Complement factor H deficiency results in decreased neuroretinal expression of Cd59a in aged mice

Carsten Faber; Jennifer Williams; Helene Bæk Juel; John Greenwood; Mogens Holst Nissen; Stephen E. Moss

doi:10.1167/iovs.12-10385

Complement factor H deficiency results in decreased neuroretinal expression of Cd59a in aged mice

Carsten Faber, Jennifer Williams, Helene Bæk Juel, John Greenwood, Mogens Holst Nissen, Stephen E. Moss

Department of Immunology and Microbiology

14 Citations (Scopus)

Abstract

Purpose. The complement system is closely linked to the pathogenesis of AMD. Several complement genes are expressed in RPE, and complement proteins accumulate in drusen. Further, a common variant of complement factor H (CFH) confers increased risk of developing AMD. Because the mechanisms by which changes in the function of CFH influence development of AMD are unclear, we examined ocular complement expression as a consequence of age in control and CFH null mutant mice.

Methods. Gene expression in neuroretinas and RPE/choroid from young and aged WT and Cfh−/− C57BL/6J mice was analyzed by microarrays. Expression of a wide range of complement genes was compared with expression in liver.

Results. An age-associated increased expression of complement, particularly C1q, C3, and factor B, in the RPE/choroid coincided with increased expression of the negative regulators Cfh and Cd59a in the neuroretina. Young mice deficient in CFH expressed Cd59a similar to WT, but failed to upregulate Cd59a expression with age. Hepatic expression of Cd59a increased with age regardless of Cfh genotype.

Conclusions. While the connection between CFH deficiency and failure to upregulate CD59a remains unknown, these results suggest that expression of CD59 is tissue-specific and that neuroretinal regulation depends on CFH. This could contribute to the visual functional deficits and morphological changes in the Cfh−/− mouse retina that occur with age.

Original language	English
Journal	Investigative Ophthalmology & Visual Science
Volume	53
Issue number	10
Pages (from-to)	6324-6330
Number of pages	7
ISSN	0146-0404
DOIs	https://doi.org/10.1167/iovs.12-10385
Publication status	Published - 19 Sept 2012

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@article{c3b9edee867b491a9f6379dcd122e9b1,

title = "Complement factor H deficiency results in decreased neuroretinal expression of Cd59a in aged mice",

abstract = "Purpose. The complement system is closely linked to the pathogenesis of AMD. Several complement genes are expressed in RPE, and complement proteins accumulate in drusen. Further, a common variant of complement factor H (CFH) confers increased risk of developing AMD. Because the mechanisms by which changes in the function of CFH influence development of AMD are unclear, we examined ocular complement expression as a consequence of age in control and CFH null mutant mice. Methods. Gene expression in neuroretinas and RPE/choroid from young and aged WT and Cfh−/− C57BL/6J mice was analyzed by microarrays. Expression of a wide range of complement genes was compared with expression in liver. Results. An age-associated increased expression of complement, particularly C1q, C3, and factor B, in the RPE/choroid coincided with increased expression of the negative regulators Cfh and Cd59a in the neuroretina. Young mice deficient in CFH expressed Cd59a similar to WT, but failed to upregulate Cd59a expression with age. Hepatic expression of Cd59a increased with age regardless of Cfh genotype. Conclusions. While the connection between CFH deficiency and failure to upregulate CD59a remains unknown, these results suggest that expression of CD59 is tissue-specific and that neuroretinal regulation depends on CFH. This could contribute to the visual functional deficits and morphological changes in the Cfh−/− mouse retina that occur with age. ",

author = "Carsten Faber and Jennifer Williams and Juel, {Helene B{\ae}k} and John Greenwood and Nissen, {Mogens Holst} and Moss, {Stephen E.}",

year = "2012",

month = sep,

day = "19",

doi = "10.1167/iovs.12-10385",

language = "English",

volume = "53",

pages = "6324--6330",

journal = "Investigative Ophthalmology & Visual Science",

issn = "0146-0404",

publisher = "Association for Research in Vision and Ophthalmology",

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T1 - Complement factor H deficiency results in decreased neuroretinal expression of Cd59a in aged mice

AU - Faber, Carsten

AU - Williams, Jennifer

AU - Juel, Helene Bæk

AU - Greenwood, John

AU - Nissen, Mogens Holst

AU - Moss, Stephen E.

PY - 2012/9/19

Y1 - 2012/9/19

N2 - Purpose. The complement system is closely linked to the pathogenesis of AMD. Several complement genes are expressed in RPE, and complement proteins accumulate in drusen. Further, a common variant of complement factor H (CFH) confers increased risk of developing AMD. Because the mechanisms by which changes in the function of CFH influence development of AMD are unclear, we examined ocular complement expression as a consequence of age in control and CFH null mutant mice. Methods. Gene expression in neuroretinas and RPE/choroid from young and aged WT and Cfh−/− C57BL/6J mice was analyzed by microarrays. Expression of a wide range of complement genes was compared with expression in liver. Results. An age-associated increased expression of complement, particularly C1q, C3, and factor B, in the RPE/choroid coincided with increased expression of the negative regulators Cfh and Cd59a in the neuroretina. Young mice deficient in CFH expressed Cd59a similar to WT, but failed to upregulate Cd59a expression with age. Hepatic expression of Cd59a increased with age regardless of Cfh genotype. Conclusions. While the connection between CFH deficiency and failure to upregulate CD59a remains unknown, these results suggest that expression of CD59 is tissue-specific and that neuroretinal regulation depends on CFH. This could contribute to the visual functional deficits and morphological changes in the Cfh−/− mouse retina that occur with age.

AB - Purpose. The complement system is closely linked to the pathogenesis of AMD. Several complement genes are expressed in RPE, and complement proteins accumulate in drusen. Further, a common variant of complement factor H (CFH) confers increased risk of developing AMD. Because the mechanisms by which changes in the function of CFH influence development of AMD are unclear, we examined ocular complement expression as a consequence of age in control and CFH null mutant mice. Methods. Gene expression in neuroretinas and RPE/choroid from young and aged WT and Cfh−/− C57BL/6J mice was analyzed by microarrays. Expression of a wide range of complement genes was compared with expression in liver. Results. An age-associated increased expression of complement, particularly C1q, C3, and factor B, in the RPE/choroid coincided with increased expression of the negative regulators Cfh and Cd59a in the neuroretina. Young mice deficient in CFH expressed Cd59a similar to WT, but failed to upregulate Cd59a expression with age. Hepatic expression of Cd59a increased with age regardless of Cfh genotype. Conclusions. While the connection between CFH deficiency and failure to upregulate CD59a remains unknown, these results suggest that expression of CD59 is tissue-specific and that neuroretinal regulation depends on CFH. This could contribute to the visual functional deficits and morphological changes in the Cfh−/− mouse retina that occur with age.

U2 - 10.1167/iovs.12-10385

DO - 10.1167/iovs.12-10385

M3 - Journal article

SN - 0146-0404

VL - 53

SP - 6324

EP - 6330

JO - Investigative Ophthalmology & Visual Science

JF - Investigative Ophthalmology & Visual Science

IS - 10

ER -

Complement factor H deficiency results in decreased neuroretinal expression of Cd59a in aged mice

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