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@ARTICLE{Graf:142984,
author = {R. Graf and J. Seagal and K. L. Otipoby and K.-P. Lam and
S. Ayoub and B. Zhang and S. Sander$^*$ and V. T. Chu and K.
Rajewsky},
title = {{BCR}-dependent lineage plasticity in mature {B} cells.},
journal = {Science},
volume = {363},
number = {6428},
issn = {0036-8075},
address = {Cambridge, Mass.},
publisher = {Moses King},
reportid = {DKFZ-2019-00612},
pages = {748 - 753},
year = {2019},
abstract = {B2 cells engage in classical antibody responses, whereas B1
cells are considered carriers of innate immunity, biased
toward recognizing epitopes present on the surfaces of
common pathogens and self antigens. To explore the role of B
cell antigen receptor (BCR) specificity in driving B1 cell
differentiation, we developed a transgenic system allowing
us to change BCR specificity in B cells in an inducible and
programmed manner. Mature B2 cells differentiated into bona
fide B1 cells upon acquisition of a B1 cell-typical
self-reactive BCR through a phase of proliferative
expansion. Thus, B2 cells have B1 cell differentiation
potential in addition to their classical capacity to
differentiate into memory and plasma cells, and B1
differentiation can be instructed by BCR-mediated
self-reactivity, in the absence of B1-lineage
precommitment.},
cin = {D180},
ddc = {500},
cid = {I:(DE-He78)D180-20160331},
pnm = {314 - Tumor immunology (POF3-314)},
pid = {G:(DE-HGF)POF3-314},
typ = {PUB:(DE-HGF)16},
pubmed = {pmid:30765568},
doi = {10.1126/science.aau8475},
url = {https://inrepo02.dkfz.de/record/142984},
}
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