics in age-related macular degeneration: new discoveries and future perspectives

Gemenetzi

Lotery

2020

Cell. Mol. Life Sci.

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Section: Amd Pathogenic Mechanisms and Interaction Of Genetic/environmentioning

confidence: 99%

Epigenetics in age-related macular degeneration: new discoveries and future perspectives

Gemenetzi

Lotery

2020

Cell. Mol. Life Sci.

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“…In einer kürzlich durch-geführten, genomweiten Assoziationsstudie (GWAS) wurden 52 häufige und seltene Genvarianten identifiziert, die unabhängig voneinander mit AMD assoziiert sind [108]. Unter ihnen befindet sich mehr als ein Drittel (19/52) in oder in der Nähe eines Komplementgens [103,105,108,109]. Insbesondere Varianten der Komplementgene CFH, CFI, C2/CFB, C3, C9, CD55 und Vitronectin (VTN) wurden mit einem erhöhten Risiko für die Entwicklung von AMD in Verbindung gebracht [108, 110 -112].…”

Section: Komplement-und Altersbedingte Makuladegeneration (Amd)unclassified

Das Komplementsystem: von den Grundlagen zur klinischen Bedeutung

Schröder‐Braunstein

Kirschfink

2020

Transfusionsmedizin - Immunhämatologie, Hämotherapie, Immungene

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ZusammenfassungAls Teil der unspezifischen Abwehr ist das Komplementsystem jederzeit verfügbar und somit bereits in der Frühphase von Infektionen von unschätzbarem Wert, bevor nach Bereitstellung spezifischer Antikörper und T-Zellen das adaptive Immunsystem zielgerichtet seine volle Wirkung entfaltet. Aufgrund seiner Rolle in der Pathophysiologie verschiedener Krankheitsbilder besitzt das Komplement eine besondere Bedeutung für die Klinik. Sowohl für die Aufklärung von Komplementdefekten und -fehlregulationen als auch zur Früherkennung lebensbedrohlicher Prozesse, wie z. B. der Entwicklung eines Multiorganversagens nach schwerem Trauma, Verbrennungen oder Sepsis sowie zur Einschätzung der Wirksamkeit neuer Therapieansätze, ist eine moderne Komplementdiagnostik heutzutage unabdingbar. Mit diesem Übersichtsartikel wollen wir einen Bogen spannen von den Grundlagen des Komplementsystems über dessen klinische Relevanz und diagnostische Maßnahmen bis hin zu aktuellen Möglichkeiten einer zielgerichteten Therapie.

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“…This observation has led to the hypothesis that rare TIMP3 protein-altering variants together with alleles at other AMD risk loci contribute to AMD development (Fritsche et al, 2016). A retrospective, observational case series has recently shown that patients initially diagnosed with neovascular AMD carry the SFD-associated p.(Ser38Cys)-TIMP3 mutation (Warwick & Lotery, 2017). SFD phenotypic expressivity varies considerably including large intra-and interfamilial variability in the age of onset of visual symptoms (Gliem, Muller, Mangold, Holz, et al, 2015).…”

Section: Mutati On S In Timp3mentioning

confidence: 99%

Sorsby fundus dystrophy: Insights from the past and looking to the future

Anand‐Apte

Chao

Singh

et al. 2018

J of Neuroscience Research

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Sorsby fundus dystrophy (SFD), an autosomal dominant, fully penetrant, degenerative disease of the macula, is manifested by symptoms of night blindness or sudden loss of visual acuity, usually in the third to fourth decades of life due to choroidal neovascularization (CNV). SFD is caused by specific mutations in the Tissue Inhibitor of Metalloproteinase-3, (TIMP3) gene. The predominant histo-pathological feature in the eyes of patients with SFD are confluent 20-30 m thick, amorphous deposits found between the basement membrane of the retinal pigment epithelium (RPE) and the inner collagenous layer of Bruch's membrane. SFD is a rare disease but it has generated significant interest because it closely resembles the exudative or "wet" form of the more common age-related macular degeneration (AMD). In addition, in both SFD and AMD donor eyes, sub-retinal deposits have been shown to accumulate TIMP3 protein. Understanding the molecular functions of wild-type and mutant TIMP3 will provide significant insights into the patho-physiology of SFD and perhaps AMD. This review summarizes the current knowledge on TIMP3 and how mutations in TIMP3 cause SFD to provide insights into how we can study this disease going forward. Findings from these studies could have potential therapeutic implications for both SFD and AMD.

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Genetics and genetic testing for age-related macular degeneration

Cited by 54 publications

References 102 publications

Epigenetics in age-related macular degeneration: new discoveries and future perspectives

Epigenetics in age-related macular degeneration: new discoveries and future perspectives

Das Komplementsystem: von den Grundlagen zur klinischen Bedeutung

Sorsby fundus dystrophy: Insights from the past and looking to the future

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