Gene expression in the brain during reovirus encephalitis

et al. 2013

Self Cite

f Reovirus infection is a well-characterized experimental system for the study of viral pathogenesis and antiviral immunity within the central nervous system (CNS). We have previously shown that c-Jun N-terminal kinase (JNK) and the Fas death receptor each play a role in neuronal apoptosis occurring in reovirus-infected brains. Death-associated protein 6 (Daxx) is a cellular protein that mechanistically links Fas signaling to JNK signaling in several models of apoptosis. In the present study, we demonstrate that Daxx is upregulated in reovirus-infected brain tissue through a type I interferon-mediated mechanism. Daxx upregulation is limited to brain regions that undergo reovirus-induced apoptosis and occurs in the cytoplasm and nucleus of neurons. Cytoplasmic Daxx is present in Fas-expressing cells during reovirus encephalitis, suggesting a role for Daxx in Fas-mediated apoptosis following reovirus infection. Further, in vitro expression of a dominant negative form of Daxx (DN-Daxx), which binds to Fas but which does not transmit downstream signaling, inhibits apoptosis of reovirus-infected cells. In contrast, in vitro depletion of Daxx results in increased expression of caspase 3 and apoptosis, suggesting that Daxx plays an antiapoptotic role in the nucleus. Overall, these data imply a regulatory role for Daxx in reovirus-induced apoptosis, depending on its location in the nucleus or cytoplasm.

Section: Brain Expression Of Daxx Mrna and Protein Is Upregulated Dursupporting

confidence: 55%

Section: Brain Expression Of Daxx Mrna and Protein Is Upregulated Durmentioning

confidence: 94%

Section: Brain Expression Of Daxx Mrna and Protein Is Upregulated Durmentioning

confidence: 99%

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Daxx Upregulation within the Cytoplasm of Reovirus-Infected Cells Is Mediated by Interferon and Contributes to Apoptosis

Dionne

Zhuang

et al. 2013

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“…For example, (i) Daxx is upregulated in the spleens of mice infected with neuroinvasive strains of WNV compared to noninvasive strains (23); (ii) the death receptor-associated genes encoding cIAP2, TRAIL, TNF, and TRAF1 are upregulated in WNV-infected human retinal pigment epithelium (24), and (iii) multiple pathways involved in apoptosis, including induction of apoptosis by HIV-1, were identified in the brains of horses with exposure to WNV (25). In addition, we previously performed microarray analysis on RNA extracted from the brains of reovirus-infected mice (26). The expression of all DR-associated WNV-induced genes with an expression change of Ն2 was also significantly changed following infection of the brain with reovirus (not shown), including the gene encoding Daxx (27), suggesting that similar patterns of gene expression are seen in the brain following infection with a variety of viruses.…”

Section: Discussionmentioning

confidence: 99%

Death Receptor-Mediated Apoptotic Signaling Is Activated in the Brain following Infection with West Nile Virus in the Absence of a Peripheral Immune Response

Clarke

Quick

et al. 2014

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Apoptosis is an important mechanism of West Nile virus (WNV) pathogenesis within the central nervous system (CNS).N euronal apoptosis is an important mechanism of virus-induced pathogenesis within the central nervous system (CNS) (1). During West Nile virus (WNV) encephalitis, the proapoptotic executioner caspase, caspase 3, is activated, and mice lacking caspase 3 have reduced neuronal death and tissue injury following West Nile virus infection (2). Despite the importance of apoptosis in WNV pathogenesis, the exact pathways involved in triggering apoptotic cell death in the CNS have not yet been defined.Activation of initiator caspases 8 (3, 4) and 9 (3) occurs in cultured neuronal cells infected with WNV, and inhibition of these initiator caspases leads to reduced cleavage of the caspase 3 substrate poly(ADP-ribose) polymerase (PARP) (3, 4). These studies indicate that both extrinsic and intrinsic apoptotic signaling pathways are activated in vitro following WNV infection and are consistent with in vitro studies demonstrating that mitochondrial apoptotic signaling protein Bax is upregulated in neuronal cells following WNV infection (5) and that cytochrome c is released from the mitochondria (3). However, it remains to be seen whether the same apoptotic pathways are also activated in the intact brain during WNV encephalitis.Innate and adaptive immune responses also influence WNV pathogenesis within the CNS. Toll-like receptors 3 and 7 (TLR3 and TLR7) and the cytoplasmic proteins encoded by retinoic acidinducible gene I (RIG-I) and melanoma-differentiation-associated gene 5 (MDA5) are important for detection of WNV within the CNS, and defects in these, or additional, components of the interferon (IFN) response show enhanced viral burden and increased lethality (6). Although IFN restricts infection, pathogenic WNV strains attenuate IFN function at several steps of the induction and signaling cascade, allowing the virus to establish infection (6). Studies performed in mice (7-11) and humans (12-14) have also highlighted the role of CD8 ϩ T cells and the associated importance of pathways involving Fas ligand (10) and tumor necrosis factor (TNF)-related apoptosis-inducing factor ligand (TRAIL) (15) effector mechanisms in containing WNV CNS infection.In this report, we demonstrate that genes involved in death receptor (DR) apoptotic signaling are upregulated in the mouse brain following WNV infection. We also show for the first time that the activity of the DR-associated initiator caspase, caspase 8, is increased in the brain following WNV infection. WNV-induced activation of caspase 8 in the CNS is associated with cleavage of the proapoptotic Bcl-2 family protein Bid and with activation of caspase 9, suggesting that the caspase 8-dependent cleavage of Bid promotes intrinsic apoptotic signaling within the brains of infected animals. Utilization of WNV-infected ex vivo brain slice cultures (BSC), a novel model of WNV encephalitis, revealed that inhibition of caspase 8 decreased virus-induced activation of caspase 3 an...

