Foxo and Fos regulate the decision between cell death and survival in response to UV irradiation

Luo, Xi; Puig, Óscar; Hyun, Joogyung; Bohmann, Dirk; Jasper, Heinrich

doi:10.1038/sj.emboj.7601484

Cited by 122 publications

(156 citation statements)

References 67 publications

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“…As dp53 and the JNK pathway appear to be key factors in apoptosis, we first examined their ability to induce proapoptotic genes. As expected from previous work, 11,12,20,25 both dp53 and JNK can activate hid and rpr: in sal4dp53 and in sal4 hep ACT discs (where hep ACT provides constitutive activity of the JNK pathway 26 ), the two proapoptotic genes become expressed in the spalt (sal) domain (Figures 1d-g). The induction also occurs in discs of the null allelic combination dronc I24 /dronc I29 (hereafter referred to as dronc À ), indicating that hid and rpr induction by dp53 and JNK is not mediated by a feedback loop (Figures 1h-k).…”

Section: Resultsmentioning

confidence: 48%

A dp53/JNK-dependant feedback amplification loop is essential for the apoptotic response to stress in Drosophila

2011

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Programmed cell death (apoptosis) is a conserved process aimed to eliminate unwanted cells. The key molecules are a group of proteases called caspases that cleave vital proteins, which leads to the death of cells. In Drosophila, the apoptotic pathway is usually represented as a cascade of events in which an initial stimulus activates one or more of the proapoptotic genes (hid, rpr, grim), which in turn activate caspases. In stress-induced apoptosis, the dp53 (Drosophila p53) gene and the Jun N-terminal kinase (JNK) pathway function upstream in the activation of the proapoptotic genes. Here we demonstrate that dp53 and JNK also function downstream of proapoptotic genes and the initiator caspase Dronc (Drosophila NEDD2-like caspase) and that they establish a feedback loop that amplifies the initial apoptotic stimulus. This loop plays a critical role in the apoptotic response because in its absence there is a dramatic decrease in the amount of cell death after a pulse of the proapoptotic proteins Hid and Rpr. Thus, our results indicate that stress-induced apoptosis in Drosophila is dependant on an amplification loop mediated by dp53 and JNK. Furthermore, they also demonstrate a mechanism of mutual activation of proapoptotic genes.

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Section: Resultsmentioning

confidence: 48%

A dp53/JNK-dependant feedback amplification loop is essential for the apoptotic response to stress in Drosophila

2011

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“…survival signals results in FOXO translocating to the nucleus from the cytoplasm and inducing apoptosis (19,20). Recently, it was reported that low levels of insulin-like growth factor 1 in human blood induced midgut FOXO activation, resulting in increased Anopheles stephensi lifespan (21).…”

Section: Significancementioning

confidence: 99%

“…JNK activates the transcription factors forkhead box O (FOXO) and Fos, that in turn activate Hid expression (19). FOXO is part of a family of transcription factors that is phosphorylated by Akt or IKK in response to signals promoting survival (19).…”

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confidence: 99%

Plasmodium falciparum evades mosquito immunity by disrupting JNK-mediated apoptosis of invaded midgut cells

Ramphul

Garver

Molina-Cruz

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

105

113

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The malaria parasite, Plasmodium, must survive and develop in the mosquito vector to be successfully transmitted to a new host. The Plasmodium falciparum Pfs47 gene is critical for malaria transmission. Parasites that express Pfs47 (NF54 WT) evade mosquito immunity and survive, whereas Pfs47 knockouts (KO) are efficiently eliminated by the complement-like system. Two alternative approaches were used to investigate the mechanism of action of Pfs47 on immune evasion. First, we examined whether Pfs47 affected signal transduction pathways mediating mosquito immune responses, and show that the Jun-N-terminal kinase (JNK) pathway is a key mediator of Anopheles gambiae antiplasmodial responses to P. falciparum infection and that Pfs47 disrupts JNK signaling. Second, we used microarrays to compare the global transcriptional responses of A. gambiae midguts to infection with WT and KO parasites. The presence of Pfs47 results in broad and profound changes in gene expression in response to infection that are already evident 12 h postfeeding, but become most prominent at 26 h postfeeding, the time when ookinetes invade the mosquito midgut. Silencing of 15 differentially expressed candidate genes identified caspase-S2 as a key effector of Plasmodium elimination in parasites lacking Pfs47. We provide experimental evidence that JNK pathway regulates activation of caspases in Plasmodium-invaded midgut cells, and that caspase activation is required to trigger midgut epithelial nitration. Pfs47 alters the cell death pathway of invaded midgut cells by disrupting JNK signaling and prevents the activation of several caspases, resulting in an ineffective nitration response that makes the parasite undetectable by the mosquito complement-like system.

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“…In Drosophila, JNK has been implicated in development in dorsal and thorax closure, imaginal disc eversion, planar cell polarity. It is also involved in the immune response, response to cellular damage, wound healing, longevity and apoptosis (for reviews covering these topics see [50][51][52] Initial studies have shown that the activation of the Tumor Necrosis Factor/Tumor Necrosis Factor Receptor (TNF/TNFR) system in flies (Eiger/Wengen) induces JNKdependent cell death in stress situations but is not required for developmental apoptosis [53][54][55]. However, a recent study showed that JNK signaling contributed to morphogenetic apoptosis during normal development.…”

Section: Jnk-dependent Cell Deathmentioning

confidence: 99%

Cell death: what can we learn from flies? Editorial for the special review issue on Drosophila apoptosis

Mollereau

2009

Apoptosis

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Foxo and Fos regulate the decision between cell death and survival in response to UV irradiation

Cited by 122 publications

References 67 publications

A dp53/JNK-dependant feedback amplification loop is essential for the apoptotic response to stress in Drosophila

A dp53/JNK-dependant feedback amplification loop is essential for the apoptotic response to stress in Drosophila

Plasmodium falciparum evades mosquito immunity by disrupting JNK-mediated apoptosis of invaded midgut cells

Cell death: what can we learn from flies? Editorial for the special review issue on Drosophila apoptosis

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