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Network analysis identifies proinflammatory plasma cell polarization for secretion of ISG15 in human autoimmunity


ABSTRACT: Plasma cells (PCs) as effectors of humoral immunity produce immunoglobulins to match pathogenic insult. However, emerging data suggests more diverse roles for PCs as regulators of immune and inflammatory responses via secretion of factors other than immunoglobulins. The extent to which such responses are pre-programmed in B-lineage cells or can be induced in PCs by the microenvironment is unknown. Here we dissect the impact of IFNs on the regulatory networks of human plasma cells. We show that core PC programs are unaffected, while PCs respond to IFNs with distinctive transcriptional responses. The ISG15-system emerges as a major transcriptional output induced in a sustained fashion by IFN-α in PCs and linked both to intracellular conjugation and ISG15 secretion. This leads to the identification of ISG15-secreting plasmablasts/PCs in patients with active SLE. Thus ISG15-secreting PCs represent a distinct pro-inflammatory PC subset providing an immunoglobulin-independent mechanism of PC action in human autoimmunity B-cells were isolated from the peripheral blood of three adult donors and differentiated in vitro (see individual samples for culture conditions)

ORGANISM(S): Homo sapiens

SUBMITTER: Matthew Care 

PROVIDER: E-GEOD-75007 | biostudies-arrayexpress |

REPOSITORIES: biostudies-arrayexpress

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Network Analysis Identifies Proinflammatory Plasma Cell Polarization for Secretion of ISG15 in Human Autoimmunity.

Care Matthew A MA   Stephenson Sophie J SJ   Barnes Nicholas A NA   Fan Im I   Zougman Alexandre A   El-Sherbiny Yasser M YM   Vital Edward M EM   Westhead David R DR   Tooze Reuben M RM   Doody Gina M GM  

Journal of immunology (Baltimore, Md. : 1950) 20160629 4


Plasma cells (PCs) as effectors of humoral immunity produce Igs to match pathogenic insult. Emerging data suggest more diverse roles exist for PCs as regulators of immune and inflammatory responses via secretion of factors other than Igs. The extent to which such responses are preprogrammed in B-lineage cells or can be induced in PCs by the microenvironment is unknown. In this study, we dissect the impact of IFNs on the regulatory networks of human PCs. We show that core PC programs are unaffect  ...[more]

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