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T Cell Repertoire Dynamics during Pregnancy in Multiple Sclerosis

Authors :
Nils Schweingruber
Caren Ramien
Alexander Scheffold
Manuel A. Friese
Jan Broder Engler
Stefan M. Gold
Marissa Vignali
Sina C. Rosenkranz
Petra C. Arck
Harlan Robins
Erik Yusko
Kostas Patas
Anne Willing
Christoph Heesen
Catherine Sanders
Kenneth Chan
Stefanie Gamradt
Anja Harrison
Anke Diemert
Eva Tolosa
Ryan O. Emerson
Source :
Cell Reports, Vol 29, Iss 4, Pp 810-815.e4 (2019)
Publication Year :
2019
Publisher :
Elsevier, 2019.

Abstract

Summary: 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. : Ramien et al. interrogate the immune repertoire in multiple sclerosis (MS) during pregnancy. They report a shift in T cell repertoire composition driven by a small number of “private” clones. This specific rather than global immunomodulation may help to explain the protective effect of pregnancy in human autoimmunity. Keywords: multiple sclerosis, pregnancy, T cell receptor α and β pairing, immunosequencing, repertoire sequencing, immune phenotyping, immune tolerance, human

Details

Language :
English
ISSN :
22111247
Volume :
29
Issue :
4
Database :
OpenAIRE
Journal :
Cell Reports
Accession number :
edsair.doi.dedup.....a9c2ac74f53fea3e200326d1b1e4f57e