Protein kinase R
Protein kinase RNA-activated also known as protein kinase R (PKR), interferon-induced, double-stranded RNA-activated protein kinase, or eukaryotic translation initiation factor 2-alpha kinase 2 (EIF2AK2) is an enzyme that in humans is encoded by the EIF2AK2 gene on chromosome 2.[5][6] PKR is a serine/tyrosine kinase that is 551 amino acids long.[7]
PKR is inducible by various mechanisms of stress and protects against viral infections.[8] It also has a role in several signaling pathways.[9][10]
Mechanism of action
[edit]Protein kinase-R is activated by double-stranded RNA (dsRNA), introduced to the cells by a viral infection.[9] In situations of viral infection, the dsRNA created by viral replication and gene expression binds to the N-terminal domain, activating the protein.[9] PKR activation via dsRNA is length dependent, requiring the dsRNA to be 30 bp in length to bind to PKR molecules.[9] However, excess dsRNA can diminish activation of PKR.[9] Binding to dsRNA is believed to activate PKR by inducing dimerization of the kinase domains and subsequent auto-phosphorylation reactions.[9] It is not yet established whether PKR activates in cis, with a protomer's activation loop reaching into its own catalytic site, or in trans, with the activation loop being phosphorylated in a face to face geometry by a conjugate protomer.[11] PKR can also be activated by the protein PACT via phosphorylation of S287 on its M3 domain.[12] The promoter region of PKR has interferon-stimulated response elements to which Type I interferons (IFN) bind to induce the transcription of PKR genes.[12][13] Some research suggests that PKR can be stimulated by heat shock proteins, heparin, growth factors, bacterial infection, pro-inflammatory cytokines, reactive oxygen species, DNA damage, mechanical stress, and excess nutrient intake.[12]
Once active, PKR is able to phosphorylate the eukaryotic translation initiation factor eIF2α.[12] This inhibits further cellular mRNA translation, thereby preventing viral protein synthesis.[10] Overall, this leads to apoptosis of virally infected cells to prevent further viral spread. PKR can also induce apoptosis in bacterial infection by responding to LPS and proinflammatory cytokines.[10] Apoptosis can also occur via PKR activation of the FADD and caspase signaling pathway.[13]
PKR also has pro-inflammatory functions, as it can mediate the activation of the transcription factor NF-kB, by phosphorylating its inhibitory subunit, IkB.[13] This leads to the expression of adhesion molecules and transcription factors that activate them, which induce inflammation responses such as the secretion of pro-inflammatory cytokines.[12] PKR also activates several mitogen-activated protein kinases (MAPK) to lead to inflammation.[13]
To balance the effects of apoptosis and inflammation, PKR has regulatory functions. Active PKR is also able to activate tumor suppressor PP2A which regulates the cell cycle and the metabolism.[14] There is also evidence that PKR is autophagic as a regulatory mechanism.[13]
PKR stress pathway
[edit]PKR is in the center of cellular response to different stress signals such as pathogens, lack of nutrients, cytokines, irradiation, mechanical stress, or ER stress.[12] The PKR pathway leads to a stress response through activation of other stress pathways such as JNK, p38, NFkB, PP2A and phosphorylation of eIF2α.[10] ER stress caused by excess of unfolded proteins leads to inflammatory responses.[15] PKR contributes to this response by interacting with several inflammatory kinases such as IKK, JNK, ElF2α, insulin receptors and others.[15] This metabolically activated inflammatory complex is called metabolic inflammasome or metaflammasome.[16][17] Via the JNK signaling pathway, PKR also plays a role in insulin resistance, diabetes, and obesity by phosphorylating IRS1.[18] Inhibiting PKR in mice led to lower inflammation in adipose tissues, increased sensitivity to insulin, and amelioration of diabetic symptoms.[18] PKR also participates in the mitochondrial unfolded protein response (UPRmt).[19] Here, PKR is induced via the transcription factor AP-1 and activated independently of PACT.[19] In this context, PKR has been shown to be relevant to intestinal inflammation.[19]
Viral defense
[edit]Viruses have developed many mechanisms to counteract the PKR mechanism. It may be done by Decoy dsRNA, degradation, hiding of viral dsRNA, dimerization block, dephosphorylation of substrate or by a pseudosubstrate. Some mechanisms are still unknown, for instance, in Lymphocytic choriomeningitis virus infection the virus is not recognized by PKR,[20] and the current anti-dsRNA antibodies have limitation in detecting dsRNA species of negative stranded RNA viruses,[21] which necessitates the use of a different approach to understand this viral defense mechanism.
