schliessen

Filtern

 

Bibliotheken

Cover Image

MICA, a gene contributing strong susceptibility to ankylosing spondylitis

Objective The human major histocompatibility complex class I chain-related gene A (MICA) controls the immune process by balancing activities of  natural killer cells, γδ T cells and αβ CD8 T cells, and immunosuppressive CD4 T cells. MICA is located near HLA-B on chromosome 6. Recent genomewide assoc... Full description

Journal Title: Annals of the Rheumatic Diseases 2014, Vol.73 (8), p.1552-1557
Main Author: Zhou, Xiaodong
Other Authors: Wang, Jiucun , Zou, Hejian , Ward, Michael M , Weisman, Michael H , Espitia, Maribel G , Xiao, Xiangjun , Petersdorf, Effie , Mignot, Emmanuel , Martin, Javier , Gensler, Lianne S , Scheet, Paul , Reveille, John D
Format: Electronic Article Electronic Article
Language: English
Subjects:
Adult
Analysis
Ankylosing spondylitis
Article
Asian Americans - genetics
Asian Americans - statistics & numerical data
Care and treatment
Chronic illnesses
Cohort Studies
Deoxyribonucleic acid
Disease
DNA
European Continental Ancestry Group - genetics
European Continental Ancestry Group - statistics & numerical data
Female
Genealogy
Genes
Genetic Markers
Genetic Predisposition to Disease - ethnology
Genetic Predisposition to Disease - genetics
Genomes
Histocompatibility Antigens Class I - genetics
HLA-B Antigens - genetics
Humans
Immune response
Inflammation
Linkage Disequilibrium
Male
Middle Aged
Pathogenesis
Risk Factors
Spondylitis, Ankylosing - ethnology
Spondylitis, Ankylosing - genetics
Studies
United States - epidemiology
White people
Womens health
Publisher: England: BMJ Publishing Group Ltd
ID: ISSN: 0003-4967
Link: https://www.ncbi.nlm.nih.gov/pubmed/23727634
Zum Text:
SendSend as email Add to Book BagAdd to Book Bag
Staff View
recordid: cdi_proquest_journals_1777903299
title: MICA, a gene contributing strong susceptibility to ankylosing spondylitis
format: Article
creator:
  • Zhou, Xiaodong
  • Wang, Jiucun
  • Zou, Hejian
  • Ward, Michael M
  • Weisman, Michael H
  • Espitia, Maribel G
  • Xiao, Xiangjun
  • Petersdorf, Effie
  • Mignot, Emmanuel
  • Martin, Javier
  • Gensler, Lianne S
  • Scheet, Paul
  • Reveille, John D
subjects:
  • Adult
  • Analysis
  • Ankylosing spondylitis
  • Article
  • Asian Americans - genetics
  • Asian Americans - statistics & numerical data
  • Care and treatment
  • Chronic illnesses
  • Cohort Studies
  • Deoxyribonucleic acid
  • Disease
  • DNA
  • European Continental Ancestry Group - genetics
  • European Continental Ancestry Group - statistics & numerical data
  • Female
  • Genealogy
  • Genes
  • Genetic Markers
  • Genetic Predisposition to Disease - ethnology
  • Genetic Predisposition to Disease - genetics
  • Genomes
  • Histocompatibility Antigens Class I - genetics
  • HLA-B Antigens - genetics
  • Humans
  • Immune response
  • Inflammation
  • Linkage Disequilibrium
  • Male
  • Middle Aged
  • Pathogenesis
  • Risk Factors
  • Spondylitis, Ankylosing - ethnology
  • Spondylitis, Ankylosing - genetics
  • Studies
  • United States - epidemiology
  • White people
  • Womens health
ispartof: Annals of the Rheumatic Diseases, 2014, Vol.73 (8), p.1552-1557