“…Increased levels of p53 have been shown to promote cell death by transcriptionally activating proapoptotic genes, including Bax and PUMA. Our prior microarray studies indicated that Bax and PUMA are not upregulated in the brain throughout the course of reovirus infection (21), suggesting that the transcriptional activity of p53 does not contribute to pathology during reovirus encephalitis. The cytoplasmic location of p53 ( Fig.…”

Section: Levels Of P53 Are Increased In the Brain Following Reovirus mentioning

confidence: 99%

Mitochondrial p53 Contributes to Reovirus-Induced Neuronal Apoptosis and Central Nervous System Injury in a Mouse Model of Viral Encephalitis

Zhuang

Berens

et al. 2016

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The tumor suppressor p53 plays a critical part in determining cell fate both as a regulator of the transcription of several proapoptotic genes and through its binding interactions with Bcl-2 family proteins at mitochondria. We now demonstrate that p53 protein levels are increased in infected brains during reovirus encephalitis. This increase occurs in the cytoplasm of reovirus-infected neurons and is associated with the activation of caspase 3. Increased levels of p53 in reovirus-infected brains are not associated with increased expression levels of p53 mRNA, suggesting that p53 regulation occurs at the protein level. Increased levels of p53 are also not associated with the increased expression levels of p53-regulated, proapoptotic genes. In contrast, upregulated p53 accumulates in mitochondria. Previous reports demonstrated that the binding of p53 to Bak at mitochondria causes Bak activation and results in apoptosis. We now show that Bak is activated and that activated Bak is bound to p53 during reovirus encephalitis. In addition, survival is enhanced in reovirus-infected Bak ؊/؊ mice compared to controls, demonstrating a role for Bak in reovirus pathogenesis. Inhibition of the mitochondrial translocation of p53 with pifithrin prevents the formation of p53/Bak complexes following reovirus infection of ex vivo brain slice cultures and results in decreased apoptosis and tissue injury. These results suggest that the mitochondrial localization of p53 regulates reovirus-induced pathogenesis in the central nervous system (CNS) through its interactions with Bak. IMPORTANCEThere are virtually no specific treatments of proven efficacy for virus-induced neuroinvasive diseases. A better understanding of the pathogenesis of virus-induced CNS injury is crucial for the rational development of novel therapies. Our studies demonstrate that p53 is activated in the brain following reovirus infection and may provide a therapeutic target for virus-induced CNS disease. V iral encephalitis causes morbidity and mortality throughout the world (1, 2). New therapies, including those targeting specific mechanisms of virus-induced central nervous system (CNS) injury, are urgently needed. Intracerebral injection of neonatal mice with type 3 (T3) strains of reovirus is a well-characterized experimental model for studying viral pathogenesis within the CNS. Reovirus specifically targets neurons within the hippocampus, thalamus, and cortex, causing lethal encephalitis. We and others have previously shown that apoptosis of infected neurons is an important pathogenic mechanism during reovirus encephalitis and that reovirus-induced neuronal apoptosis involves the activation of both extrinsically (death receptor) and intrinsically (mitochondrial) mediated pathways, leading to the activation of cellular caspases (3-7).The tumor suppressor p53 plays a critical role in cell death signaling following a variety of insults (8, 9), including infection of BHK-21 cells with avian reovirus (10) and during reovirus oncolysis (11). Increased levels of...