Gene-level association analysis of systemic sclerosis: A comparison of African-Americans and White populations.

Gorlova, Olga Y; Li, Yafang; Gorlov, Ivan; Ying, Jun; Chen, Wei V; Assassi, Shervin; Reveille, John D; Arnett, Frank C; Zhou, Xiaodong; Bossini-Castillo, Lara; Lopez-Isac, Elena; Acosta-Herrera, Marialbert; Gregersen, Peter K; Lee, Annette T; Steen, Virginia D; Fessler, Barri J; Khanna, Dinesh; Schiopu, Elena; Silver, Richard M; Molitor, Jerry A; Furst, Daniel E; Kafaja, Suzanne; Simms, Robert W; Lafyatis, Robert A; Carreira, Patricia; Simeon, Carmen Pilar; Castellvi, Ivan; Beltran, Emma; Ortego, Norberto; Amos, Christopher I; Martin, Javier; Mayes, Maureen D

Gorlova, Olga Y; Li, Yafang; Gorlov, Ivan; Ying, Jun; Chen, Wei V; Assassi, Shervin; Reveille, John D; Arnett, Frank C; Zhou, Xiaodong; Bossini-Castillo, Lara; Lopez-Isac, Elena; Acosta-Herrera, Marialbert; Gregersen, Peter K; Lee, Annette T; Steen, Virginia D; Fessler, Barri J; Khanna, Dinesh; Schiopu, Elena; Silver, Richard M; Molitor, Jerry A; Furst, Daniel E; Kafaja, Suzanne; Simms, Robert W; Lafyatis, Robert A; Carreira, Patricia; Simeon, Carmen Pilar; Castellvi, Ivan; Beltran, Emma; Ortego, Norberto; Amos, Christopher I; Martin, Javier; Mayes, Maureen D.

Afiliação

Gorlova OY; Department of Biomedical Data Science, Geisel School of Medicine, Dartmouth College, Lebanon, NH, United States of America.
Li Y; Department of Biomedical Data Science, Geisel School of Medicine, Dartmouth College, Lebanon, NH, United States of America.
Gorlov I; Department of Biomedical Data Science, Geisel School of Medicine, Dartmouth College, Lebanon, NH, United States of America.
Ying J; Department of Internal Medicine, Division of Rheumatology, University of Texas McGovern Medical School, Houston, TX, United States of America.
Chen WV; Department of Biostatistics, UT MD Anderson Cancer Center, Houston, TX, United States of America.
Assassi S; Department of Internal Medicine, Division of Rheumatology, University of Texas McGovern Medical School, Houston, TX, United States of America.
Reveille JD; Department of Internal Medicine, Division of Rheumatology, University of Texas McGovern Medical School, Houston, TX, United States of America.
Arnett FC; Department of Internal Medicine, Division of Rheumatology, University of Texas McGovern Medical School, Houston, TX, United States of America.
Zhou X; Department of Internal Medicine, Division of Rheumatology, University of Texas McGovern Medical School, Houston, TX, United States of America.
Bossini-Castillo L; Wellcome Trust Sanger Institute, Hinxton, United Kingdom.
Lopez-Isac E; Institute of Parasitology and Biomedicine López-Neyra, IPBLN-CSIC, Granada, Spain.
Acosta-Herrera M; Institute of Parasitology and Biomedicine López-Neyra, IPBLN-CSIC, Granada, Spain.
Gregersen PK; Robert S. Boas Center for Genomics and Human Genetics, Feinstein Institute for Medical Research, Manhasset, NY, United States of America.
Lee AT; Robert S. Boas Center for Genomics and Human Genetics, Feinstein Institute for Medical Research, Manhasset, NY, United States of America.
Steen VD; Division of Rheumatology, Georgetown University Medical Center, Washington, D.C., United States of America.
Fessler BJ; Division of Rheumatology, University of Alabama-Birmingham, Birmingham, AL, United States of America.
Khanna D; Division of Rheumatology, University of Michigan, Ann Arbor, MI, United States of America.
Schiopu E; Division of Rheumatology, University of Michigan, Ann Arbor, MI, United States of America.
Silver RM; Division of Rheumatology, Medical University of South Carolina, Charleston, SC, United States of America.
Molitor JA; Division of Rheumatic and Autoimmune Diseases, University of Minnesota, Minneapolis, MN, United States of America.
Furst DE; Division of Rheumatology, University of California-Los Angeles, Los Angeles, CA, United States of America.
Kafaja S; University of Washington, Seattle, WA, United States of America.
Simms RW; University of Florence, Florence, Italy.
Lafyatis RA; Division of Rheumatology, University of California-Los Angeles, Los Angeles, CA, United States of America.
Carreira P; Division of Rheumatology, Boston University, Boston, MA, United States of America.
Simeon CP; University of Pittsburgh, Pittsburgh, PA, United States of America.
Castellvi I; Department of Rheumatology, Hospital Universitario, Madrid, Spain.
Beltran E; Department of Internal Medicine, Valle de Hebrón Hospital, Barcelona, Spain.
Ortego N; Hospital de la Santa Creu i Sant Pau, Barcelona, Spain.
Amos CI; Hospital Universitario y Politécnico La Fe, Valencia, Spain.
Martin J; University Hospital San Cecilio, Granada, Spain.
Mayes MD; Department of Biomedical Data Science, Geisel School of Medicine, Dartmouth College, Lebanon, NH, United States of America.

