Regulation of RIG-I Activation by K63-Linked Polyubiquitination

Okamoto, Masaaki; Kouwaki, Takahisa; Fukushima, Yoshio; Oshiumi, Hiroyuki

doi:10.3389/fimmu.2017.01942

Cited by 78 publications

(78 citation statements)

References 50 publications

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“…Several E3 ligases other than TRIM25 promote ubiquitination of RIG-I leading to controversial discussions about their relative importance (64)(65)(66)(67)(68)(69). Among these are several TRIM proteins (TRIM4, 15,40) and Riplet, a close relative of TRIM25, that lost the B-Box domains and parts of the CC (70)(71)(72).…”

Section: Discussionmentioning

confidence: 99%

Mechanistic insights into RNA binding and RNA-regulated RIG-I ubiquitination by TRIM25

Haubrich

Augsten²,

Álvarez³

et al. 2020

Preprint

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TRIM25 is a ubiquitin E3 ligase active in innate immunity and cell fate decisions. Mounting evidence suggests that TRIM25’s E3 ligase activity is regulated by RNAs. However, while mutations affecting RNA-binding have been described, the precise RNA binding site has not been identified nor which domains are involved. Here, we present biophysical evidence for the presence of RNA binding sites on both TRIM25 PRY/SPRY and coiled-coil domains, and map the binding site on the PRY/SPRY with residue resolution. Cooperative RNA-binding of both domains enhances their otherwise transient interaction in solution and increases the E3 ligase activity of TRIM25. Mutational analysis shows that RNA binding affects ubiquitination of RIG-I in mammalian cells. In addition, we present a simple model system for RNA-induced liquid-liquid phase separation of TRIM25 in vitro, resembling previously observed cellular RNA granules, that facilitates the recruitment of RIG-I.

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Section: Discussionmentioning

confidence: 99%

Mechanistic insights into RNA binding and RNA-regulated RIG-I ubiquitination by TRIM25

Haubrich

Augsten²,

Álvarez³

et al. 2020

Preprint

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“…About a decade ago, influenza virus NS1 was shown to bind E3 ligase TRIM25, thereby interfering with K63-linked ubiquitination of RIG-I, and therefore uniquely inhibiting innate immune signaling in the type-I IFN pathway [127]. There has been a recent debate as to whether these chains are actually conjugated to RIG-I or other factors within the cascade or whether they are free ubiquitin chains that provide a scaffold for activating the aggregation of RIG-I and MAVS, which in turn enables downstream signaling [128]. Influenza B virus-encoded NS1 additionally inhibits ISG15 antiviral activity by binding the N-terminus of human ISG15 (and not mouse ISG15) [129].…”

Section: Manipulation Of Ubiquitin and Isg15 Regulated Innate Immune mentioning

confidence: 99%

Innate Immune Evasion by Human Respiratory RNA Viruses

2019

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The impact of respiratory virus infections on the health of children and adults can be very significant. Yet, in contrast to most other childhood infections as well as other viral and bacterial diseases, prophylactic vaccines or effective antiviral treatments against viral respiratory infections are either still not available, or provide only limited protection. Given the widespread prevalence, a general lack of natural sterilizing immunity, and/or high morbidity and lethality rates of diseases caused by influenza, respiratory syncytial virus, coronaviruses, and rhinoviruses, this difficult situation is a genuine societal challenge. A thorough understanding of the virushost interactions during these respiratory infections will most probably be pivotal to ultimately meet these challenges. This review attempts to provide a comparative overview of the knowledge about an important part of the interaction between respiratory viruses and their host: the arms race between host innate immunity and viral innate immune eva-

