miR‐193b represses influenza A virus infection by inhibiting Wnt/β‐catenin signalling

Yang, Xiaoyun; Zhao, Chunling; Bamunuarachchi, Gayan; Wang, Yan; Liang, Yurong; Huang, Chaoqun; Zhu, Zhengyu; Xu, Dao; Kong, Lin; Senavirathna, Lakmini; Xu, Lan; Liu, Lin

doi:10.1111/cmi.13001

Cited by 29 publications

(17 citation statements)

References 87 publications

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“…Virulent viruses can suppress β-catenin-dependent transcription by misusing the RIG-I/NF-κB signaling cascade that is induced in the course of infection by viral RNA [ 36 ], and we hypothesize that COVID-19 is similar to other viruses in this regard [ 37 ]. Therefore, activation of Wnt/β-catenin signaling could be a major therapeutic intervention in the context of viral infection [ 38 ] if implemented early in the infectious lifecycle ( Figure 2 ) where the immediate check on viral spread can happen before the adaptive immune response has time to develop several days after infection. More specifically, type I interferons are a critical part of our innate immune defense as they induce an array of proteins that interfere with virus replication in order to restrict and limit viral spread from cell to cell [ 39 ] in that early window before the adaptive immune response can even take effect.…”

Section: Tissue-specific Stem Cells and Covid Pathogenesismentioning

confidence: 99%

Experimental Models to Study COVID-19 Effect in Stem Cells

Chugh

Bhanja

Norris

et al. 2021

Cells

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The new strain of coronavirus (severe acute respiratory syndrome coronavirus type 2 (SARS-CoV-2)) emerged in 2019 and hence is often referred to as coronavirus disease 2019 (COVID-19). This disease causes hypoxic respiratory failure and acute respiratory distress syndrome (ARDS), and is considered as the cause of a global pandemic. Very limited reports in addition to ex vivo model systems are available to understand the mechanism of action of this virus, which can be used for testing of any drug efficacy against virus infectivity. COVID-19 induces tissue stem cell loss, resulting inhibition of epithelial repair followed by inflammatory fibrotic consequences. Development of clinically relevant models is important to examine the impact of the COVID-19 virus in tissue stem cells among different organs. In this review, we discuss ex vivo experimental models available to study the effect of COVID-19 on tissue stem cells.

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Section: Tissue-specific Stem Cells and Covid Pathogenesismentioning

confidence: 99%

Experimental Models to Study COVID-19 Effect in Stem Cells

Chugh

Bhanja

Norris

et al. 2021

Cells

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“…Aberrant expression of miRNAs is involved in the pathogenesis of various diseases including cancer, cardiac hypertrophy, respiratory diseases and others [21][22][23][24]. Depending on the circumstances, miRNAs can either promote or suppress tumour formation by modulating cell proliferation, death, invasion, metastasis and/or angiogenesis [25][26][27]. In immune cells within the TME, miRNAs can stimulate or suppress antitumour immunity by controlling immune regulatory molecules in both tumours and immune cells [28].…”

Section: Introductionmentioning

confidence: 99%

miR-149-3p reverses CD8 ⁺ T-cell exhaustion by reducing inhibitory receptors and promoting cytokine secretion in breast cancer cells

et al. 2019

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Blockade of inhibitory receptors (IRs) is one of the most effective immunotherapeutic approaches to treat cancer. Dysfunction of miRNAs is a major cause of aberrant expression of IRs and contributes to the immune escape of cancer cells. How miRNAs regulate immune checkpoint proteins in breast cancer remains largely unknown. In this study, downregulation of miRNAs was observed in PD-1-overexpressing CD8+ T cells using miRNA array analysis of mouse breast cancer homografts. The data reveal that miR-149-3p was predicted to bind the 3'UTRs of mRNAs encoding T-cell inhibitor receptors PD-1, TIM-3, BTLA and Foxp1. Treatment of CD8+ T cells with an miR-149-3p mimic reduced apoptosis, attenuated changes in mRNA markers of T-cell exhaustion and downregulated mRNAs encoding PD-1, TIM-3, BTLA and Foxp1. On the other hand, T-cell proliferation and secretion of effector cytokines indicative of increased T-cell activation (IL-2, TNF-α, IFN-γ) were upregulated after miR-149-3p mimic treatment. Moreover, the treatment with a miR-149-3p mimic promoted the capacity of CD8+ T cells to kill targeted 4T1 mouse breast tumour cells. Collectively, these data show that miR-149-3p can reverse CD8+ T-cell exhaustion and reveal it to be a potential antitumour immunotherapeutic agent in breast cancer.

