Expression of the serpin serine protease inhibitor 6 protects dendritic cells from cytotoxic T lymphocyte–induced apoptosis: differential modulation by T helper type 1 …

JP Medema, DH Schuurhuis, D Rea… - The Journal of …, 2001 - rupress.org
JP Medema, DH Schuurhuis, D Rea, J van Tongeren, J de Jong, SA Bres, S Laban…
The Journal of experimental medicine, 2001rupress.org
Dendritic cells (DCs) play a central role in the immune system as they drive activation of T
lymphocytes by cognate interactions. However, as DCs express high levels of major
histocompatibility complex class I, this intimate contact may also result in elimination of DCs
by activated cytotoxic T lymphocytes (CTLs) and thereby limit induction of immunity. We
show here that immature DCs are indeed susceptible to CTL-induced killing, but become
resistant upon maturation with anti-CD40 or lipopolysaccharide. Protection is achieved by …
Dendritic cells (DCs) play a central role in the immune system as they drive activation of T lymphocytes by cognate interactions. However, as DCs express high levels of major histocompatibility complex class I, this intimate contact may also result in elimination of DCs by activated cytotoxic T lymphocytes (CTLs) and thereby limit induction of immunity. We show here that immature DCs are indeed susceptible to CTL-induced killing, but become resistant upon maturation with anti-CD40 or lipopolysaccharide. Protection is achieved by expression of serine protease inhibitor (SPI)-6, a member of the serpin family that specifically inactivates granzyme B and thereby blocks CTL-induced apoptosis. Anti-CD40 and LPS-induced SPI-6 expression is sustained for long periods of time, suggesting a role for SPI-6 in the longevity of DCs. Importantly, T helper 1 cells, which mature DCs and boost CTL immunity, induce SPI-6 expression and subsequent DC resistance. In contrast, T helper 2 cells neither induce SPI-6 nor convey protection, despite the fact that they trigger DC maturation with comparable efficiency. Our data identify SPI-6 as a novel marker for DC function, which protects DCs against CTL-induced apoptosis.
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