Insulin receptor substrate-4 interacts with ubiquitin-specific protease 18 to activate the Jak/STAT signaling pathway

Jiao, Baihai; Shi, Xuezhen; Chen, Yanzhao; Yé, Haiyan; Yao, Ming; Hong, Wenxu; Li, Shilin; Duan, Xiaoqiong; Li, Yujia; Wang, Yancui

doi:10.18632/oncotarget.22510

Cited by 12 publications

(8 citation statements)

References 42 publications

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“…3 and Supplementary Table S4 ). Among the genes included in these GO terms, we found irs4, which inhibits JAK/Stat signaling pathway, modulating the immune response 32 ; PDE5A (phosphodiesterase 5A), whose pharmacological inhibition have been associated with anti-inflammatory and neuroprotective effects 33 ; and shh (sonic hedgehog), which has been implicated in macrophage polarization after SCI, regulating pro- and anti-inflammatory response 34 . This analysis suggests that there is an active mechanism to control and limit the immune response.…”

Section: Resultsmentioning

confidence: 99%

Analysis of the early response to spinal cord injury identified a key role for mTORC1 signaling in the activation of neural stem progenitor cells

et al. 2021

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Xenopus laevis are able to regenerate the spinal cord during larvae stages through the activation of neural stem progenitor cells (NSPCs). Here we use high-resolution expression profiling to characterize the early transcriptome changes induced after spinal cord injury, aiming to identify the signals that trigger NSPC proliferation. The analysis delineates a pathway that starts with a rapid and transitory activation of immediate early genes, followed by migration processes and immune response genes, the pervasive increase of NSPC-specific ribosome biogenesis factors, and genes involved in stem cell proliferation. Western blot and immunofluorescence analysis showed that mTORC1 is rapidly and transiently activated after SCI, and its pharmacological inhibition impairs spinal cord regeneration and proliferation of NSPC through the downregulation of genes involved in the G1/S transition of cell cycle, with a strong effect on PCNA. We propose that the mTOR signaling pathway is a key player in the activation of NPSCs during the early steps of spinal cord regeneration.

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Section: Resultsmentioning

confidence: 99%

Analysis of the early response to spinal cord injury identified a key role for mTORC1 signaling in the activation of neural stem progenitor cells

et al. 2021

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“…Of note, the IFN-I regulatory functions of USP18 depend on its capacity to bind IFNAR2 and inhibit JAK/STAT signaling and involves other factors. Through direct interaction with USP18, the insulin receptor substrate-4 was shown to counteract its inhibitory effect on JAK/STAT signaling [51]. Conversely, STAT2 was shown to be a crucial component of the USP18-mediated suppression of IFN-I signaling [52].…”

Section: Discussionmentioning

confidence: 99%

USP18 is a significant driver of memory CD4 T-cell reduced viability caused by type I IFN signaling during primary HIV-1 infection

et al. 2019

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The loss of Memory CD4 T-cells (Mem) is a major hallmark of HIV-1 immuno-pathogenesis and occurs early during the first months of primary infection. A lot of effort has been put into understanding the molecular mechanisms behind this loss, yet they still have not been fully identified. In this study, we unveil the unreported role of USP18 in the deleterious effects of sustained type I IFN signaling on Mem, including HIV-1-specific CD4 T-cells. We find that interfering with IFN-I signaling pathway in infected patients, notably by targeting the interferon-stimulated gene USP18, resulted in reduced PTEN expression similar to those observed in uninfected control donors. We show that AKT activation in response to cytokine treatment, T-cell receptor (TcR) triggering, as well as HIV-1 Gag stimulation was significantly improved in infected patients when PTEN or USP18 were inhibited. Finally, our data demonstrate that higher USP18 in Mem from infected patients prevent proper cell survival and long-lasting maintenance in an AKT-dependent manner. Altogether, we establish a direct role for type I IFN/USP18 signaling in the maintenance of total and virus-specific Mem and provide a new mechanism for the reduced survival of these populations during primary HIV-1 infection.

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“…When ligands bind to their receptors, the intracellular portion of JAKs will be activated, which recruits and phosphorylates STATs. Activated STATs translocate into the nucleus and bind to the promoters of related genes, inducing the expression of specific genes (120)(121)(122)(123). These cytokines are highly important in initiating and orchestrating innate and adaptive immune responses but may also be a source of excessive or uncontrolled inflammation and tissue damage in patients with COVID-19.…”

Section: Janus Kinase Inhibitorsmentioning

confidence: 99%

The development of COVID-19 treatment

et al. 2023

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The emergence of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) caused a pandemic named coronavirus disease 2019 (COVID-19) that has become the greatest worldwide public health threat of this century. Recent studies have unraveled numerous mysteries of SARS-CoV-2 pathogenesis and thus largely improved the studies of COVID-19 vaccines and therapeutic strategies. However, important questions remain regarding its therapy. In this review, the recent research advances on COVID-19 mechanism are quickly summarized. We mainly discuss current therapy strategies for COVID-19, with an emphasis on antiviral agents, neutralizing antibody therapies, Janus kinase inhibitors, and steroids. When necessary, specific mechanisms and the history of therapy are present, and representative strategies are described in detail. Finally, we discuss key outstanding questions regarding future directions of the development of COVID-19 treatment.

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Insulin receptor substrate-4 interacts with ubiquitin-specific protease 18 to activate the Jak/STAT signaling pathway

Cited by 12 publications

References 42 publications

Analysis of the early response to spinal cord injury identified a key role for mTORC1 signaling in the activation of neural stem progenitor cells

Analysis of the early response to spinal cord injury identified a key role for mTORC1 signaling in the activation of neural stem progenitor cells

USP18 is a significant driver of memory CD4 T-cell reduced viability caused by type I IFN signaling during primary HIV-1 infection

The development of COVID-19 treatment

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