Departments of Epidemiology and Biomathematics, University of Texas, M.D. Anderson Cancer Center, 1155 Pressler Street, Unit 1340, Houston, Texas 77030, USA
Genetics and Genomics Branch, NIAMS, NIH, 9 Memorial Drive, MSC 0908, Building 9, Room 1W108, Bethesda, Maryland 20892, USA
Mount Sinai Hospital, SLRI, Room 656A, 600 University Avenue, Toronto, Ontario M5G 1X5 Canada
Rowe Program of Human Genetics, Department of Medicine, 4303 Tupper Hall, University of California – Davis, Davis, California 95616, USA
The Rosalind Russell Medical Research Center for Arthritis, Department of Medicine, Division of Rheumatology, University of California at San Francisco, California 94122, USA
Center for Genomics and Human Genetics, North Shore-Feinstein Medical Research Institute, 350 Community Drive, Manhasset, New York 11030, USA
Cancer Research-UK, Institute for Cancer Studies, School of Medicine and Biomedical Sciences, University of Sheffield, Beech Hill Road, Sheffield, S10 2RX, UK
Centre for Integrated Genomic Medical Research, Stopford Building, University of Manchester, Oxford Road, Manchester, M13 9PL, UK
GenHotel-EA 3886, University Evry-Paris 7/AP-HP, Evry-Genopole, Cedex, France
Broad Institute of MIT and Harvard, Brigham and Women's Hospital, Division of Rheumatology, 7 Cambridge Center, Cambridge, Massachusetts 02142, USA
Celera Diagnostics, 1401 Harbor Bay Parkway, Alameda, California 94502, USA
Department of Genetics, Southwest Foundation for Biomedical Research, 7620 Northwest Loop 410, San Antonio, Texas 78227, USA
Abstract
For Genetic Analysis Workshop 15 Problem 2, we organized data from several ongoing studies designed to identify genetic and environmental risk factors for rheumatoid arthritis. Data were derived from the North American Rheumatoid Arthritis Consortium (NARAC), collaboration among Canadian researchers, the European Consortium on Rheumatoid Arthritis Families (ECRAF), and investigators from Manchester, England. All groups used a common standard for defining rheumatoid arthritis, but NARAC also further selected for a more severe phenotype in the probands. Genotyping and family structures for microsatellite-based linkage analysis were provided from all centers. In addition, all centers but ECRAF have genotyped families for linkage analysis using SNPs and these data were additionally provided. NARAC also had additional data from a dense genotyping analysis of a region of chromosome 18 and results from candidate gene studies, which were provided. Finally, smoking influences risk for rheumatoid arthritis, and data were provided from the NARAC study on this behavior as well as some additional phenotypes measuring severity. Several questions could be evaluated using the data that were provided. These include comparing linkage analysis using single-nucleotide polymorphisms versus microsatellites and identifying credible regions of linkage outside the HLA region on chromosome 6p13, which has been extensively documented; evaluating the joint effects of smoking with genetic factors; and identifying more homogenous subsets of families for whom genetic susceptibility might be stronger, so that linkage and association studies may be more efficiently conducted.
Background
Rheumatoid arthritis (RA) is a complex disease with a moderately strong genetic component. The recurrence risk ratio for siblings is typically estimated at around six in Caucasians, but with a broad range of values, primarily because the prevalence in the population is not well characterized
The HLA region on 6p21 has been implicated by numerous studies, and there is consistent evidence that DR alleles contribute to disease risk. The 'shared epitope' hypothesis was proposed by Gregersen et al.
