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Aberrant B ‐lymphocyte responses in lupus: inherent or induced and potential therapeutic targets
Author(s) -
Taher Taher E.,
Muhammad Hawzheen A.,
Rahim Asad,
FloresBorja Fabian,
Renaudineau Yves,
Isenberg David A.,
Mageed Rizgar A.
Publication year - 2013
Publication title -
european journal of clinical investigation
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.164
H-Index - 107
eISSN - 1365-2362
pISSN - 0014-2972
DOI - 10.1111/eci.12111
Subject(s) - systemic lupus erythematosus , disease , immunology , lymphocyte , context (archaeology) , pathogenesis , autoimmune disease , immune system , biology , medicine , antibody , pathology , paleontology
Background Lupus is a prototype autoimmune disease of unknown aetiology. The disease is complex; manifest diverse clinical symptoms and disease mechanisms. This complexity has provided many leads to explore: from disease mechanisms to approaches for therapy. B ‐lymphocytes play a central role in the pathogenesis of the disease. However, the cause of aberrant B ‐lymphocyte responses in patients and, indeed, its causal relationship with the disease remain unclear. Design This article provides a synopsis of current knowledge of immunological abnormalities in lupus with an emphasis on abnormalities in the B ‐lymphocyte compartment. Results There is evidence for abnormalities in most compartments of the immune system in animal models and patients with lupus including an ever expanding list of abnormalities within the B ‐lymphocyte compartment. In addition, recent genome‐wide linkage analyses in large cohorts of patients have identified new sets of genetic association factors some with potential links with defective B ‐lymphocyte responses although their full pathophysiological effects remain to be determined. The accumulating knowledge may help in the identification and application of new targeted therapies for treating lupus disease. Conclusions Cellular, molecular and genetic studies have provided significant insights into potential causes of immunological defects associated with lupus. Most of this insight relate to defects in B ‐ and T ‐lymphocyte tolerance, signalling and responses. For B ‐lymphocytes, there is evidence for altered regulation of inter and intracellular signalling pathways at multiple levels. Some of these abnormalities will be discussed within the context of potential implications for disease pathogenesis and targeted therapies.

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