Association of low-density lipoprotein receptor polymorphisms and outcome of hepatitis C infection
Association of low-density lipoprotein receptor polymorphisms and outcome of hepatitis C infection
The low-density lipoprotein receptor (LDLR) has been proposed to promote hepatitis C virus endocytosis and the cell membrane protein CD81 may also promote HCV host cell entry. The CD81 gene was sequenced to screen for novel polymorphisms, but no SNPs were identified. Polymorphisms within the LDLR gene are associated with the pathogenesis of familial hypercholesterolemia, atherosclerosis and obesity. We therefore studied genetic variation within the LDLR gene and clinical features of hepatitis C infection. An amino acid change in exon 8 was associated with severity of fibrosis; a SNP in exon 10 correlated with viral clearance and overall inflammation, and a SNP in the 3'UTR appeared to influence treatment response. There were no other significant associations between any of the SNPs studied and the clinical measures of hepatitis C infection. We furthermore report on linkage disequilibrium within the gene and haplotype frequencies in our population. Our findings support a possible role for the LDLR in the modulation of disease progression by affecting immune responses, rather than functioning as receptor for HCV.
adolescent, adult, aged, aged, 80 and over, antigens, CD/genetics, Female director critical mass, haplotypes, hepacivirus/metabolism, hepatitis C/genetics, humans, linkage disequilibrium, male body, membrane proteins/genetics, middle aged, polymorphism, genetic, receptors, LDL/genetics, tetraspanin 28
359-67
Hennig, B.J.W.
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Hellier, S.
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Frodsham, A J
fbc97752-a212-4bfd-a9a1-a7ca3f827769
Zhang, L.
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Klenerman, P.
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Knapp, S.
b7e3f8e9-0b4b-4433-8077-d6e3fbf4ccee
Wright, M
56ad372b-2007-40ff-bdfe-91bc01a6e95f
Thomas, H.C.
6da4bb85-eade-4290-9d3a-c0e63ac8ef1d
Thursz, M.
2c345793-0ae5-4a81-b663-6c47236e2a73
Hill, A.V.S.
55020310-08eb-4a32-97fb-94c7bed2ec38
Hennig, B.J.W.
06b115a9-52c0-4f95-9b5d-8c87cc326fb2
Hellier, S.
7698887c-29e4-4afc-9b97-1b5c067c4c04
Frodsham, A J
fbc97752-a212-4bfd-a9a1-a7ca3f827769
Zhang, L.
1f3632f4-d2c8-46db-9d37-df521550f325
Klenerman, P.
aa4c00a6-1a4d-4a4f-ac21-2131996344a7
Knapp, S.
b7e3f8e9-0b4b-4433-8077-d6e3fbf4ccee
Wright, M
56ad372b-2007-40ff-bdfe-91bc01a6e95f
Thomas, H.C.
6da4bb85-eade-4290-9d3a-c0e63ac8ef1d
Thursz, M.
2c345793-0ae5-4a81-b663-6c47236e2a73
Hill, A.V.S.
55020310-08eb-4a32-97fb-94c7bed2ec38
Hennig, B.J.W., Hellier, S., Frodsham, A J, Zhang, L., Klenerman, P., Knapp, S., Wright, M, Thomas, H.C., Thursz, M. and Hill, A.V.S.
(2002)
Association of low-density lipoprotein receptor polymorphisms and outcome of hepatitis C infection.
Genes and Immunity, 3 (6), .
(doi:10.1038/sj.gene.6363883).
Abstract
The low-density lipoprotein receptor (LDLR) has been proposed to promote hepatitis C virus endocytosis and the cell membrane protein CD81 may also promote HCV host cell entry. The CD81 gene was sequenced to screen for novel polymorphisms, but no SNPs were identified. Polymorphisms within the LDLR gene are associated with the pathogenesis of familial hypercholesterolemia, atherosclerosis and obesity. We therefore studied genetic variation within the LDLR gene and clinical features of hepatitis C infection. An amino acid change in exon 8 was associated with severity of fibrosis; a SNP in exon 10 correlated with viral clearance and overall inflammation, and a SNP in the 3'UTR appeared to influence treatment response. There were no other significant associations between any of the SNPs studied and the clinical measures of hepatitis C infection. We furthermore report on linkage disequilibrium within the gene and haplotype frequencies in our population. Our findings support a possible role for the LDLR in the modulation of disease progression by affecting immune responses, rather than functioning as receptor for HCV.
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e-pub ahead of print date: 5 September 2002
Keywords:
adolescent, adult, aged, aged, 80 and over, antigens, CD/genetics, Female director critical mass, haplotypes, hepacivirus/metabolism, hepatitis C/genetics, humans, linkage disequilibrium, male body, membrane proteins/genetics, middle aged, polymorphism, genetic, receptors, LDL/genetics, tetraspanin 28
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Local EPrints ID: 478152
URI: http://eprints.soton.ac.uk/id/eprint/478152
ISSN: 1466-4879
PURE UUID: 41de9501-3232-4a6c-b904-1aa9248d35a3
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Date deposited: 22 Jun 2023 16:49
Last modified: 17 Mar 2024 02:03
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Contributors
Author:
B.J.W. Hennig
Author:
S. Hellier
Author:
A J Frodsham
Author:
L. Zhang
Author:
P. Klenerman
Author:
S. Knapp
Author:
M Wright
Author:
H.C. Thomas
Author:
M. Thursz
Author:
A.V.S. Hill
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