A genome screen in multiple sclerosis reveals susceptibility loci on chromosome 6p21 and 17q22

被引：559

作者：

Sawcer, S

Jones, HB

Feakes, R

Gray, J

Smaldon, N

Chataway, J

Robertson, N

Clayton, D

Goodfellow, PN

Compston, A

机构：

[1] UNIV CAMBRIDGE, DEPT GENET, CAMBRIDGE CB2 3EH, ENGLAND

[2] INST PUBL HLTH, MRC, BIOSTAT UNIT, CAMBRIDGE CB2 2SR, ENGLAND

[3] MRC, CAMBRIDGE CTR BRAIN REPAIR, CAMBRIDGE CB2 2SR, ENGLAND

来源：

NATURE GENETICS | 1996年 / 13卷 / 04期

关键词：

D O I：

10.1038/ng0896-464

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

The population prevalence of multiple sclerosis is 0.1%; however, the risk of the disease in the siblings of affected individuals is very much higher at 3-5%. The importance of genetic factors in accounting for this increased risk is confirmed by the results of twin and adoption studies. Despite the evidence for a strong genetic effect, a weak major histocompatibility complex (MHC) association is the only consistently observed feature in the genetics of multiple sclerosis. Other candidates have been proposed, including genes encoding the immunoglobulin heavy chain, T cell receptor β chain and APOC2, but none has yet been confirmed. Evidence for linkage and association to the myelin basic protein gene has been reported in a genetically isolated Finnish population but it has not been possible to reproduce these results in other populations. We used a two- stage approach to search the human genome for the genes causing susceptibility to multiple sclerosis. Two principal regions of linkage are identified, chromosomes 17q22 and 6p21 (MHC). Our results are compatible with genetic models involving epistatic interaction between these and several additional genes.

引用

页码：464 / 468

页数：5

共 34 条

[1] SUSCEPTIBILITY FOR MULTIPLE-SCLEROSIS IS DETERMINED, IN PART, BY INHERITANCE OF A 175-KB REGION OF THE TCR V-BETA-CHAIN LOCUS AND HLA CLASS-II GENES
BEALL, SS
BIDDISON, WE
MCFARLIN, DE
MCFARLAND, HF
HOOD, LE
[J]. JOURNAL OF NEUROIMMUNOLOGY, 1993, 45 (1-2) : 53 - 60
[2] COMPSTON DAS, 1976, LANCET, V2, P1261
[3] A GENOME-WIDE SEARCH FOR HUMAN TYPE-1 DIABETES SUSCEPTIBILITY GENES
DAVIES, JL
KAWAGUCHI, Y
BENNETT, ST
COPEMAN, JB
CORDELL, HJ
PRITCHARD, LE
REED, PW
GOUGH, SCL
JENKINS, SC
PALMER, SM
BALFOUR, KM
ROWE, BR
FARRALL, M
BARNETT, AH
BAIN, SC
TODD, JA
[J]. NATURE, 1994, 371 (6493) : 130 - 136
[4] TOUCHDOWN PCR TO CIRCUMVENT SPURIOUS PRIMING DURING GENE AMPLIFICATION
DON, RH
COX, PT
WAINWRIGHT, BJ
BAKER, K
MATTICK, JS
[J]. NUCLEIC ACIDS RESEARCH, 1991, 19 (14) : 4008 - 4008
[5] EBERS GC, 1982, LANCET, V2, P88
[6] A POPULATION-BASED STUDY OF MULTIPLE-SCLEROSIS IN TWINS
EBERS, GC
BULMAN, DE
SADOVNICK, AD
PATY, DW
WARREN, S
HADER, W
MURRAY, TJ
SELAND, TP
DUQUETTE, P
GREY, T
NELSON, R
NICOLLE, M
BRUNET, D
[J]. NEW ENGLAND JOURNAL OF MEDICINE, 1986, 315 (26) : 1638 - 1642
[7] A GENETIC-BASIS FOR FAMILIAL AGGREGATION IN MULTIPLE-SCLEROSIS
EBERS, GC
SADOVNICK, AD
RISCH, NJ
BULMAN, D
RICE, GPA
HASHIMOTO, SA
PATY, D
OGER, JJF
METZ, L
BELL, R
WARREN, S
HADER, W
AUTY, T
NATH, A
GRAY, T
OCONNOR, P
NELSON, R
FREEDMAN, M
BRUNET, D
PAULSETH, R
FRANCIS, G
DUQUETTE, P
MURRAY, TJ
BAHN, V
PRYSEPHILLIPS, W
[J]. NATURE, 1995, 377 (6545) : 150 - 151
[8] THE 1993-94 GENETHON HUMAN GENETIC-LINKAGE MAP
GYAPAY, G
MORISSETTE, J
VIGNAL, A
DIB, C
FIZAMES, C
MILLASSEAU, P
MARC, S
BERNARDI, G
LATHROP, M
WEISSENBACH, J
[J]. NATURE GENETICS, 1994, 7 (02) : 246 - 339
[9] IMMUNOGLOBULIN HEAVY-CHAIN VARIABLE REGION POLYMORPHISMS AND MULTIPLE-SCLEROSIS SUSCEPTIBILITY
HASHIMOTO, LL
WALTER, MA
COX, DW
EBERS, GC
[J]. JOURNAL OF NEUROIMMUNOLOGY, 1993, 44 (01) : 77 - 84
[10] IMMUNOGLOBULIN-GAMMA CONSTANT GENE REGION POLYMORPHISMS IN MULTIPLE-SCLEROSIS
HILLERT, J
[J]. JOURNAL OF NEUROIMMUNOLOGY, 1993, 43 (1-2) : 9 - 14

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