AUTOIMMUNE DISEASE. Patients with LRBA Deficiency Show CTLA4 Loss and Immune Dysregulation Responsive to Abatacept Therapy

Overview

Journal Science

Specialty Science

Date 2015 Jul 25

PMID 26206937

Citations 304

Authors

Bernice Lo

Kejian Zhang

Wei Lu

Lixin Zheng

Qian Zhang

Chrysi Kanellopoulou

Yu Zhang

Zhiduo Liu

Jill M Fritz

Rebecca Marsh

Ammar Husami

Diane Kissell

Shannon Nortman

Vijaya Chaturvedi

Hilary Haines

Lisa R Young

Jun Mo

Alexandra H Filipovich

Jack J Bleesing

Peter Mustillo

Michael Stephens

Cesar M Rueda

Claire A Chougnet

Kasper Hoebe

Joshua McElwee

Jason D Hughes

Elif Karakoc-Aydiner

Helen F Matthews

Susan Price

Helen C Su

V Koneti Rao

Michael J Lenardo

Michael B Jordan

Affiliations

Soon will be listed here.

Abstract

Mutations in the LRBA gene (encoding the lipopolysaccharide-responsive and beige-like anchor protein) cause a syndrome of autoimmunity, lymphoproliferation, and humoral immune deficiency. The biological role of LRBA in immunologic disease is unknown. We found that patients with LRBA deficiency manifested a dramatic and sustained improvement in response to abatacept, a CTLA4 (cytotoxic T lymphocyte antigen-4)-immunoglobulin fusion drug. Clinical responses and homology of LRBA to proteins controlling intracellular trafficking led us to hypothesize that it regulates CTLA4, a potent inhibitory immune receptor. We found that LRBA colocalized with CTLA4 in endosomal vesicles and that LRBA deficiency or knockdown increased CTLA4 turnover, which resulted in reduced levels of CTLA4 protein in FoxP3(+) regulatory and activated conventional T cells. In LRBA-deficient cells, inhibition of lysosome degradation with chloroquine prevented CTLA4 loss. These findings elucidate a mechanism for CTLA4 trafficking and control of immune responses and suggest therapies for diseases involving the CTLA4 pathway.

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