| Literature DB >> 31644905 |
Caren Ramien1, Erik C Yusko2, Jan Broder Engler1, Stefanie Gamradt3, Kostas Patas4, Nils Schweingruber5, Anne Willing1, Sina Cathérine Rosenkranz5, Anke Diemert6, Anja Harrison7, Marissa Vignali2, Catherine Sanders2, Harlan S Robins8, Eva Tolosa9, Christoph Heesen5, Petra C Arck10, Alexander Scheffold11, Kenneth Chan2, Ryan O Emerson2, Manuel A Friese1, Stefan M Gold12.
Abstract
Identifying T cell clones associated with human autoimmunity has remained challenging. Intriguingly, many autoimmune diseases, including multiple sclerosis (MS), show strongly diminished activity during pregnancy, providing a unique research paradigm to explore dynamics of immune repertoire changes during active and inactive disease. Here, we characterize immunomodulation at the single-clone level by sequencing the T cell repertoire in healthy women and female MS patients over the course of pregnancy. Clonality is significantly reduced from the first to third trimester in MS patients, indicating that the T cell repertoire becomes less dominated by expanded clones. However, only a few T cell clones are substantially modulated during pregnancy in each patient. Moreover, relapse-associated T cell clones identified in an individual patient contract during pregnancy and expand during a postpartum relapse. Our data provide evidence that profiling the T cell repertoire during pregnancy could serve as a tool to discover and track "private" T cell clones associated with disease activity in autoimmunity.Entities:
Keywords: T cell receptor α and β pairing; human; immune phenotyping; immune tolerance; immunosequencing; multiple sclerosis; pregnancy; repertoire sequencing
Year: 2019 PMID: 31644905 DOI: 10.1016/j.celrep.2019.09.025
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423