The chromatin landscape of pathogenic transcriptional cell states in rheumatoid arthritis

Author:

Weinand KathrynORCID,Sakaue SaoriORCID,Nathan AparnaORCID,Jonsson Anna HelenaORCID,Zhang FanORCID,Watts Gerald F. M.,Al Suqri MajdORCID,Zhu Zhu, ,Albrecht Jennifer,Apruzzese William,Banda Nirmal,Barnas Jennifer L.,Bathon Joan M.,Ben-Artzi Ami,Boyce Brendan F.,Boyle David L.,Bridges S. Louis,Bykerk Vivian P.,Campbell Debbie,Carr Hayley L.,Ceponis Arnold,Chicoine Adam,Cordle Andrew,Curtis Michelle,Deane Kevin D.,DiCarlo Edward,Dunn Patrick,Filer Andrew,Firestein Gary S.,Forbess Lindsy,Geraldino-Pardilla Laura,Goodman Susan M.,Gravallese Ellen M.,Gregersen Peter K.,Guthridge Joel M.,Gutierrez-Arcelus Maria,Gurajala Siddarth,Holers V. Michael,Horowitz Diane,Hughes Laura B.,Ishigaki Kazuyoshi,Ivashkiv Lionel B.,James Judith A.,Kang Joyce B.,Keras Gregory,Korsunsky Ilya,Lakhanpal Amit,Lederer James A.,Li Zhihan J.,Li Yuhong,Liao Katherine P.,Mandelin Arthur M.,Mantel Ian,Maybury Mark,McDavid Andrew,Mears Joseph,Meednu Nida,Millard Nghia,Moreland Larry W.,Nerviani Alessandra,Orange Dana E.,Perlman Harris,Pitzalis Costantino,Rangel-Moreno Javier,Raza Karim,Reshef Yakir,Ritchlin Christopher,Rivellese Felice,Robinson William H.,Rumker Laurie,Sahbudin Ilfita,Scheel-Toellner Dagmar,Seifert Jennifer A.,Slowikowski Kamil,Smith Melanie H.,Tabechian Darren,Utz Paul J.,Weisenfeld Dana,Weisman Michael H.,Xiao Qian,Rao Deepak A.ORCID,Anolik Jennifer H.ORCID,Brenner Michael B.ORCID,Donlin Laura T.ORCID,Wei KevinORCID,Raychaudhuri SoumyaORCID

Abstract

AbstractSynovial tissue inflammation is a hallmark of rheumatoid arthritis (RA). Recent work has identified prominent pathogenic cell states in inflamed RA synovial tissue, such as T peripheral helper cells; however, the epigenetic regulation of these states has yet to be defined. Here, we examine genome-wide open chromatin at single-cell resolution in 30 synovial tissue samples, including 12 samples with transcriptional data in multimodal experiments. We identify 24 chromatin classes and predict their associated transcription factors, including a CD8 + GZMK+ class associated with EOMES and a lining fibroblast class associated with AP-1. By integrating with an RA tissue transcriptional atlas, we propose that these chromatin classes represent ‘superstates’ corresponding to multiple transcriptional cell states. Finally, we demonstrate the utility of this RA tissue chromatin atlas through the associations between disease phenotypes and chromatin class abundance, as well as the nomination of classes mediating the effects of putatively causal RA genetic variants.

Funder

U.S. Department of Health & Human Services | NIH | National Human Genome Research Institute

U.S. Department of Health & Human Services | NIH | National Institute of Arthritis and Musculoskeletal and Skin Diseases

Uehara Memorial Foundation Osamu Hayaishi Memorial Scholarship

Arthritis National Research Foundation

Burroughs Wellcome Fund Career Awards for Medical Scientists Doris Duke Charitable Foundation Clinical Scientist Development Award Rheumatology Research Foundation Innovative Research Award

Publisher

Springer Science and Business Media LLC

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