Review for "Divergent chemokine receptor expression and the consequence for human IgG4 B cell responses"

Author(s):  
Louisa James
2020 ◽  
Vol 50 (8) ◽  
pp. 1113-1125
Author(s):  
Peter‐Paul A. Unger ◽  
Laura C. Lighaam ◽  
Ellen Vermeulen ◽  
Simone Kruithof ◽  
Mateusz Makuch ◽  
...  

Author(s):  
Peter-Paul A. Unger ◽  
Laura C. Lighaam ◽  
Ellen Vermeulen ◽  
Simone Kruithof ◽  
Mateusz Makuch ◽  
...  

2012 ◽  
Vol 209 (10) ◽  
pp. 1825-1840 ◽  
Author(s):  
Craig P. Chappell ◽  
Kevin E. Draves ◽  
Natalia V. Giltiay ◽  
Edward A. Clark

Dendritic cells (DCs) are best known for their ability to activate naive T cells, and emerging evidence suggests that distinct DC subsets induce specialized T cell responses. However, little is known concerning the role of DC subsets in the initiation of B cell responses. We report that antigen (Ag) delivery to DC-inhibitory receptor 2 (DCIR2) found on marginal zone (MZ)–associated CD8α− DCs in mice leads to robust class-switched antibody (Ab) responses to a T cell–dependent (TD) Ag. DCIR2+ DCs induced rapid up-regulation of multiple B cell activation markers and changes in chemokine receptor expression, resulting in accumulation of Ag-specific B cells within extrafollicular splenic bridging channels as early as 24 h after immunization. Ag-specific B cells primed by DCIR2+ DCs were remarkably efficient at driving naive CD4 T cell proliferation, yet DCIR2-induced responses failed to form germinal centers or undergo affinity maturation of serum Ab unless toll-like receptor (TLR) 7 or TLR9 agonists were included at the time of immunization. These results demonstrate DCIR2+ DCs have a unique capacity to initiate extrafollicular B cell responses to TD Ag, and thus define a novel division of labor among splenic DC subsets for B cell activation during humoral immune responses.


2003 ◽  
Vol 15 (5) ◽  
pp. 277-286 ◽  
Author(s):  
Daniel J Campbell ◽  
Gudrun F Debes ◽  
Brent Johnston ◽  
Eric Wilson ◽  
Eugene C Butcher

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