STAT92E is a positive regulator of<i>Drosophila</i>inhibitor of apoptosis 1 (DIAP/1) and protects against radiation-induced apoptosis

Betz, Aurel; Ryoo, Hyung Don; Steller, Hermann; Darnell, James

doi:10.1073/pnas.0806291105

Cited by 36 publications

(57 citation statements)

References 29 publications

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“…In the Drosophila developing wing, phosphorylated Stat92E has been shown to be necessary for protection against stress-induced apoptosis, but not for wing developmental apoptosis (Betz et al, 2008). Here we provide evidence that Upd and the JAK/STAT pathway control developmental apoptosis during Drosophila oogenesis.…”

Section: Discussionmentioning

confidence: 55%

JAK/STAT autocontrol of ligand-producing cell number through apoptosis

et al. 2013

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SUMMARYDuring development, specific cells are eliminated by apoptosis to ensure that the correct number of cells is integrated in a given tissue or structure. How the apoptosis machinery is activated selectively in vivo in the context of a developing tissue is still poorly understood. In the Drosophila ovary, specialised follicle cells [polar cells (PCs)] are produced in excess during early oogenesis and reduced by apoptosis to exactly two cells per follicle extremity. PCs act as an organising centre during follicle maturation as they are the only source of the JAK/STAT pathway ligand Unpaired (Upd), the morphogen activity of which instructs distinct follicle cell fates. Here we show that reduction of Upd levels leads to prolonged survival of supernumerary PCs, downregulation of the pro-apoptotic factor Hid, upregulation of the anti-apoptotic factor Diap1 and inhibition of caspase activity. Upd-mediated activation of the JAK/STAT pathway occurs in PCs themselves, as well as in adjacent terminal follicle and interfollicular stalk cells, and inhibition of JAK/STAT signalling in any one of these cell populations protects PCs from apoptosis. Thus, a Stat-dependent unidentified relay signal is necessary for inducing supernumerary PC death. Finally, blocking apoptosis of PCs leads to specification of excess adjacent border cells via excessive Upd signalling. Our results therefore show that Upd and JAK/STAT signalling induce apoptosis of supernumerary PCs to control the size of the PC organising centre and thereby produce appropriate levels of Upd. This is the first example linking this highly conserved signalling pathway with developmental apoptosis in Drosophila.

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Section: Discussionmentioning

confidence: 55%

JAK/STAT autocontrol of ligand-producing cell number through apoptosis

et al. 2013

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“…So far, only isolated studies have implicated JAK/STAT in cell survival (Betz et al, 2008;Hasan et al, 2015;Guarner et al, 2014;Ohayon et al, 2009). For example, the apoptosis inhibitor IAP has been suggested to be a positively regulated target of Stat92E, protecting cells from apoptosis (Betz et al, 2008;Hasan et al, 2015). We identify the JAK/STAT effector Zfh2 as a potential repressor of kay and hid activity -a molecular pathway expected to restrain excessive JNK-activity and induction of apoptosis (Fig.…”

Section: Discussionmentioning

confidence: 99%

“…However, continuous overexpression of Upd can also induce apoptosis (not shown) and, thus potentially also sustained JNK-dependent compensatory proliferation, driving tissue growth. So far, only isolated studies have implicated JAK/STAT in cell survival (Betz et al, 2008;Hasan et al, 2015;Guarner et al, 2014;Ohayon et al, 2009). For example, the apoptosis inhibitor IAP has been suggested to be a positively regulated target of Stat92E, protecting cells from apoptosis (Betz et al, 2008;Hasan et al, 2015).…”

Section: Discussionmentioning

confidence: 99%

“…In fly tumours, STATresponsive enhancers have been mapped (Davie et al, 2015), but few target genes regulating tissue size have been described (Tsai and Sun, 2004;Betz et al, 2008;Hasan et al, 2015). However, several studies suggest that developmental functions of JAK/STAT are mediated by the transcriptional repressors Chinmo (Flaherty et al, 2010), Zfh1 (Ohayon et al, 2009;Leatherman and Dinardo, 2008) and Zfh2 (Perea et al, 2013;Guarner et al, 2014;Ayala-Camargo et al, 2013).…”

Section: Introductionmentioning

confidence: 99%

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JAK/STAT signalling mediates cell survival in response to tissue stress

et al. 2016

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Tissue homeostasis relies on the ability of tissues to respond to stress. Tissue regeneration and tumour models in Drosophila have shown that c-Jun amino-terminal kinase (JNK) acts as a prominent stress-response pathway promoting injury-induced apoptosis and compensatory proliferation. A central question remaining unanswered is how both responses are balanced by activation of a single pathway. Signalling through the Janus kinase/Signal transducers and activators of transcription (JAK/STAT) pathway, which is a potential JNK target, is implicated in promoting compensatory proliferation. While we observe JAK/STAT activation in imaginal discs upon damage, our data demonstrate that JAK/STAT and its downstream effector Zfh2 promote the survival of JNK signalling cells. The JNK component fos and the pro-apoptotic gene hid are regulated in a JAK/STAT-dependent manner. This molecular pathway restrains JNK-induced apoptosis and spatial propagation of JNK signalling, thereby limiting the extent of tissue damage, as well as facilitating systemic and proliferative responses to injury. We find that the pro-survival function of JAK/STAT also drives tumour growth under conditions of chronic stress. Our study defines the function of JAK/STAT in tissue stress and illustrates how crosstalk between conserved signalling pathways establishes an intricate equilibrium between proliferation, apoptosis and survival to restore tissue homeostasis.

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“…This simplicity makes the Drosophila JAK/STAT pathway an ideal target for loss-offunction studies. Such studies have shown that Drosophila JAK/ STAT signaling is involved in diverse biological processes, including early and late development, innate immunity, germ-cell adhesion, and inhibition of apoptosis (6)(7)(8)(9)(10).…”

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confidence: 99%

Cytokine signaling through the JAK/STAT pathway is required for long-term memory in Drosophila

Copf

Goguel²,

Lampin-Saint-Amaux³

et al. 2011

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

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Cytokine signaling through the JAK/STAT pathway regulates multiple cellular responses, including cell survival, differentiation, and motility. Although significant attention has been focused on the role of cytokines during inflammation and immunity, it has become clear that they are also implicated in normal brain function. However, because of the large number of different genes encoding cytokines and their receptors in mammals, the precise role of cytokines in brain physiology has been difficult to decipher. Here, we took advantage of Drosophila's being a genetically simpler model system to address the function of cytokines in memory formation. Expression analysis showed that the cytokine Upd is enriched in the Drosophila memory center, the mushroom bodies. Using tissue-and adult-specific expression of RNAi and dominantnegative proteins, we show that not only is Upd specifically required in the mushroom bodies for olfactory aversive long-term memory but the Upd receptor Dome, as well as the Drosophila JAK and STAT homologs Hop and Stat92E, are also required, while being dispensable for less stable memory forms.

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STAT92E is a positive regulator ofDrosophilainhibitor of apoptosis 1 (DIAP/1) and protects against radiation-induced apoptosis

Cited by 36 publications

References 29 publications

JAK/STAT autocontrol of ligand-producing cell number through apoptosis

JAK/STAT autocontrol of ligand-producing cell number through apoptosis

JAK/STAT signalling mediates cell survival in response to tissue stress

Cytokine signaling through the JAK/STAT pathway is required for long-term memory in Drosophila

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