description: Objective The human major histocompatibility complex class I chain-related gene A (MICA) controls the immune process by balancing activities of  natural killer cells, γδ T cells and αβ CD8 T cells, and immunosuppressive CD4 T cells. MICA is located near HLA-B on chromosome 6. Recent genomewide association studies indicate that genes most strongly linked to ankylosing spondylitis (AS) susceptibility come from the region containing HLA-B and MICA. While HLA-B27 is a well-known risk genetic marker for AS, the potential effect of linkage disequilibrium (LD) shields any associations of genes around HLA-B with AS. The aim of this study was to investigate a novel independent genetic association of MICA to AS. Methods We examined 1543 AS patients and 1539 controls from two ethnic populations by sequencing MICA and genotyping HLA-B alleles. Initially, 1070 AS patients and 1003 controls of European ancestry were used as a discovery cohort, followed by a confirmation cohort of 473 Han Chinese AS patients and 536 controls. We performed a stratified analysis based on HLA-B27 carrier status. We also conducted logistic regression with a formal interaction term. Results Sequencing of MICA identified that MICA*007:01 is a significant risk allele for AS in both Caucasian and Han Chinese populations, and that MICA*019 is a major risk allele in Chinese AS patients. Conditional analysis of MICA alleles on HLA-B27 that unshielded LD effect confirmed associations of the MICA alleles with AS. Conclusions Parallel with HLA-B27, MICA confers strong susceptibility to AS in US white and Han Chinese populations.
language: eng
source:
identifier: ISSN: 0003-4967
fulltext: no_fulltext
issn:
  • 0003-4967
  • 1468-2060
url: Link


@attributes
NO1
SEARCH_ENGINEprimo_central_multiple_fe
SEARCH_ENGINE_TYPEPrimo Central Search Engine
RANK2.5358257
LOCALfalse
PrimoNMBib
record
control
sourceidgale_proqu
recordidTN_cdi_proquest_journals_1777903299
sourceformatXML
sourcesystemPC
galeidA383136881
sourcerecordidA383136881
originalsourceidFETCH-LOGICAL-1651t-96ba68acc8eca841c836be381461de167b737cc1be0ab5ecc43e976b18b1e7b70
addsrcrecordideNqNUk1v1DAQjRCILoW_AJG4cGCLHccfOVCpqoBWKuICZ8t2JlsviR1iB2n_PRO2lG6FRGXJI3veex7PvKJ4RckJpUy8MyFM1zAPrU_rilCGG2O8elSsaC0UngR5XKwIIWxdN0IeFc9S2uKRKKqeFkcVk5UUrF4Vl58vz8_elqbcQIDSxZAnb-fsw6ZMeYpLmJODMXvre593ZY6lCd93fUy_MWMM7Q4TPj0vnnSmT_DiJh4X3z5--Hp-sb768gnfuFpTwWleN8IaoYxzCpxRNXWKCQtMYd20BSqklUw6Ry0QYzk4VzNopLBUWQqYJMfF6V53nO0ArQMs2fR6nPxgpp2OxuvDTPDXehN_aqZkTaRAgYu9QBwhGD_BAbcNkHVsdSWktspKwZlyEhpKpQHOBXeM8oq3HbYPpd7c1DLFHzOkrAeP3ep7EyDOSVNFlBC8lvL_UF6zSlWyWaCv70G3cZ4CNlVTKWVDWNU0f1Eb04P2oYv4W7eI6jOmGLpEKYqok3-gcLUweBw3dB7vDwhyT3BTTGmC7rY7lOjFe_qO9_TiPb33HjJf3h3MLe-P2RDw_p6089lkv5jO-P4BD1R7vh22D67qF5gj-4I
sourcetypeOpen Access Repository
isCDItrue
recordtypearticle
pqid1777903299
display
typearticle
titleMICA, a gene contributing strong susceptibility to ankylosing spondylitis
creatorZhou, Xiaodong ; Wang, Jiucun ; Zou, Hejian ; Ward, Michael M ; Weisman, Michael H ; Espitia, Maribel G ; Xiao, Xiangjun ; Petersdorf, Effie ; Mignot, Emmanuel ; Martin, Javier ; Gensler, Lianne S ; Scheet, Paul ; Reveille, John D