For instance, Epstein–Barr virus (EBV) uses the gene EBER1 to produce decoy dsRNA. This leads to cancers such as Burkitt's lymphoma, Hodgkin's disease, nasopharyngeal carcinoma and various leukemias.
Defense type | Virus | Molecule |
---|---|---|
Decoy dsRNA | Adenovirus | VAI RNA |
Epstein–Barr virus | EBER | |
HIV | TAR | |
PKR degradation | Poliovirus | 2Apro |
Hide viral dsRNA | Vaccinia virus | E3L |
Reovirus | σ3 | |
Influenza virus | NS1 | |
Dimerization block | Influenza virus | p58IPK |
Hepatitis C virus | NS5A | |
Pseudosubstrate | Vaccinia virus | K3L |
HIV | Tat | |
Dephosphorylation of substrate | Herpes simplex virus | ICP34.5 |
Unknown mechanism | Lymphocytic choriomeningitis virus | NP[22] |
Memory and learning
[edit]PKR knockout mice or inhibition of PKR in mice enhances memory and learning.[23]
Neuronal degeneration disease
[edit]First report in 2002 has been shown that immunohistochemical marker for phosphorylated PKR and eIF2α was displayed positively in degenerating neurons in the hippocampus and the frontal cortex of patients with Alzheimer's disease (AD), suggesting the link between PKR and AD. Additionally, many of these neurons were also immunostained with an antibody for phosphorylated Tau protein.[24] Activated PKR was specifically found in the cytoplasm and nucleus, as well as co-localized with neuronal apoptotic markers.[25] Further studies have assessed the levels of PKR in blood and cerebrospinal fluid (CSF) of AD patients and controls. The result of an analysis of the concentrations of total and phosphorylated PKR (pPKR) in peripheral blood mononuclear cells (PBMCs) in 23 AD patients and 19 control individuals showed statistically significant increased levels of the ratio of phosphorylated PKR/PKR in AD patients compared with controls.[26] Assessments of CSF biomarkers, such as Aβ1-42, Aβ1-40, Tau, and phosphorylated Tau at threonine 181, have been a validated use in clinical research and in routine practice to determine whether patients have CSF abnormalities and AD brain lesions. A study found that "total PKR and pPKR concentrations were elevated in AD and amnestic mild cognitive impairment subjects with a pPKR value (optical density units) discriminating AD patients from control subjects with a sensitivity of 91.1% and a specificity of 94.3%. Among AD patients, total PKR and pPKR levels correlate with CSF p181tau levels. Some AD patients with normal CSF Aß, T-tau, or p181tau levels had abnormal total PKR and pPKR levels".[27] It was concluded that the PKR-eIF2α pro-apoptotic pathway could be involved in neuronal degeneration that leads to various neuropathological lesions as a function of neuronal susceptibility.
PKR and beta amyloid
Activation of PKR can cause accumulation of amyloid β-peptide (Aβ) via de-repression of BACE1 (β-site APP Cleaving Enzyme) expression in Alzheimer Disease patients.[28] Normally, the 5′ untranslated region (5′ UTR) in the BACE1 promoter would fundamentally inhibit the expression of BACE1 gene. However, BACE1 expression can be activated by phosphorylation of eIF2a, which reverses the inhibitory effect exerted by BACE1 5′ UTR. Phosphorylation of eIF2a is triggered by activation of PKR. Viral infection such as herpes simplex virus (HSV) or oxidative stress can both increase BACE1 expression through activation of PKR-eIF2a pathway.[29]
In addition, the increased activity of BACE1 could also lead to β-cleaved carboxy-terminal fragment of β-Amyloid precursor protein (APP-βCTF) induced dysfunction of endosomes in AD.[30] Endosomes are highly active β-Amyloid precursor protein (APP) processing sites, and endosome abnormalities are associated with upregulated expression of early endosomal regulator, Rab5. These are the earliest known disease-specific neuronal response in AD. Increased activity of BACE1 leads to synthesis of the APP-βCTF. An elevated level of βCTF then causes Rab5 overactivation. βCTF recruits APPL1 to rab5 endosomes, where it stabilizes active GTP-Rab5, leading to pathologically accelerated endocytosis, endosome swelling and selectively impaired axonal transport of Rab5 endosomes.
