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CD93 is required for maintenance of antibody secretion and persistence of plasma cells in the bone marrow niche.


ABSTRACT: Plasma cells represent the end stage of B-cell development and play a key role in providing an efficient antibody response, but they are also involved in numerous pathologies. Here we show that CD93, a receptor expressed during early B-cell development, is reinduced during plasma-cell differentiation. High CD93/CD138 expression was restricted to antibody-secreting cells both in T-dependent and T-independent responses as naive, memory, and germinal-center B cells remained CD93-negative. CD93 was expressed on (pre)plasmablasts/plasma cells, including long-lived plasma cells that showed decreased cell cycle activity, high levels of isotype-switched Ig secretion, and modification of the transcriptional network. T-independent and T-dependent stimuli led to re-expression of CD93 via 2 pathways, either before or after CD138 or Blimp-1 expression. Strikingly, while humoral immune responses initially proceeded normally, CD93-deficient mice were unable to maintain antibody secretion and bone-marrow plasma-cell numbers, demonstrating that CD93 is important for the maintenance of plasma cells in bone marrow niches.

SUBMITTER: Chevrier S 

PROVIDER: S-EPMC2656176 | biostudies-literature | 2009 Mar

REPOSITORIES: biostudies-literature

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CD93 is required for maintenance of antibody secretion and persistence of plasma cells in the bone marrow niche.

Chevrier Stéphane S   Genton Céline C   Kallies Axel A   Karnowski Alexander A   Otten Luc A LA   Malissen Bernard B   Malissen Marie M   Botto Marina M   Corcoran Lynn M LM   Nutt Stephen L SL   Acha-Orbea Hans H  

Proceedings of the National Academy of Sciences of the United States of America 20090219 10


Plasma cells represent the end stage of B-cell development and play a key role in providing an efficient antibody response, but they are also involved in numerous pathologies. Here we show that CD93, a receptor expressed during early B-cell development, is reinduced during plasma-cell differentiation. High CD93/CD138 expression was restricted to antibody-secreting cells both in T-dependent and T-independent responses as naive, memory, and germinal-center B cells remained CD93-negative. CD93 was  ...[more]

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