creatorcontribZhou, Xiaodong ; Wang, Jiucun ; Zou, Hejian ; Ward, Michael M ; Weisman, Michael H ; Espitia, Maribel G ; Xiao, Xiangjun ; Petersdorf, Effie ; Mignot, Emmanuel ; Martin, Javier ; Gensler, Lianne S ; Scheet, Paul ; Reveille, John D
descriptionObjective The human major histocompatibility complex class I chain-related gene A (MICA) controls the immune process by balancing activities of  natural killer cells, γδ T cells and αβ CD8 T cells, and immunosuppressive CD4 T cells. MICA is located near HLA-B on chromosome 6. Recent genomewide association studies indicate that genes most strongly linked to ankylosing spondylitis (AS) susceptibility come from the region containing HLA-B and MICA. While HLA-B27 is a well-known risk genetic marker for AS, the potential effect of linkage disequilibrium (LD) shields any associations of genes around HLA-B with AS. The aim of this study was to investigate a novel independent genetic association of MICA to AS. Methods We examined 1543 AS patients and 1539 controls from two ethnic populations by sequencing MICA and genotyping HLA-B alleles. Initially, 1070 AS patients and 1003 controls of European ancestry were used as a discovery cohort, followed by a confirmation cohort of 473 Han Chinese AS patients and 536 controls. We performed a stratified analysis based on HLA-B27 carrier status. We also conducted logistic regression with a formal interaction term. Results Sequencing of MICA identified that MICA*007:01 is a significant risk allele for AS in both Caucasian and Han Chinese populations, and that MICA*019 is a major risk allele in Chinese AS patients. Conditional analysis of MICA alleles on HLA-B27 that unshielded LD effect confirmed associations of the MICA alleles with AS. Conclusions Parallel with HLA-B27, MICA confers strong susceptibility to AS in US white and Han Chinese populations.
identifier
0ISSN: 0003-4967
1EISSN: 1468-2060
2DOI: 10.1136/annrheumdis-2013-203352
3PMID: 23727634
4CODEN: ARDIAO
languageeng
publisherEngland: BMJ Publishing Group Ltd
subjectAdult ; Analysis ; Ankylosing spondylitis ; Article ; Asian Americans - genetics ; Asian Americans - statistics & numerical data ; Care and treatment ; Chronic illnesses ; Cohort Studies ; Deoxyribonucleic acid ; Disease ; DNA ; European Continental Ancestry Group - genetics ; European Continental Ancestry Group - statistics & numerical data ; Female ; Genealogy ; Genes ; Genetic Markers ; Genetic Predisposition to Disease - ethnology ; Genetic Predisposition to Disease - genetics ; Genomes ; Histocompatibility Antigens Class I - genetics ; HLA-B Antigens - genetics ; Humans ; Immune response ; Inflammation ; Linkage Disequilibrium ; Male ; Middle Aged ; Pathogenesis ; Risk Factors ; Spondylitis, Ankylosing - ethnology ; Spondylitis, Ankylosing - genetics ; Studies ; United States - epidemiology ; White people ; Womens health
ispartofAnnals of the Rheumatic Diseases, 2014, Vol.73 (8), p.1552-1557
rights
0Published by the BMJ Publishing Group Limited. For permission to use (where not already granted under a licence) please go to http://group.bmj.com/group/rights-licensing/permissions
1Published by the BMJ Publishing Group Limited. For permission to use (where not already granted under a licence) please go to http://group.bmj.com/group/rights-licensing/permissions.