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“…Recently, a great attention has been paid to noncoding RNAs (ncRNAs) as they have been extensively reported to play various key roles in the regulation of cellular response and metabolic pathways (Cech & Steitz, 2014;Yang et al, 2019). ncRNAs include various categories of RNAs, among them, long noncoding RNAs (lncRNAs) are the most substantial ncRNAs regulating the immune response to viral infection Li et al, 2015;Maarouf, Rai, Goraya, & Chen, 2018;Ouyang et al, 2014;Ouyang, Hu, & Chen, 2016).…”

Section: Infections Of Humans and Animals By Influenza A Virusmentioning

confidence: 99%

Identification of lncRNA‐155 encoded by MIR155HG as a novel regulator of innate immunity against influenza A virus infection

Maarouf

Chen

et al. 2019

Cellular Microbiology

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Long noncoding RNAs (lncRNAs) are single-stranded RNA molecules longer than 200 nt that regulate many cellular processes. MicroRNA 155 host gene (MIR155HG) encodes the microRNA (miR)-155 that regulates various signalling pathways of innate and adaptive immune responses against viral infections. MIR155HG also encodes a lncRNA that we call lncRNA-155. Here, we observed that expression of lncRNA-155 was markedly upregulated during influenza A virus (IAV) infection both in vitro (several cell lines) and in vivo (mouse model). Interestingly, robust expression of lncRNA-155 was also induced by infections with several other viruses. Disruption of lncRNA-155 expression in A549 cells diminished the antiviral innate immunity against IAV. Furthermore, knockout of lncRNA-155 in mice significantly increased IAV replication and virulence in the animals. In contrast, overexpression of lncRNA-155 in human cells suppressed IAV replication, suggesting that lncRNA-155 is involved in host antiviral innate immunity induced by IAV infection. Moreover, we found that lncRNA-155 had a profound effect on expression of protein tyrosine phosphatase 1B (PTP1B) during the infection with IAV. Inhibition of PTP1B by lncRNA-155 resulted in higher production of interferon-beta (IFN-β) and several critical interferon-stimulated genes (ISGs). Together, these observations reveal that MIR155HG derived lncRNA-155 can be induced by IAV, which modulates host innate immunity during the virus infection via regulation of PTP1B-mediated interferon response. KEYWORDS influenza A virus, innate immunity, lncRNA, miR-155, MIR155HG, PTP1B List of Abbreviations: 293T, HEK293T/human embryonic kidney cells; A549, human lung epithelial cells; bic, B-cell Integration Cluster; CA/04, A/California/04/2009; DMEM, Dulbecco's modified Eagle's medium; dpi, days post infection; EV, empty vector; FBS, fetal bovine serum; HA, haemagglutination assay; h-lncRNA-155, human lncRNA-155; hpi, hours post infection; IFN, interferon; IFN-β, interferon-beta; IRF3, interferon regulatory factor 3; IRF7, interferon regulatory factor 7; ISGs, interferon-stimulated genes; KO, bic/miR-155 −/− knock out mice; LLC, mouse Lewis lung carcinoma cells; lncRNAs, long noncoding RNAs; NIH/3T3, mouse embryonic fibroblasts; MDA5, antimelanoma differentiation-associated gene 5; MDCK, Madin-Darby canine kidney cells; miR, microRNA; MIR155HG, miR-155 host gene; m-lncRNA-155, bic/mouse lncRNA-155; NP, IAV nucleoprotein; nt, nucleotide; NRAV, negative regulator of antiviral response;PFA, plaque formation assay; PR8, A/Puerto Rico/8/1934; pre-miR-155, precursor miRNA; pri-miRNA, primary-miRNA; PRRs, pattern recognition receptors; PTP1B, tyrosine-protein phosphatase nonreceptor type 1; RAW 264.7, mouse Abelson murine leukaemia virus transformed macrophages; SeV, Sendai virus; SHIP1, Src homology 2-containing inositol phosphatase 1;sh-luc, Sh-luciferase; shRNAs, short hairpin RNAs; siRNA, small interfering RNA; SOCS1, suppressor of cytokine signalling 1; SPF, specific pathogen free; STAT1, signal transducer a...

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miR‐193b represses influenza A virus infection by inhibiting Wnt/β‐catenin signalling

Cited by 29 publications

References 87 publications

Experimental Models to Study COVID-19 Effect in Stem Cells

Experimental Models to Study COVID-19 Effect in Stem Cells

miR-149-3p reverses CD8 ⁺ T-cell exhaustion by reducing inhibitory receptors and promoting cytokine secretion in breast cancer cells

Identification of lncRNA‐155 encoded by MIR155HG as a novel regulator of innate immunity against influenza A virus infection

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miR‐193b represses influenza A virus infection by inhibiting Wnt/β‐catenin signalling

Cited by 29 publications

References 87 publications

Experimental Models to Study COVID-19 Effect in Stem Cells

Experimental Models to Study COVID-19 Effect in Stem Cells

miR-149-3p reverses CD8 + T-cell exhaustion by reducing inhibitory receptors and promoting cytokine secretion in breast cancer cells

Identification of lncRNA‐155 encoded by MIR155HG as a novel regulator of innate immunity against influenza A virus infection

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miR-149-3p reverses CD8 ⁺ T-cell exhaustion by reducing inhibitory receptors and promoting cytokine secretion in breast cancer cells