Specific autoantibodies are noted to co-occur with rheumatoid arthritis. Rheumatoid factor (RF) IgM is a measure of active disease correlated with erosive arthritic disease. However, a more newly identified autoantibody, anti-cyclic citrullinated peptide (anti-CCP), is more specific for the disease and is a better predictor of erosive outcome
Additional loci that have been implicated include
Aside from identified genetic factors and sex, few environmental cofactors have yet been identified as affecting risk for rheumatoid arthritis. However, current smoking confers about a two-fold increased risk
The primary goal of the studies that were submitted for the Genetic Analysis Workshop 15 has been to identify genetic factors that predispose for rheumatoid arthritis. Four independent academic groups and one company have provided data for the workshop. In addition, given some previously identified evidence for effects of smoking on rheumatoid arthritis risk and difference in risk according to gender, there is considerable interest in identify gene × environment and gene × gene combinations that yield particularly high risks to individuals for rheumatoid arthritis.
Methods
Data for the workshops were provided by five centers. Two centers (Canada and NARAC) had SNP genotyping performed jointly. The data were transmitted from each center to the University of Texas M.D. Anderson Cancer Center, where the data sets were checked to assure the availability of data definitions and to evaluate the formatting and completeness of the data transfer. Subsequently, data were transmitted to the Southwest Foundation for Biomedical Research for integration and transfer to GAW15 participants. Questions about data integrity or meaning were transmitted to the University of Texas M.D. Anderson Cancer Center, which then interacted with the data providers to obtain answers. All affected subjects in all of the studies met the standard ACR criteria for affection with rheumatoid arthritis
Distribution of selected clinical characteristics among study participants from rheumatoid arthritis studies for GAW15 Problem 2
Study source
US Microsa
US-SNPsb
Canada Affymetrix
Canada Illuminac
France
UK Cohort 1d
UK Cohort 2e
Ascertainment criteria
2 ACR+ sibs, 1 with erosions
2 ACR+ sibs, 1 with erosions
2 ACR+ sibs
2 ACR+ sibs
2 ACR+ sibs
2 ACR+ sibs
Number of families
511
757
79
60
88
174
195
Affected sibs/family
2.13
2.15
2
2
2.18
2.13
2.09
% SE+
71%
79%
N/A
N/A
N/A
90%
82%
% Erosion
95%
97%
39%
N/A
N/A
76%
71%
Median age onset
39.1
38.9
43.8
N/A
N/A
39.3
44.0
% RF+
81.1%
74.3%
71.1%
N/A
N/A
62.5%
56.7%
aNumbers from Jawaheer et al. [17]. One family was eliminated from GAW15 data because one sib did not meet ACR criteria for RA.
bOf these families, 9 had only phenotype information and no SNP genotypes, 509 families have both SNP and microsatellite data, 2 families have microsatellite data only, and 237 have SNP data only.
c47 families have genotype data using both Affymetrix and Illumina platforms.
d174 affected families had microsatellite data and of these 157 also had SNP genotyping.
eSelected microsatellite markers were genotyped for variable numbers of these families.
The North American Rheumatoid Arthritis Consortium study (NARAC)
Microsatellite scans
The familial clustering patterns, association with extra-articular findings, and correlation in ages of onset in most of the NARAC collection have been described by Jawaheer et al.
