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Decreased production of class-switched antibodies in neonatal B cells is associated with increased expression of miR-181b.


ABSTRACT: The increased susceptibility to infections of neonates is caused by an immaturity of the immune system as a result of both qualitative and quantitative differences between neonatal and adult immune cells. With respect to B cells, neonatal antibody responses are known to be decreased. Accountable for this is an altered composition of the neonatal B cell compartment towards more immature B cells. However, it remains unclear whether the functionality of individual neonatal B cell subsets is altered as well. In the current study we therefore compared phenotypical and functional characteristics of corresponding neonatal and adult B cell subpopulations. No phenotypic differences could be identified with the exception of higher IgM expression in neonatal B cells. Functional analysis revealed differences in proliferation, survival, and B cell receptor signaling. Most importantly, neonatal B cells showed severely impaired class-switch recombination (CSR) to IgG and IgA. This was associated with increased expression of miR-181b in neonatal B cells. Deficiency of miR-181b resulted in increased CSR. With this, our results highlight intrinsic differences that contribute to weaker B cell antibody responses in newborns.

SUBMITTER: Glaesener S 

PROVIDER: S-EPMC5794184 | biostudies-literature | 2018

REPOSITORIES: biostudies-literature

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Decreased production of class-switched antibodies in neonatal B cells is associated with increased expression of miR-181b.

Glaesener Stephanie S   Jaenke Christine C   Habener Anika A   Geffers Robert R   Hagendorff Petra P   Witzlau Katrin K   Imelmann Esther E   Krueger Andreas A   Meyer-Bahlburg Almut A  

PloS one 20180201 2


The increased susceptibility to infections of neonates is caused by an immaturity of the immune system as a result of both qualitative and quantitative differences between neonatal and adult immune cells. With respect to B cells, neonatal antibody responses are known to be decreased. Accountable for this is an altered composition of the neonatal B cell compartment towards more immature B cells. However, it remains unclear whether the functionality of individual neonatal B cell subsets is altered  ...[more]

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