2Copyright: 2014 Published by the BMJ Publishing Group Limited. For permission to use (where not already granted under a licence) please go to http://group.bmj.com/group/rights-licensing/permissions
lds50peer_reviewed
oafree_for_read
citedbyFETCH-LOGICAL-1651t-96ba68acc8eca841c836be381461de167b737cc1be0ab5ecc43e976b18b1e7b70
citesFETCH-LOGICAL-1651t-96ba68acc8eca841c836be381461de167b737cc1be0ab5ecc43e976b18b1e7b70
links
openurl$$Topenurl_article
thumbnail$$Usyndetics_thumb_exl
backlink$$Uhttps://www.ncbi.nlm.nih.gov/pubmed/23727634$$D View this record in MEDLINE/PubMed
search
creatorcontrib
0Zhou, Xiaodong
1Wang, Jiucun
2Zou, Hejian
3Ward, Michael M
4Weisman, Michael H
5Espitia, Maribel G
6Xiao, Xiangjun
7Petersdorf, Effie
8Mignot, Emmanuel
9Martin, Javier
10Gensler, Lianne S
11Scheet, Paul
12Reveille, John D
title
0MICA, a gene contributing strong susceptibility to ankylosing spondylitis
1Annals of the Rheumatic Diseases
addtitleAnn Rheum Dis
descriptionObjective The human major histocompatibility complex class I chain-related gene A (MICA) controls the immune process by balancing activities of  natural killer cells, γδ T cells and αβ CD8 T cells, and immunosuppressive CD4 T cells. MICA is located near HLA-B on chromosome 6. Recent genomewide association studies indicate that genes most strongly linked to ankylosing spondylitis (AS) susceptibility come from the region containing HLA-B and MICA. While HLA-B27 is a well-known risk genetic marker for AS, the potential effect of linkage disequilibrium (LD) shields any associations of genes around HLA-B with AS. The aim of this study was to investigate a novel independent genetic association of MICA to AS. Methods We examined 1543 AS patients and 1539 controls from two ethnic populations by sequencing MICA and genotyping HLA-B alleles. Initially, 1070 AS patients and 1003 controls of European ancestry were used as a discovery cohort, followed by a confirmation cohort of 473 Han Chinese AS patients and 536 controls. We performed a stratified analysis based on HLA-B27 carrier status. We also conducted logistic regression with a formal interaction term. Results Sequencing of MICA identified that MICA*007:01 is a significant risk allele for AS in both Caucasian and Han Chinese populations, and that MICA*019 is a major risk allele in Chinese AS patients. Conditional analysis of MICA alleles on HLA-B27 that unshielded LD effect confirmed associations of the MICA alleles with AS. Conclusions Parallel with HLA-B27, MICA confers strong susceptibility to AS in US white and Han Chinese populations.
subject
0Adult
1Analysis
2Ankylosing spondylitis
3Article
4Asian Americans - genetics
5Asian Americans - statistics & numerical data
6Care and treatment
7Chronic illnesses
8Cohort Studies
9Deoxyribonucleic acid
10Disease
11DNA
12European Continental Ancestry Group - genetics
13European Continental Ancestry Group - statistics & numerical data
14Female
15Genealogy
16Genes
17Genetic Markers
18Genetic Predisposition to Disease - ethnology
19Genetic Predisposition to Disease - genetics
20Genomes
21Histocompatibility Antigens Class I - genetics
22HLA-B Antigens - genetics
23Humans
24Immune response
25Inflammation
26Linkage Disequilibrium
27Male
28Middle Aged
29Pathogenesis
30Risk Factors
31Spondylitis, Ankylosing - ethnology
32Spondylitis, Ankylosing - genetics
33Studies
34United States - epidemiology
