Targeting B Cells in the Pre-phase of Systemic Autoimmunity Globally Interferes with Autoimmune Pathology

Overview

Journal iScience

Publisher Cell Press

Date 2021 Sep 29

PMID 34585117

Citations 4

Authors

Anja Werner

Simon Schafer

Olga Zaytseva

Heike Albert

Anja Lux

Jasminka Kristic

Marija Pezer

Gordan Lauc

Thomas Winkler

Falk Nimmerjahn

Affiliations

Soon will be listed here.

Abstract

Systemic lupus erythematosus (SLE) is characterized by a loss of self-tolerance, systemic inflammation, and multi-organ damage. While a variety of therapeutic interventions are available, it has become clear that an early diagnosis and treatment may be key to achieve long lasting therapeutic responses and to limit irreversible organ damage. Loss of humoral tolerance including the appearance of self-reactive antibodies can be detected years before the actual onset of the clinical autoimmune disease, representing a potential early point of intervention. Not much is known, however, about how and to what extent this pre-phase of disease impacts the onset and development of subsequent autoimmunity. By targeting the B cell compartment in the pre-disease phase of a spontaneous mouse model of SLE we now show, that resetting the humoral immune system during the clinically unapparent phase of the disease globally alters immune homeostasis delaying the downstream development of systemic autoimmunity.

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