2016
DOI: 10.1155/2016/5758192
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Complement Receptor Type 1 Suppresses Human B Cell Functions in SLE Patients

Abstract: Complement receptors (CRs) play an integral role in innate immunity and also function to initiate and shape the adaptive immune response. Our earlier results showed that complement receptor type 1 (CR1, CD35) is a potent inhibitor of the B cell receptor- (BCR-) induced functions of human B lymphocytes. Here we show that this inhibition occurs already at the initial steps of B cell activation since ligation of CR1 reduces the BCR-induced phosphorylation of key signaling molecules such as Syk and mitogen activat… Show more

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Cited by 15 publications
(27 citation statements)
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“…Whereas the role of human CR2 in B-cell activation is relatively well-established, much less is known about the exact function of CR1 (CD35). In contrast to CR2, CR1 has been described to mediate inhibitory signals ( 157 159 ). CR1 ligands include aggregated C3 and aggregated C3(H 2 O), which in contrast do not bind to CR2.…”
Section: Complement and Adaptive Immunitymentioning
confidence: 99%
“…Whereas the role of human CR2 in B-cell activation is relatively well-established, much less is known about the exact function of CR1 (CD35). In contrast to CR2, CR1 has been described to mediate inhibitory signals ( 157 159 ). CR1 ligands include aggregated C3 and aggregated C3(H 2 O), which in contrast do not bind to CR2.…”
Section: Complement and Adaptive Immunitymentioning
confidence: 99%
“…Having stressed the potential importance of this novel mechanism, we also understand that the causes of anti-nuclear autoantibodies and SLE disease are complex and are not explained by single mechanisms. For example, because C1s is effectively activated after C1 incubation with the nucleoli, it is also expected to cleave C4 and cause C4b deposition on the nucleoli to trigger C4b-mediated clearance and B cell tolerance (13,43,44).…”
Section: Discussionmentioning
confidence: 99%
“…Because apoptotic bodies are known to accumulate in SLE patients and, in mice, injection of dead cells causes antinuclear autoimmunity (11,13,41,42), the clearance functions of C1q and C4 are clearly relevant to SLE pathogenesis. However, other mechanisms may also be important by which these complement proteins increase host tolerance to autologous nuclear Ags, for example, C1q regulation of dendritic cells (DCs) and C4mediated B cell inhibition or tolerance (13,(43)(44)(45)(46). How C1r/C1s deficiency causes SLE has been mainly intuited based on studies of C1q and C4 (28,47).…”
mentioning
confidence: 99%
“…In the germinal centers, C3 degradation fragment‐coated immune complexes are recognized and retained by follicular DCs, enhancing the differentiation of memory and effector B cells . Regulators of complement also limit over‐reaction of the immune system, thus reducing inflammation, but nevertheless allow an antigen‐specific response by B cells . CR2, C4 binding protein, and CD46 modulate immunoglobulin class‐switching of B cells …”
Section: Interaction Between Complement and The Adaptive Immune Systemmentioning
confidence: 99%
“…60,61 Regulators of complement also limit over-reaction of the immune system, thus reducing inflammation, but nevertheless allow an antigen-specific response by B cells. 62,63 CR2, C4 binding protein, and CD46 modulate immunoglobulin class-switching of B cells. [64][65][66] Immune cell-derived complement plays a fundamental role in T-cell differentiation, activation, and expansion.…”
Section: Inter Ac Tion Bet Ween Complement and The Adaptive Immunementioning
confidence: 99%