Interrupting CD28 costimulation before antigen rechallenge affects CD8+ T‐cell expansion and effector functions during secondary response in mice |
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| Authors: | Monika Fröhlich Tea Gogishvili Daniela Langenhorst Fred Lühder Thomas Hünig |
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| Affiliation: | 1. Institute for Virology and Immunobiology, University of Würzburg, Würzburg, Germany;2. Department of Medicine II‐Hematology and Medical Oncology, University of Würzburg, Würzburg, Germany;3. Institute for Multiple Sclerosis Research, Department of Neuroimmunology, Gemeinnützige Hertie‐Stiftung and University Medical Centre G?ttingen, G?ttingen, Germany |
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| Abstract: | ![]()
The role of CD28‐mediated costimulation in secondary CD8+ T‐cell responses remains controversial. Here, we have used two tools — blocking mouse anti‐mouse CD28‐specific antibodies and inducible CD28‐deleting mice — to obtain definitive answers in mice infected with ovalbumin‐secreting Listeria monocytogenes. We report that both blockade and global deletion of CD28 reveal its requirement for full clonal expansion and effector functions such as degranulation and IFN‐γ production during the secondary immune response. In contrast, cell‐intrinsic deletion of CD28 in transferred TCR‐transgenic CD8+ T cells before primary infection leads to impaired clonal expansion but an increase in cells able to express effector functions in both primary and secondary responses. We suggest that the proliferation‐impaired CD8+ T cells respond to CD28‐dependent help from their environment by enhanced functional differentiation. Finally, we report that cell‐intrinsic deletion of CD28 after the peak of the primary response does not affect the establishment, maintenance, or recall of long‐term memory. Thus, if given sufficient time, the progeny of primed CD8+ T cells adapt to the absence of this costimulator. |
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| Keywords: | CD28 costimulation CD8+ T cells CD8+ effector cell CD8+ T‐cell memory |
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