SNP scans
Illumina performed analysis of about 5600 genome-wide SNPs on all families including 66 families from Katherine Siminovitch, a collaborator in Canada. Results of the analysis of the NARAC Caucasian families were published and indicate previously unreported linkages on chromosomes 2, 4, and 11 along with the known linkage on chromosome 6p
Association mapping
A dense panel of 2719 SNPs were genotyped by Illumina for an approximately 10-kb region of chromosome 18q that showed evidence for linkage in the U.S. and French linkage scans. Of these, 2300 met quality control criteria and have been retained and distributed for analysis. These markers were individually genotyped on 460 cases and 460 controls. Controls were recruited from a New York City population and cases have been recruited from multiple U.S. centers. As a part of the data release process, we also distributed the estimated Northern versus Southern European ancestry of cases and controls
Quantitative phenotypes
Two quantitative phenotypes that are used for identifying RA-affected individuals include anti-CCP and RF-IgM. The heritability of these measures is hard to obtain from the selected sib pairs we are studying. After proband correction, the heritability estimates are 11% and 30%; before correction the heritabilities are 15% and 67%. Linkage analysis of Rf-IgM and anti-CCP phenotypes with microsattelites
Clinical measures
Clinical measures that are available include age at onset, sex, ethnicity, presence of erosions, and duration of disease. Data were also provided concerning the physician-reported severity of disease (JAM scores) as well as the patient's functional status (HAQ scores). Smoking increases risk for rheumatoid arthritis, and limited smoking data are available for families and controls. Digitized hand radiographs are available on the NARAC website. The currently available X-ray scores were derived by a single radiologist at the Bethesda Naval Medical Center. Jawaheer et al. studied clinical characteristics of the study subjects
The European Consortium on Rheumatoid Arthritis Families (ECRAF)
ECRAF provided high-density microsatellite data from 88 families, including 75 affected sib pairs, 12 affected sib trios, and 1 affected sib quaternion typed with 1089 microsatellite markers
United Kingdom – Manchester
The UK group led by Jane Worthington and Sally John provided data from analysis of 10,156 SNP markers that were genotyped and passed quality control filters on 157 families
Canada – Toronto
The Canadian group, led by Katherine Siminovitch, provided 60 families that have been genotyped using the Illumina platform used by NARAC (performed at the same time as the NARAC study) as well as 79 families (one sib pair had only one affected sibling and is excluded from tabulations) that were genotyped using an Affymetrix 100 K platform. Patients (
Discussion
Although previous research has identified a few loci that consistently show association with rheumatoid arthritis, a great deal remains unknown about the mechanisms by which genetic factors interrelate to increase disease risk, and the impact that environmental factors such as smoking behavior have upon disease risk. The collaborative approach that has been adopted by rheumatoid arthritis researchers provided an excellent platform for integrating data from multiple sites in an effort to obtain a larger and more powerful collection of data resources than was possible from a single site. In addition, the Genetic Analysis Workshop platform allowed the data to be more thoroughly and impartially queried than is possible by any of the single collaborating sites. The following sets of questions were posed to the GAW participants:
1. When analyzing dense SNP data and when parental data are missing what is the best procedure for dealing with linkage disequilibrium? We have noted some very high LOD scores in both the Canadian and NARAC data sets that can be eliminated by removing excess LD, but does this lead to an excess loss of information?
2. How best to analyze data from the pseudo-autosomal region?
3. Is there evidence for gene × environment interactions? Do
4. Do the quantitative variables provide any increased power to identify genetic loci? Although microsatellite data have been analyzed for the quantitative traits, at this time the SNP data have not yet been analyzed.
5. Meta-analysis: What are the best ways to combine data across the studies? Is there any strong evidence for gene × gene interactions? Is there more than one locus on chromosome 6 influencing disease risk? Can the
6. Association data: Are there any loci on chromosome 18 that reliably predict disease risk? Are there any subsets with particularly high risks for disease?
Conclusion
The data that were provided is composed largely of affected sib-pairs. Efforts were made to collect extended relatives when they were available. However, the aggregation of rheumatoid arthritis in families usually occurs in siblings and parents of the proband and only rarely occurs in extended pedigrees. Due to fiscal constraints, only a few of the families from NARAC included unaffected relatives, and none of the other sites provided data from unaffected relatives. A variety of methods are required to unravel the complex genetic and environmental interactions that cause this complex disease. The value of the genetic analysis workshop has been that it brings together analysts with a wide variety of skills and approaches. The data providers were thankful for the opportunity to have the extensive data that have been developed and studied in detail by a wide range of analysts.
Competing interests
The authors report the following competing interests relating to this publication. Dr. Lindsey Criswell reports receiving consulting fees from Celera Diagnostics. Dr Ann Begovich is an employee of Celera which funded some of the genotyping work included in this manuscript.
Acknowledgements
We thank Toi Soh for assistance in preparing this paper. The research performed in this study has been supported by NIH grant AR44422, NIH contract N01-AR-7-2232, funding from Genome Canada and Associations AFP, Polyarctique-Groupe Taitbout and Rhumatisme et Travail. Funding for UK researchers was provided by the arthritis research campaign.
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