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“…To date, most studies have implicated TRIM25 as a critical mediator of innate immune signalling through ubiquitination of RIG-I [2,11,[101][102][103][104][105][106][107][108][109][110][111][112][113][114][115][116][117][118], while only a handful of studies have proposed RIG-I-independent mechanisms [46,119]. Recent years have brought both exciting discoveries and rousing controversies regarding how ubiquitin and E3 ligases precisely function to activate RIG-I for antiviral signalling, with some groups suggesting a single factor operates as the critical component while others have put forth a cooperative model based on trends gleaned from numerous studies.…”

Section: Innate Antiviral Signalling Functions Of Trim25: Rig-i-depenmentioning

confidence: 99%

“…Recent years have brought both exciting discoveries and rousing controversies regarding how ubiquitin and E3 ligases precisely function to activate RIG-I for antiviral signalling, with some groups suggesting a single factor operates as the critical component while others have put forth a cooperative model based on trends gleaned from numerous studies. For viruses that are sensed by the RIG-I PRR, initial recognition of vRNA and binding of the viral 5′ tri-and diphosphate PAMPs occurs via the RIG-I helicase and C-terminal domains (CTDs) [108,120,121]. Identification of vRNA triggers a conformational change in RIG-I, freeing up the N-terminal 2CARD domain which would otherwise be suppressed by the CTD and a linker region between the helicase and CTD.…”

Section: Innate Antiviral Signalling Functions Of Trim25: Rig-i-depenmentioning

confidence: 99%

“…The K63-linked ubiquitination of RIG-I by TRIM25 is well established, but additional E3 ubiquitin ligases such as Riplet, MEX3C and TRIM4 have been identified as playing critical roles in fully activating the RIG-I pathway (Fig. 5) [101,108]. Therefore, the fact that TRIM25 may be involved in different aspects of antiviral signalling does not exclude the possibility that TRIM25 and Riplet have redundant functions in the activation of RIG-I, and that one factor may be dominant over the other.…”

Section: Innate Antiviral Signalling Functions Of Trim25: Rig-i-depenmentioning

confidence: 99%

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To TRIM or not to TRIM: the balance of host–virus interactions mediated by the ubiquitin system

Hage

Rajsbaum

2019

Journal of General Virology

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The innate immune system responds rapidly to protect against viral infections, but an overactive response can cause harmful damage. To avoid this, the response is tightly regulated by post-translational modifications (PTMs). The ubiquitin system represents a powerful PTM machinery that allows for the reversible linkage of ubiquitin to activate and deactivate a target's function. A precise enzymatic cascade of ubiquitin-activating, conjugating and ligating enzymes facilitates ubiquitination. Viruses have evolved to take advantage of the ubiquitin pathway either by targeting factors to dampen the antiviral response or by hijacking the system to enhance their replication. The tripartite motif (TRIM) family of E3 ubiquitin ligases has garnered attention as a major contributor to innate immunity. Many TRIM family members limit viruses either indirectly as components in innate immune signalling, or directly by targeting viral proteins for degradation. In spite of this, TRIMs and other ubiquitin ligases can be appropriated by viruses and repurposed as valuable tools in viral replication. This duality of function suggests a new frontier of research for TRIMs and raises new challenges for discerning the subtleties of these pro-viral mechanisms. Here, we review current findings regarding the involvement of TRIMs in host-virus interactions. We examine ongoing developments in the field, including novel roles for unanchored ubiquitin in innate immunity, the direct involvement of ubiquitin ligases in promoting viral replication, recent controversies on the role of ubiquitin and TRIM25 in activation of the pattern recognition receptor RIG-I, and we discuss the implications these studies have on future research directions.

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Regulation of RIG-I Activation by K63-Linked Polyubiquitination

Cited by 78 publications

References 50 publications

Mechanistic insights into RNA binding and RNA-regulated RIG-I ubiquitination by TRIM25

Mechanistic insights into RNA binding and RNA-regulated RIG-I ubiquitination by TRIM25

Innate Immune Evasion by Human Respiratory RNA Viruses

To TRIM or not to TRIM: the balance of host–virus interactions mediated by the ubiquitin system

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