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author Jiang, Simon H.
Athanasopoulos, Vicki
Ellyard, Julia I.
Chuah, Aaron
Cappello, Jean
Cook, Amelia
Prabhu, Savit B.
Cardenas, Jacob
Gu, Jinghua
Stanley, Maurice
Roco, Jonathan A.
Papa, Ilenia
Yabas, Mehmet
Walters, Giles D.
Burgio, Gaetan
McKeon, Kathryn
Byers, James M.
Burrin, Charlotte
Enders, Anselm
Miosge, Lisa A.
Canete, Pablo F.
Jelusic, Marija
Tasic, Velibor
Lungu, Adrian C.
Alexander, Stephen I.
Kitching, Arthur R.
Fulcher, David A.
Shen, Nan
Arsov, Todor
Gatenby, Paul A.
Babon, Jeff J.
Mallon, Dominic F.
de Lucas Collantes, Carmen
Stone, Eric A.
Wu, Philip
Field, Matthew A.
Andrews, Thomas D.
Cho, Eun
Pascual, Virginia
Cook, Matthew C.
Vinuesa, Carola G.
author_facet Jiang, Simon H.
Athanasopoulos, Vicki
Ellyard, Julia I.
Chuah, Aaron
Cappello, Jean
Cook, Amelia
Prabhu, Savit B.
Cardenas, Jacob
Gu, Jinghua
Stanley, Maurice
Roco, Jonathan A.
Papa, Ilenia
Yabas, Mehmet
Walters, Giles D.
Burgio, Gaetan
McKeon, Kathryn
Byers, James M.
Burrin, Charlotte
Enders, Anselm
Miosge, Lisa A.
Canete, Pablo F.
Jelusic, Marija
Tasic, Velibor
Lungu, Adrian C.
Alexander, Stephen I.
Kitching, Arthur R.
Fulcher, David A.
Shen, Nan
Arsov, Todor
Gatenby, Paul A.
Babon, Jeff J.
Mallon, Dominic F.
de Lucas Collantes, Carmen
Stone, Eric A.
Wu, Philip
Field, Matthew A.
Andrews, Thomas D.
Cho, Eun
Pascual, Virginia
Cook, Matthew C.
Vinuesa, Carola G.
author_sort Jiang, Simon H.
collection PubMed
description Systemic lupus erythematosus (SLE) is the prototypic systemic autoimmune disease. It is thought that many common variant gene loci of weak effect act additively to predispose to common autoimmune diseases, while the contribution of rare variants remains unclear. Here we describe that rare coding variants in lupus-risk genes are present in most SLE patients and healthy controls. We demonstrate the functional consequences of rare and low frequency missense variants in the interacting proteins BLK and BANK1, which are present alone, or in combination, in a substantial proportion of lupus patients. The rare variants found in patients, but not those found exclusively in controls, impair suppression of IRF5 and type-I IFN in human B cell lines and increase pathogenic lymphocytes in lupus-prone mice. Thus, rare gene variants are common in SLE and likely contribute to genetic risk.
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spelling pubmed-65252032019-05-20 Functional rare and low frequency variants in BLK and BANK1 contribute to human lupus Jiang, Simon H. Athanasopoulos, Vicki Ellyard, Julia I. Chuah, Aaron Cappello, Jean Cook, Amelia Prabhu, Savit B. Cardenas, Jacob Gu, Jinghua Stanley, Maurice Roco, Jonathan A. Papa, Ilenia Yabas, Mehmet Walters, Giles D. Burgio, Gaetan McKeon, Kathryn Byers, James M. Burrin, Charlotte Enders, Anselm Miosge, Lisa A. Canete, Pablo F. Jelusic, Marija Tasic, Velibor Lungu, Adrian C. Alexander, Stephen I. Kitching, Arthur R. Fulcher, David A. Shen, Nan Arsov, Todor Gatenby, Paul A. Babon, Jeff J. Mallon, Dominic F. de Lucas Collantes, Carmen Stone, Eric A. Wu, Philip Field, Matthew A. Andrews, Thomas D. Cho, Eun Pascual, Virginia Cook, Matthew C. Vinuesa, Carola G. Nat Commun Article Systemic lupus erythematosus (SLE) is the prototypic systemic autoimmune disease. It is thought that many common variant gene loci of weak effect act additively to predispose to common autoimmune diseases, while the contribution of rare variants remains unclear. Here we describe that rare coding variants in lupus-risk genes are present in most SLE patients and healthy controls. We demonstrate the functional consequences of rare and low frequency missense variants in the interacting proteins BLK and BANK1, which are present alone, or in combination, in a substantial proportion of lupus patients. The rare variants found in patients, but not those found exclusively in controls, impair suppression of IRF5 and type-I IFN in human B cell lines and increase pathogenic lymphocytes in lupus-prone mice. Thus, rare gene variants are common in SLE and likely contribute to genetic risk. Nature Publishing Group UK 2019-05-17 /pmc/articles/PMC6525203/ /pubmed/31101814 http://dx.doi.org/10.1038/s41467-019-10242-9 Text en © The Author(s) 2019 Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons license and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/.
spellingShingle Article
Jiang, Simon H.
Athanasopoulos, Vicki
Ellyard, Julia I.
Chuah, Aaron
Cappello, Jean
Cook, Amelia
Prabhu, Savit B.
Cardenas, Jacob
Gu, Jinghua
Stanley, Maurice
Roco, Jonathan A.
Papa, Ilenia
Yabas, Mehmet
Walters, Giles D.
Burgio, Gaetan
McKeon, Kathryn
Byers, James M.
Burrin, Charlotte
Enders, Anselm
Miosge, Lisa A.
Canete, Pablo F.
Jelusic, Marija
Tasic, Velibor
Lungu, Adrian C.
Alexander, Stephen I.
Kitching, Arthur R.
Fulcher, David A.
Shen, Nan
Arsov, Todor
Gatenby, Paul A.
Babon, Jeff J.
Mallon, Dominic F.
de Lucas Collantes, Carmen
Stone, Eric A.
Wu, Philip
Field, Matthew A.
Andrews, Thomas D.
Cho, Eun
Pascual, Virginia
Cook, Matthew C.
Vinuesa, Carola G.
Functional rare and low frequency variants in BLK and BANK1 contribute to human lupus
title Functional rare and low frequency variants in BLK and BANK1 contribute to human lupus
title_full Functional rare and low frequency variants in BLK and BANK1 contribute to human lupus
title_fullStr Functional rare and low frequency variants in BLK and BANK1 contribute to human lupus
title_full_unstemmed Functional rare and low frequency variants in BLK and BANK1 contribute to human lupus
title_short Functional rare and low frequency variants in BLK and BANK1 contribute to human lupus
title_sort functional rare and low frequency variants in blk and bank1 contribute to human lupus
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6525203/
https://www.ncbi.nlm.nih.gov/pubmed/31101814
http://dx.doi.org/10.1038/s41467-019-10242-9
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