Lifeguard Inhibits Fas Ligand-mediated Endoplasmic Reticulum-Calcium Release Mandatory for Apoptosis in Type II Apoptotic Cells

Urresti, Jorge; Ruiz‐Meana, Marisol; Coccia, Elena; Arévalo, Juan Carlos; Castellano, José; Fernández-Sanz, Celia; Galenkamp, Koen M.O.; Planells-Ferrer, Laura; Moubarak, Rana S.; Llecha-Cano, N; Reix, Stéphanie; Garcı́a-Dorado, David; Barneda-Zahonero, Bruna; Comella, Joan X.

doi:10.1074/jbc.m115.677682

Cited by 22 publications

(23 citation statements)

References 49 publications

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“…We found more neurogenesis (BrdU positive neurons) in the hippocampus 8 weeks after pneumococcal infection, improved learning after meningitis, and more pronounced sprouting 90 days after MPTP intoxication 3,4 . These findings are consistent with the now established role of Fas/CD95 for regenerative processes, including proliferation and differentiation of neuronal precursors and neurite outgrowth 30,24,31 . It is tempting to speculate that facilitating these regenerative effects of Fas/CD95 signaling is the "purpose" of the Faim2 downregulation observed in disease states.…”

supporting

confidence: 91%

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The two sides of Faim2 -- modulation of cell death and regeneration

Falkenburger¹,

Aachen²

2017

J Neurol Neuromedicine

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supporting

confidence: 91%

“…Faim2 has been shown to physically interact with Fas and prevent downstream activation of caspases 7,8,24 . Still, it is unclear whether the interaction of Faim2 with Fas prevents Fas trimerization, ligand binding, trafficking, or formation of the "death inducing signaling complex" with FADD and the initiator caspase 8.…”

mentioning

confidence: 99%

The two sides of Faim2 -- modulation of cell death and regeneration

Falkenburger¹,

Aachen²

2017

J Neurol Neuromedicine

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“…Efficient release of apoptotic proteins from the intermembrane space of mitochondria depends on a stimulus-triggered increase in cytosolic Ca 2+ [15]. In CD95 signaling, CD95L-induced Ca 2+ efflux from the endoplasmic reticulum is important for mitochondrial permeabilization and CD95-mediated apoptosis [16, 17]. We analyzed TRAIL-induced changes in cytosolic Ca 2+ under hypoxic and normoxic conditions (Figure 3A).…”

Section: Resultsmentioning

confidence: 99%

Hypoxia regulates TRAIL sensitivity of colorectal cancer cells through mitochondrial autophagy

et al. 2016

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The capacity of tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) to selectively induce cell death in malignant cells triggered numerous attempts for therapeutic exploitation. In clinical trials, however, TRAIL did not live up to the expectations, as tumors exhibit high rates of TRAIL resistance in vivo. Response to anti-cancer therapy is determined not only by cancer cell intrinsic factors (e.g. oncogenic mutations), but also modulated by extrinsic factors such as the hypoxic tumor microenvironment.Here, we address the effect of hypoxia on pro-apoptotic TRAIL signaling in colorectal cancer cells. We show that oxygen levels modulate susceptibility to TRAIL-induced cell death, which is severely impaired under hypoxia (0.5% O2). Mechanistically, this is attributable to hypoxia-induced mitochondrial autophagy. Loss of mitochondria under hypoxia restricts the availability of mitochondria-derived pro-apoptotic molecules such as second mitochondria-derived activator of caspase (SMAC), thereby disrupting amplification of the apoptotic signal emanating from the TRAIL death receptors and efficiently blocking cell death in type-II cells. Moreover, we identify strategies to overcome TRAIL resistance in low oxygen environments. Counteracting hypoxia-induced loss of endogenous SMAC by exogenous substitution of SMAC mimetics fully restores TRAIL sensitivity in colorectal cancer cells. Alternatively, enforcing a mitochondria-independent type-I mode of cell death by targeting the type-II phenotype gatekeeper X-linked inhibitor of apoptosis protein (XIAP) is equally effective.Together, our results indicate that tumor hypoxia impairs TRAIL efficacy but this limitation can be overcome by combining TRAIL with SMAC mimetics or XIAP-targeting drugs. Our findings may help to exploit the potential of TRAIL in cancer therapy.

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“…This appears to occur through its regulation by PI3K. Another mechanism through which LFG regulates apoptosis is via interaction with Bcl-X L and Bcl-2 at the ER to inhibit calcium release (Urresti et al, 2016). This interaction with Bcl-X L is contrary to previous findings where LFG was shown to interact with Bax (Reimers et al, 2006).…”

Section: Introductionmentioning

confidence: 67%

“…The CG3814-induced phenotypes may occur through a mechanism that does not involve interaction with pro-survival Bcl-2 proteins at the ER membrane (Urresti et al, 2016), to regulate the release of calcium from the ER. Therefore, knockdown of CG3814/ LFG in the neurons appears to result in neuronal degeneration and death.…”

Section: Discussionmentioning

confidence: 99%

Knockdown of the putative Lifeguard homologue CG3814 in neurons of Drosophila melanogaster

M’Angale

Staveley

2016

Genet. Mol. Res.

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ABSTRACT.Lifeguard is an integral transmembrane protein that modulates FasL-mediated apoptosis by interfering with the activation of caspase 8. It is evolutionarily conserved, with homologues present in plants, nematodes, zebra fish, frog, chicken, mouse, monkey, and human. The Lifeguard homologue in Drosophila, CG3814, contains the Bax inhibitor-1 family motif of unknown function. Downregulation of Lifeguard disrupts cellular homeostasis and disease by sensitizing neurons to FasL-mediated apoptosis. We used bioinformatic analyses to identify CG3814, a putative homologue of Lifeguard, and knocked down CG3814/LFG expression under the control of the Dopa decarboxylase (Ddc-Gal4) transgene in Drosophila melanogaster neurons to investigate whether it possesses neuroprotective activity. Knockdown of CG3814/LFG in Ddc-Gal4-expressing neurons resulted in a shortened lifespan and impaired locomotor ability, phenotypes that are strongly associated with the degeneration and loss of dopaminergic neurons. Lifeguard interacts with anti-apoptotic Bcl-2 proteins and possibly pro-apoptotic proteins to exert its neuroprotective function. The co-expression of Buffy, the sole anti-apoptotic Bcl-2 gene family member in Drosophila, and CG3814/LFG by stable inducible RNA interference, suppresses the shortened lifespan and the premature agedependent loss in climbing ability. Suppression of CG3814/LFG in the Drosophila eye reduces the number of ommatidia and increases disruption of the ommatidial array. Overexpression of Buffy, along with the knockdown of CG3814/LFG, counteracts the eye phenotypes. Knockdown of CG3814/LFG in Ddc-Gal4-expressing neurons in Drosophila diminishes its neuroprotective ability and results in a shortened lifespan and loss of climbing ability, phenotypes that are improved upon overexpression of the pro-survival Buffy.

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Lifeguard Inhibits Fas Ligand-mediated Endoplasmic Reticulum-Calcium Release Mandatory for Apoptosis in Type II Apoptotic Cells

Cited by 22 publications

References 49 publications

The two sides of Faim2 -- modulation of cell death and regeneration

The two sides of Faim2 -- modulation of cell death and regeneration

Hypoxia regulates TRAIL sensitivity of colorectal cancer cells through mitochondrial autophagy

Knockdown of the putative Lifeguard homologue CG3814 in neurons of Drosophila melanogaster

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