Journal
JOURNAL OF CELL BIOLOGY
Volume 217, Issue 9, Pages 3267-3283Publisher
ROCKEFELLER UNIV PRESS
DOI: 10.1083/jcb.201712085
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Funding
- Wellcome Trust (Investigator Award) [110091]
- Medical Research Council [G1001044]
- Swedish Foundation for Strategic Research
- Swedish Cancer Foundation
- Manchester Collaborative Centre for Inflammation Research
- precompetitive open-innovation award from GlaxoSmithKline
- AstraZeneca
- University of Manchester
- European Molecular Biology Organization Short Term Fellowship [ASTF 183-2016]
- MRC [G1001044] Funding Source: UKRI
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Natural Killer (NK) cells can engage multiple virally infected or tumor cells sequentially and deliver perforin for cytolytic killing of these targets. Using microscopy to visualize degranulation from individual NK cells, we found that repeated activation via the Fc receptor CD16 decreased the amount of perforin secreted. However, perforin secretion was restored upon subsequent activation via a different activating receptor, NKG2D. Repeated stimulation via NKG2D also decreased perforin secretion, but this was not rescued by stimulation via CD16. These different outcomes of sequential stimulation could be accounted for by shedding of CD16 being triggered by cellular activation. The use of pharmacological inhibitors and NK cells transfected to express a noncleavable form of CD16 revealed that CD16 shedding also increased NK cell motility and facilitated detachment of NK cells from target cells. Disassembly of the immune synapse caused by CD16 shedding aided NK cell survival and boosted serial engagement of target cells. Thus, counterintuitively, shedding of CD16 may positively impact immune responses.
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