CD103(+) pulmonary dendritic cells preferentially acquire and present apoptotic cell-associated antigen
Details
Publication Year 2011-08-29, Volume 208, Issue #9, Page 1789-1797
Journal Title
JOURNAL OF EXPERIMENTAL MEDICINE
Publication Type
Journal Article
Abstract
Cells undergoing programmed cell death (apoptosis) are removed in situ by macrophages and dendritic cells (DCs) through a specialized form of phagocytosis (efferocytosis). In the lung, there are two primary DC subsets with the potential to migrate to the local lymph nodes (LNs) and initiate adaptive immune responses. In this study, we show that only CD103(+) DCs were able to acquire and transport apoptotic cells to the draining LNs and cross present apoptotic cell-associated antigen to CD8 T cells. In contrast, both the CD11b(hi) and the CD103(+) DCs were able to ingest and traffic latex beads or soluble antigen. CD103(+) DCs selectively exhibited high expression of TLR3, and ligation of this receptor led to enhanced in vivo cytotoxic T cell responses to apoptotic cell-associated antigen. The selective role for CD103(+) DCs was confirmed in Batf3(-/-) mice, which lack this DC subtype. Our findings suggest that CD103(+) DCs are the DC subset in the lung that captures and presents apoptotic cell-associated antigen under homeostatic and inflammatory conditions and raise the possibility for more focused immunological targeting to CD8 T cell responses.
Publisher
ROCKEFELLER UNIV PRESS
Keywords
BLOOD MONOCYTE SUBSETS; DRAINING LYMPH-NODE; IN-VIVO; DC SUBSETS; LUNG; CD8-ALPHA(+); VIRUS; POPULATIONS; ACTIVATION; MIGRATION
Rights Notice
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Creation Date: 2011-08-29 12:00:00
Last Modified: 0001-01-01 12:00:00
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