Mir-17–92 regulates bone marrow homing of plasma cells and production of immunoglobulin G2c
The polycistronic mir-17–92 cluster, also known as oncomir-1 , was previously shown to be essential for early B lymphopoiesis. However, its role in late-stage B-cell differentiation and function remains unexplored. Here we ablate mir-17–92 in mature B cells and demonstrate that mir-17–92 is dispensa...
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Published in | Nature communications Vol. 6; no. 1; p. 6764 |
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Main Authors | , , , , , , |
Format | Journal Article |
Language | English |
Published |
London
Nature Publishing Group UK
17.04.2015
Nature Publishing Group |
Subjects | |
Online Access | Get full text |
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Summary: | The polycistronic
mir-17–92
cluster, also known as
oncomir-1
, was previously shown to be essential for early B lymphopoiesis. However, its role in late-stage B-cell differentiation and function remains unexplored. Here we ablate
mir-17–92
in mature B cells and demonstrate that
mir-17–92
is dispensable for conventional B-cell development in the periphery. Interestingly,
mir-17–92
-deficiency in B cells leads to enhanced homing of plasma cells to the bone marrow during T-cell-dependent immune response and selectively impairs IgG2c production. Mechanistically,
mir-17–92
directly represses the expression of Sphingosine 1-phosphate receptor 1 and transcription factor IKAROS, which are, respectively, important for plasma cell homing and IgG2c production. We further show that deletion of
mir-17–92
could reduce IgG2c anti-DNA autoantibody production and hence mitigate immune complex glomerulonephritis in Shp1-deficient mice prone to autoimmunity. Our results identify important roles for
mir-17–92
in the regulation of peripheral B-cell function.
After activation and selection, plasma cells home to the bone marrow where they persist and continue to make antibodies. Here the authors show that the
mir-17–92
cluster coordinates the process by regulating the homing receptor S1PR1 and the transcription factor IKAROS that controls IgG2c production. |
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Bibliography: | ObjectType-Article-1 SourceType-Scholarly Journals-1 ObjectType-Feature-2 content type line 23 |
ISSN: | 2041-1723 2041-1723 |
DOI: | 10.1038/ncomms7764 |