Combination of IAP antagonist and IFNγ activates novel caspase-10- and RIPK1-dependent cell death pathways

Tanzer, Maria C.; Khan, Nufail; Rickard, James A; Etemadi, Nima; Lalaoui, Najoua; Spall, Sukhdeep K; Hildebrand, Joanne M; Segal, David; Miasari, Maria; Chau, Diep; Wong, Wendy Wei-Lynn; McKinlay, Mark A.; Chunduru, Srinivas K.; Benetatos, Christopher A.; Condon, Stephen M.; Vince, James E.; Herold, Marco J.; Silke, John

doi:10.1038/cdd.2016.147

Cited by 47 publications

(37 citation statements)

References 60 publications

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“…RIPK1 deubiquitylation can be achieved through the inhibition of cIAP1/2, for instance following SMAC release upon MOMP or by pharmacological SMAC mimetics. The absence of caspase-8 and RIPK3 suffices to block death in mouse cells even in the presence of MLKL following IFNγ and SMAC mimetic treatment (59). However, human caspase-8 and RIPK3 double-deficient HT29 cells die following IFNγ and SMAC mimetic treatment (59).…”

Section: The Fadd-procaspase-8-cflipl Complex Inhibits Necroptosismentioning

confidence: 99%

“…The absence of caspase-8 and RIPK3 suffices to block death in mouse cells even in the presence of MLKL following IFNγ and SMAC mimetic treatment (59). However, human caspase-8 and RIPK3 double-deficient HT29 cells die following IFNγ and SMAC mimetic treatment (59). Death was attributed to IFNγ-induced gene expression, RIPK1 and caspase-10 in human HT29 cells, but independent of TNFR1/2, Fas, TRAILR, TWEAKR, IFNAR and ATG5, a protein essential for autophagy.…”

Section: The Fadd-procaspase-8-cflipl Complex Inhibits Necroptosismentioning

confidence: 99%

“…59 However, human caspase-8 and RIPK3 double-deficient HT29 cells die following IFNγ and SMAC mimetic treatment. 59 Death was attributed to IFNγ-induced gene expression, RIPK1 and caspase-10 in human HT29 cells, but independent of TNFR1/2, Fas, TRAILR, TWEAKR, IFNAR, and ATG5, a protein essential for autophagy. These data hint at the existence of a yet unknown intrinsic signal that mediates death through RIPK1.…”

Section: The Fadd-procaspase-8-cflip L Complex Inhibits Necroptosismentioning

confidence: 99%

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Caspase‐8: regulating life and death

Tummers

Green

2017

Immunological Reviews

513

414

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Summary Roles for cell death in development, homeostasis, and the control of infections and cancer have long been recognized. Whereas excessive cell damage results in passive necrosis, cells can be triggered to engage molecular programs that result in cell death. Such triggers include cellular stress, oncogenic signals that engage tumor suppressor mechanisms, pathogen insults, and immune mechanisms. The best-known forms of programmed cell death are apoptosis and a recently recognized regulated necrosis termed necroptosis. Of the two best understood pathways of apoptosis, the extrinsic and intrinsic (mitochondrial) pathways, the former is induced by the ligation of death receptors, a subset of the TNF receptor (TNFR) superfamily. Ligation of these death receptors can also induce necroptosis. The extrinsic apoptosis and necroptosis pathways regulate each other and their balance determines whether cells live. Integral in the regulation and initiation of death receptor-mediatedactivation of programmed cell death is the aspartate-specific cysteine protease (caspase)-8. This review describes the role of caspase-8 in the initiation of extrinsic apoptosis execution and the mechanism by which caspase-8 inhibits necroptosis. The importance of caspase-8 in development and homeostasis and the way that dysfunctional caspase-8 may contribute to the development of malignancies in mice and humans are also explored.

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Section: The Fadd-procaspase-8-cflipl Complex Inhibits Necroptosismentioning

confidence: 99%

Section: The Fadd-procaspase-8-cflipl Complex Inhibits Necroptosismentioning

confidence: 99%

Section: The Fadd-procaspase-8-cflip L Complex Inhibits Necroptosismentioning

confidence: 99%

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Caspase‐8: regulating life and death

Tummers

Green

2017

Immunological Reviews

513

414

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“…6,7,11 However, TNF or other cytokines, supplied by immune cells are likely to contribute to SM efficacy, especially in tumors that fail to produce TNF upon IAP loss. [12][13][14][15][16][17] In support of this concept, SMs are more efficient in vivo when combined with inflammatory adjuvants, which promote immune cell-derived TNF secretion. 15,18 Similarly, IAP antagonism promotes antitumor immunity in myeloma, independently from cell death induction.…”

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confidence: 91%

PD-L1 and IAPs co-operate to protect tumors from cytotoxic lymphocyte-derived TNF

et al. 2017

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Smac-mimetics are emerging as promising anti-cancer agents and are being evaluated in clinical trials for a variety of malignancies. Smac-mimetics can induce TNF production from a subset of tumor cells and simultaneously sensitize them to TNF-induced apoptosis. However, TNF derived from other cellular sources, such as cytotoxic lymphocytes (CLs) within the tumor, may also contribute to the anti-tumor activity of SMs. Here, we show that CD8 T cells and NK cells potently kill tumor cells in the presence of the SM, birinapant. Enhanced CL killing occurred through TNF secretion upon tumor antigen recognition or NK-activating receptor ligation. Importantly, the perforin/granzyme route to CL-mediated tumor cell killing was dispensable for the efficacy of birinapant, emphasizing the importance of the TNF-mediated apoptosis pathway. Time-lapse microscopy revealed that birinapant sensitized tumor cells to apoptosis as bystanders and to membrane-bound TNF delivered to tumor cells within the immunological synapse. Furthermore, PD-L1 expression on tumor cells suppressed antigen-driven TNF production by CD8 T cells, which could be antagonized through PD-1 blockade. Importantly, the elevated levels of TNF produced upon PD-1 blockade further enhanced tumor cell killing when combined with birinapant. The combined anti-tumor activity of IAP antagonism and PD-1 blockade occurred independently of perforin-mediated tumor cell death. Taken together, we identify CL-derived TNF as a potent effector of birinapant mediated anti-tumor immunity and opportunity for combination therapy through co-inhibition of immune checkpoints.

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“…Other co-agents promoting activation of necroptosis by SMAC mimetics may be proteasome inhibitors, such as bortezomib, or glucocorticoids, which have been recently shown to promote necroptosis in several non-Hodgkin lymphoma and acute lymphoblastic leukemia cell lines expressing low levels of caspase-8 (88, 89). Pro-death activity of SMAC mimetics can also be greatly enhanced by the combination with IFNγ, importantly rendering cell death independent of autocrine TNFα signaling (90,91). In the absence of caspase inhibition, SMAC mimetics and IFNγ induce RIPK1 dependent apoptosis, which is meditated by both caspase-8 and caspase-10.…”

Section: As D I S C U S S E D a B O V E A C T I V A T I O N O F R Imentioning

confidence: 99%