35White people
36Womens health
issn
00003-4967
11468-2060
fulltextfalse
rsrctypearticle
creationdate2014
recordtypearticle
recordideNqNUk1v1DAQjRCILoW_AJG4cGCLHccfOVCpqoBWKuICZ8t2JlsviR1iB2n_PRO2lG6FRGXJI3veex7PvKJ4RckJpUy8MyFM1zAPrU_rilCGG2O8elSsaC0UngR5XKwIIWxdN0IeFc9S2uKRKKqeFkcVk5UUrF4Vl58vz8_elqbcQIDSxZAnb-fsw6ZMeYpLmJODMXvre593ZY6lCd93fUy_MWMM7Q4TPj0vnnSmT_DiJh4X3z5--Hp-sb768gnfuFpTwWleN8IaoYxzCpxRNXWKCQtMYd20BSqklUw6Ry0QYzk4VzNopLBUWQqYJMfF6V53nO0ArQMs2fR6nPxgpp2OxuvDTPDXehN_aqZkTaRAgYu9QBwhGD_BAbcNkHVsdSWktspKwZlyEhpKpQHOBXeM8oq3HbYPpd7c1DLFHzOkrAeP3ep7EyDOSVNFlBC8lvL_UF6zSlWyWaCv70G3cZ4CNlVTKWVDWNU0f1Eb04P2oYv4W7eI6jOmGLpEKYqok3-gcLUweBw3dB7vDwhyT3BTTGmC7rY7lOjFe_qO9_TiPb33HjJf3h3MLe-P2RDw_p6089lkv5jO-P4BD1R7vh22D67qF5gj-4I
startdate201408
enddate201408
creator
0Zhou, Xiaodong
1Wang, Jiucun
2Zou, Hejian
3Ward, Michael M
4Weisman, Michael H
5Espitia, Maribel G
6Xiao, Xiangjun
7Petersdorf, Effie
8Mignot, Emmanuel
9Martin, Javier
10Gensler, Lianne S
11Scheet, Paul
12Reveille, John D
general
0BMJ Publishing Group Ltd
1BMJ Publishing Group LTD
scope
0CGR
1CUY
2CVF
3ECM
4EIF
5NPM
6AAYXX
7CITATION
8BSHEE
93V.
107X7
117XB
1288E
1388I
148AF
158FE
168FH
178FI
188FJ
198FK
20ABUWG
21AZQEC
22BBNVY
23BENPR
24BHPHI
25BTHHO
26DWQXO
27FYUFA
28GHDGH
29GNUQQ
30HCIFZ
31K9-
32K9.
33LK8
34M0R
35M0S
36M1P
37M2P
38M7P
39PQEST
40PQQKQ
41PQUKI
42PRINS
43Q9U
447X8
457T5
46H94
47BOBZL
48CLFQK
495PM
sort
creationdate201408
titleMICA, a gene contributing strong susceptibility to ankylosing spondylitis
authorZhou, Xiaodong ; Wang, Jiucun ; Zou, Hejian ; Ward, Michael M ; Weisman, Michael H ; Espitia, Maribel G ; Xiao, Xiangjun ; Petersdorf, Effie ; Mignot, Emmanuel ; Martin, Javier ; Gensler, Lianne S ; Scheet, Paul ; Reveille, John D
facets
frbrtype5
frbrgroupidcdi_FETCH-LOGICAL-1651t-96ba68acc8eca841c836be381461de167b737cc1be0ab5ecc43e976b18b1e7b70
rsrctypearticles
prefilterarticles
languageeng
creationdate2014
topic
0Adult
1Analysis
2Ankylosing spondylitis
3Article
4Asian Americans - genetics
5Asian Americans - statistics & numerical data
6Care and treatment
7Chronic illnesses
8Cohort Studies
9Deoxyribonucleic acid
10Disease
11DNA
12European Continental Ancestry Group - genetics
13European Continental Ancestry Group - statistics & numerical data
14Female
15Genealogy
16Genes
17Genetic Markers
18Genetic Predisposition to Disease - ethnology
19Genetic Predisposition to Disease - genetics
20Genomes
21Histocompatibility Antigens Class I - genetics
22HLA-B Antigens - genetics
23Humans
24Immune response
25Inflammation
26Linkage Disequilibrium
27Male
28Middle Aged
29Pathogenesis
30Risk Factors
31Spondylitis, Ankylosing - ethnology
32Spondylitis, Ankylosing - genetics
33Studies
34United States - epidemiology
35White people
36Womens health
toplevelpeer_reviewed
creatorcontrib
0Zhou, Xiaodong
1Wang, Jiucun
2Zou, Hejian
3Ward, Michael M
4Weisman, Michael H
5Espitia, Maribel G
6Xiao, Xiangjun
7Petersdorf, Effie
8Mignot, Emmanuel
9Martin, Javier
10Gensler, Lianne S
11Scheet, Paul
12Reveille, John D
collection
0Medline
1MEDLINE
2MEDLINE (Ovid)
3MEDLINE
4MEDLINE
5PubMed
6CrossRef
7Academic OneFile (A&I only)
8ProQuest Central (Corporate)
9Health & Medical Collection
10ProQuest Central (purchase pre-March 2016)
11Medical Database (Alumni Edition)
12Science Database (Alumni Edition)
13STEM Database
14ProQuest SciTech Collection
15ProQuest Natural Science Collection