PKR and Tau phosphorylation
It is reported earlier that phosphorylated PKR could co-localize with phosphorylated Tau protein in affected neurons.[31][24] A protein phosphatase-2A inhibitor (PP2A inhibitor) – okadaic acid (OA) – is known to increase tau phosphorylation, Aβ deposition and neuronal death. It is studied that OA also induces PKR phosphorylation and thus, eIF2a phosphorylation. eIF2a phosphorylation then induces activation of transcription factor 4 (ATF4), which induces apoptosis and nuclear translocation, contributing to neuronal death.[32]
Glycogen synthase kinase 3β (GSK-3β) is responsible for tau phosphorylation and controls several cellular functions including apoptosis. Another study demonstrated that tunicamycin or Aβ treatment can induce PKR activation in human neuroblastoma cells and can trigger GSK3β activation, as well as tau phosphorylation. They found that in AD brains, both activated PKR and GSK3β co-localize with phosphorylated tau in neurons. In SH-SY5Y cell cultures, tunicamycin and Aβ(1-42) activate PKR, which then can modulate GSK-3β activation and induce tau phosphorylation, apoptosis. All these processes are attenuated by PKR inhibitors or PKR siRNA. PKR could represent a crucial signaling point relaying stress signals to neuronal pathways by interacting with transcription factor or indirectly controlling GSK3β activation, leading to cellular degeneration in AD.[33]
Fetal alcohol syndrome
[edit]PKR also mediates ethanol-induced protein synthesis inhibition and apoptosis which is linked to fetal alcohol syndrome.[34]
Interactions
[edit]Protein kinase R has been shown to interact with:
- ASK1,[35]
- DNAJC3,[36]
- ILF3,[37][38][39][40]
- METAP2,[41]
- P53,[42]
- PPP1CA,[43]
- PRKRA,[44][45]
- STAT1,[46][47] and
- TARBP2.[48][49]
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Further reading
[edit]- Williams BR (November 1999). "PKR; a sentinel kinase for cellular stress". Oncogene. 18 (45): 6112–6120. doi:10.1038/sj.onc.1203127. PMID 10557102.
- García MA, Meurs EF, Esteban M (2007). "The dsRNA protein kinase PKR: virus and cell control". Biochimie. 89 (6–7): 799–811. doi:10.1016/j.biochi.2007.03.001. PMID 17451862.
- Thomis DC, Doohan JP, Samuel CE (May 1992). "Mechanism of interferon action: cDNA structure, expression, and regulation of the interferon-induced, RNA-dependent P1/eIF-2 alpha protein kinase from human cells". Virology. 188 (1): 33–46. doi:10.1016/0042-6822(92)90732-5. PMID 1373553.
- McCormack SJ, Thomis DC, Samuel CE (May 1992). "Mechanism of interferon action: identification of a RNA binding domain within the N-terminal region of the human RNA-dependent P1/eIF-2 alpha protein kinase". Virology. 188 (1): 47–56. doi:10.1016/0042-6822(92)90733-6. PMID 1373554.
- Mellor H, Proud CG (July 1991). "A synthetic peptide substrate for initiation factor-2 kinases". Biochemical and Biophysical Research Communications. 178 (2): 430–437. doi:10.1016/0006-291X(91)90125-Q. PMID 1677563.
- Meurs E, Chong K, Galabru J, Thomas NS, Kerr IM, Williams BR, Hovanessian AG (July 1990). "Molecular cloning and characterization of the human double-stranded RNA-activated protein kinase induced by interferon". Cell. 62 (2): 379–390. doi:10.1016/0092-8674(90)90374-N. PMID 1695551. S2CID 20477995.
- Silverman RH, Sengupta DN (1991). "Translational regulation by HIV leader RNA, TAT, and interferon-inducible enzymes". Journal of Experimental Pathology. 5 (2): 69–77. PMID 1708818.
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