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Reduced secretion of fibulin 5 in age related macular degeneration and cutis laxa

Reduced secretion of fibulin 5 in age related macular degeneration and cutis laxa
Reduced secretion of fibulin 5 in age related macular degeneration and cutis laxa
Age-related macular degeneration (ARMD) is the leading cause of irreversible visual loss in the Western world, affecting approximately 25 million people worldwide. The pathogenesis is complex and missense mutations in FBLN5 have been reported in association with ARMD. We have investigated the role of fibulin 5 in ARMD by completing the first European study of the gene FBLN5 in ARMD (using 2 European cohorts of 805 ARMD patients and 279 controls) and by determining the functional effects of the missense mutations on fibulin 5 expression. We also correlated the FBLN5 genotype with the ARMD phenotype. We found two novel sequence changes in ARMD patients that were absent in controls and expressed these and the other nine reported FBLN5 mutations associated with ARMD and two associated with the autosomal recessive disease cutis laxa. Fibulin 5 secretion was significantly reduced (P<0.001) for four ARMD (p.G412E, p.G267S, p.I169 T, and p.Q124P) and two cutis laxa (p.S227P, p.C217R) mutations. These results suggest that some missense mutations associated with ARMD lead to decreased fibulin 5 secretion with a possible corresponding reduction in elastinogenesis. This study confirms the previous work identifying an association between FBLN5 mutations and ARMD and for the first time suggests a functional mechanism by which these mutations can lead to ARMD. It further demonstrates that FBLN5 mutations can be associated with different phenotypes of ARMD (not limited to the previously described cuticular drusen type). Such knowledge may ultimately lead to the development of novel therapies for this common disease.
age-related macular degeneration, ARMD, fibulin 5, FBLN5, cutis laxa, genotype-phenotype correlation, elastinogenesis
1059-7794
568-574
Lotery, Andrew J.
5ecc2d2d-d0b4-468f-ad2c-df7156f8e514
Baas, Dominique
c9978adf-bb0d-4b10-aa3a-a513a845c4cd
Ridley, Caroline
38c8db20-9723-4806-a053-87c362749363
Jones, Richard P.O.
73e69d3e-5db8-4e30-9fe5-359417fa48c0
Klaver, Caroline C.W.
bcfef58f-f6f3-4869-af44-c7ca68400797
Stone, Edwin
daa8d958-0168-4fc6-b065-1fef3451b2c6
Nakamura, Tomoyuki
e4a22036-601c-442a-a70f-4981f6cd6eda
Luff, Andrew
a1b802a4-58fb-4abc-a028-9e54aa1167a8
Griffiths, Helen
a097fdaa-d3d6-49a9-9c69-0e6e5a5d518b
Wang, Tao
dd7d278c-abe5-46f4-9fa3-39e5629d43d7
Bergen, Arthur A.B.
befeadb8-1125-483d-8c02-51c5d362bd57
Trump, Dorothy
61d1a53a-13d8-4ccc-b3a4-24dace77eccb
Lotery, Andrew J.
5ecc2d2d-d0b4-468f-ad2c-df7156f8e514
Baas, Dominique
c9978adf-bb0d-4b10-aa3a-a513a845c4cd
Ridley, Caroline
38c8db20-9723-4806-a053-87c362749363
Jones, Richard P.O.
73e69d3e-5db8-4e30-9fe5-359417fa48c0
Klaver, Caroline C.W.
bcfef58f-f6f3-4869-af44-c7ca68400797
Stone, Edwin
daa8d958-0168-4fc6-b065-1fef3451b2c6
Nakamura, Tomoyuki
e4a22036-601c-442a-a70f-4981f6cd6eda
Luff, Andrew
a1b802a4-58fb-4abc-a028-9e54aa1167a8
Griffiths, Helen
a097fdaa-d3d6-49a9-9c69-0e6e5a5d518b
Wang, Tao
dd7d278c-abe5-46f4-9fa3-39e5629d43d7
Bergen, Arthur A.B.
befeadb8-1125-483d-8c02-51c5d362bd57
Trump, Dorothy
61d1a53a-13d8-4ccc-b3a4-24dace77eccb

Lotery, Andrew J., Baas, Dominique, Ridley, Caroline, Jones, Richard P.O., Klaver, Caroline C.W., Stone, Edwin, Nakamura, Tomoyuki, Luff, Andrew, Griffiths, Helen, Wang, Tao, Bergen, Arthur A.B. and Trump, Dorothy (2006) Reduced secretion of fibulin 5 in age related macular degeneration and cutis laxa. Human Mutation, 27 (6), 568-574. (doi:10.1002/humu.20344). (PMID:16652333)

Record type: Article

Abstract

Age-related macular degeneration (ARMD) is the leading cause of irreversible visual loss in the Western world, affecting approximately 25 million people worldwide. The pathogenesis is complex and missense mutations in FBLN5 have been reported in association with ARMD. We have investigated the role of fibulin 5 in ARMD by completing the first European study of the gene FBLN5 in ARMD (using 2 European cohorts of 805 ARMD patients and 279 controls) and by determining the functional effects of the missense mutations on fibulin 5 expression. We also correlated the FBLN5 genotype with the ARMD phenotype. We found two novel sequence changes in ARMD patients that were absent in controls and expressed these and the other nine reported FBLN5 mutations associated with ARMD and two associated with the autosomal recessive disease cutis laxa. Fibulin 5 secretion was significantly reduced (P<0.001) for four ARMD (p.G412E, p.G267S, p.I169 T, and p.Q124P) and two cutis laxa (p.S227P, p.C217R) mutations. These results suggest that some missense mutations associated with ARMD lead to decreased fibulin 5 secretion with a possible corresponding reduction in elastinogenesis. This study confirms the previous work identifying an association between FBLN5 mutations and ARMD and for the first time suggests a functional mechanism by which these mutations can lead to ARMD. It further demonstrates that FBLN5 mutations can be associated with different phenotypes of ARMD (not limited to the previously described cuticular drusen type). Such knowledge may ultimately lead to the development of novel therapies for this common disease.

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More information

Published date: 2006
Keywords: age-related macular degeneration, ARMD, fibulin 5, FBLN5, cutis laxa, genotype-phenotype correlation, elastinogenesis

Identifiers

Local EPrints ID: 40645
URI: http://eprints.soton.ac.uk/id/eprint/40645
ISSN: 1059-7794
PURE UUID: 4b1b92f8-147e-41b5-9cdc-07595f9170f2
ORCID for Andrew J. Lotery: ORCID iD orcid.org/0000-0001-5541-4305

Catalogue record

Date deposited: 07 Jul 2006
Last modified: 16 Mar 2024 03:31

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Contributors

Author: Dominique Baas
Author: Caroline Ridley
Author: Richard P.O. Jones
Author: Caroline C.W. Klaver
Author: Edwin Stone
Author: Tomoyuki Nakamura
Author: Andrew Luff
Author: Helen Griffiths
Author: Tao Wang
Author: Arthur A.B. Bergen
Author: Dorothy Trump

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