PLoS One ; 13(1): e0189498, 2018.

Article em En | MEDLINE | ID: mdl-29293537

RESUMO

Gene-level analysis of ImmunoChip or genome-wide association studies (GWAS) data has not been previously reported for systemic sclerosis (SSc, scleroderma). The objective of this study was to analyze genetic susceptibility loci in SSc at the gene level and to determine if the detected associations were shared in African-American and White populations, using data from ImmunoChip and GWAS genotyping studies. The White sample included 1833 cases and 3466 controls (956 cases and 2741 controls from the US and 877 cases and 725 controls from Spain) and the African American sample, 291 cases and 260 controls. In both Whites and African Americans, we performed a gene-level analysis that integrates association statistics in a gene possibly harboring multiple SNPs with weak effect on disease risk, using Versatile Gene-based Association Study (VEGAS) software. The SNP-level analysis was performed using PLINK v.1.07. We identified 4 novel candidate genes (STAT1, FCGR2C, NIPSNAP3B, and SCT) significantly associated and 4 genes (SERBP1, PINX1, TMEM175 and EXOC2) suggestively associated with SSc in the gene level analysis in White patients. As an exploratory analysis we compared the results on Whites with those from African Americans. Of previously established susceptibility genes identified in Whites, only TNFAIP3 was significant at the nominal level (p = 6.13x10-3) in African Americans in the gene-level analysis of the ImmunoChip data. Among the top suggestive novel genes identified in Whites based on the ImmunoChip data, FCGR2C and PINX1 were only nominally significant in African Americans (p = 0.016 and p = 0.028, respectively), while among the top novel genes identified in the gene-level analysis in African Americans, UNC5C (p = 5.57x10-4) and CLEC16A (p = 0.0463) were also nominally significant in Whites. We also present the gene-level analysis of SSc clinical and autoantibody phenotypes among Whites. Our findings need to be validated by independent studies, particularly due to the limited sample size of African Americans.

Assuntos

População Negra/genética; Estudo de Associação Genômica Ampla; Escleroderma Sistêmico/genética; População Branca/genética; Humanos; Polimorfismo de Nucleotídeo Único

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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Escleroderma Sistêmico / População Negra / População Branca / Estudo de Associação Genômica Ampla Idioma: En Ano de publicação: 2018 Tipo de documento: Article

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