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A Fusion of GMCSF and IL-21 Initiates
original article? The American Society of Gene Cell Therapy
Molecular Therapy vol. 18 no. 7, 1293–1301 july 2010 1293
We hypothesized that fusing granulocyte-macrophage
colony-stimulation factor (GMCSF) and interleukin
(IL)-21 as a single bifunctional cytokine (hereafter
GIFT-21) would lead to synergistic anticancer immune
effects because of their respective roles in mediating
inflammation. Mechanistic analysis of GIFT-21 found that
it leads to IL-21Rα-dependent STAT3 hyperactivation
while also contemporaneously behaving as a dominant-
negative inhibitor of GMCSF-driven STAT5 activation.
GIFT-21’s aberrant interactions with its cognate recep-
tors on macrophages resulted in production of 30-fold
greater amounts of IL-6, TNF-α, and MCP-1 when com-
pared to controls. Furthermore, GIFT-21 treatment of
primary B and T lymphocytes leads to STAT1-dependent
apoptosis of IL-21Rα+ lymphocytes. B16 melanoma
cells gene-enhanced to produce GIFT-21 were immune
rejected by syngeneic C57Bl/6 mice comparable to the
effect of IL-21 alone. However, a significant GIFT-21-
driven survival advantage was seen when NOD-SCID
mice were implanted with GIFT-21-secreting B16 cells,
consistent with a meaningful role of macrophages in
tumor rejection. Because GIFT-21 leads to apoptosis of
IL-21Rα+ lymphocytes, we tested its cytolytic effect on
IL-21Rα+ EL-4 lymphoma tumors implanted in C57Bl/6
mice and could demonstrate a significant increase in sur-
vival. These data indicate that GIFT-21 is a novel IL-21Rα
agonist that co-opts IL-21Rα-dependent signaling in a
manner permissive for targeted cancer immunotherapy.
Received 7 December 2009; accepted 2 March 2010; published online
13 April 2010. doi:10.1038/mt.2010.49
IntroductIon
Cellular tumor vaccines can be generated by transfecting autologous
or allogeneic tumor cells with cDNAs encoding for interleukins
(ILs), cytokines, interferons, and molecules accessory to immune
activation.1 The mechanism, by which the secre
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