16Hospital Premium Collection
17Hospital Premium Collection (Alumni Edition)
18ProQuest Central (Alumni) (purchase pre-March 2016)
19ProQuest Central (Alumni Edition)
20ProQuest Central Essentials
21Biological Science Collection
22ProQuest Central
23Natural Science Collection
24BMJ Journals
25ProQuest Central Korea
26Health Research Premium Collection
27Health Research Premium Collection (Alumni)
28ProQuest Central Student
29SciTech Premium Collection
30Consumer Health Database (Alumni Edition)
31ProQuest Health & Medical Complete (Alumni)
32ProQuest Biological Science Collection
33Consumer Health Database
34Health & Medical Collection (Alumni Edition)
35Medical Database
36Science Database
37Biological Science Database
38ProQuest One Academic Eastern Edition
39ProQuest One Academic
40ProQuest One Academic UKI Edition
41ProQuest Central China
42ProQuest Central Basic
43MEDLINE - Academic
44Immunology Abstracts
45AIDS and Cancer Research Abstracts
46OpenAIRE (Open Access)
47OpenAIRE
48PubMed Central (Full Participant titles)
jtitleAnnals of the Rheumatic Diseases
delivery
delcategoryRemote Search Resource
fulltextno_fulltext
addata
au
0Zhou, Xiaodong
1Wang, Jiucun
2Zou, Hejian
3Ward, Michael M
4Weisman, Michael H
5Espitia, Maribel G
6Xiao, Xiangjun
7Petersdorf, Effie
8Mignot, Emmanuel
9Martin, Javier
10Gensler, Lianne S
11Scheet, Paul
12Reveille, John D
formatjournal
genrearticle
ristypeJOUR
atitleMICA, a gene contributing strong susceptibility to ankylosing spondylitis
jtitleAnnals of the Rheumatic Diseases
addtitleAnn Rheum Dis
date2014-08
risdate2014
volume73
issue8
spage1552
epage1557
pages1552-1557
issn0003-4967
eissn1468-2060
codenARDIAO
abstractObjective The human major histocompatibility complex class I chain-related gene A (MICA) controls the immune process by balancing activities of  natural killer cells, γδ T cells and αβ CD8 T cells, and immunosuppressive CD4 T cells. MICA is located near HLA-B on chromosome 6. Recent genomewide association studies indicate that genes most strongly linked to ankylosing spondylitis (AS) susceptibility come from the region containing HLA-B and MICA. While HLA-B27 is a well-known risk genetic marker for AS, the potential effect of linkage disequilibrium (LD) shields any associations of genes around HLA-B with AS. The aim of this study was to investigate a novel independent genetic association of MICA to AS. Methods We examined 1543 AS patients and 1539 controls from two ethnic populations by sequencing MICA and genotyping HLA-B alleles. Initially, 1070 AS patients and 1003 controls of European ancestry were used as a discovery cohort, followed by a confirmation cohort of 473 Han Chinese AS patients and 536 controls. We performed a stratified analysis based on HLA-B27 carrier status. We also conducted logistic regression with a formal interaction term. Results Sequencing of MICA identified that MICA*007:01 is a significant risk allele for AS in both Caucasian and Han Chinese populations, and that MICA*019 is a major risk allele in Chinese AS patients. Conditional analysis of MICA alleles on HLA-B27 that unshielded LD effect confirmed associations of the MICA alleles with AS. Conclusions Parallel with HLA-B27, MICA confers strong susceptibility to AS in US white and Han Chinese populations.
copEngland
pubBMJ Publishing Group Ltd
pmid23727634
doi10.1136/annrheumdis-2013-203352
oafree_for_read