<i>Shigella</i>
            IpaH7.8 E3 ubiquitin ligase targets glomulin and activates inflammasomes to demolish macrophages

Suzuki, Shiho; Mimuro, Hitomi; Kim, Minsoo; Ogawa, Michinaga; Ashida, Hiroshi; Toyotome, Takahito; Franchi, Luigi; Suzuki, Masato; Sanada, Takahito; Suzuki, Toshihiko; Tsutsui, Hiroko; Núñez, Gabriel; Sasakawa, Chihiro

doi:10.1073/pnas.1324021111

Cited by 91 publications

(103 citation statements)

References 57 publications

(84 reference statements)

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“…Shigella species target GLMN by translocation of an E3 ligase (invasion plasmid antigen H7.8) into host cells; IpaH7.8 ubiquitinates GLMN, resulting in its degradation at the proteasome and relieving its inhibition of an unidentified Cullin ring ligase. 45 This study provides indirect evidence that activity of a Cullin ring ligase may be important for NLRP3 activation, and proposes that ubiquitination provides a non-degradative, activating stimulus for the NLRP3 inflammasome.…”

Section: Nlrp3: Ubiquitinationmentioning

confidence: 84%

Regulation of inflammasomes by ubiquitination

Bednash

Mallampalli

2016

Cell Mol Immunol

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Section: Nlrp3: Ubiquitinationmentioning

confidence: 84%

Regulation of inflammasomes by ubiquitination

Bednash

Mallampalli

2016

Cell Mol Immunol

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“…[103][104][105] Another NEL effector, IpaH7.8, possesses E3 ligase activity in vitro and targets an inhibitor of Cullin-based RING E3 ligase named GLMN for degradation, which augments inflammasome activation. 106 In addition, OspG and OspI, belonging to a different subsets of S. flexneri effectors, have recently been identified to suppress NF-κB activation by disrupting the ubiquitin system. Mammalian serine/threonine kinase imitator OspG binds to many ubiquitinated E2 proteins, including UbcH5 and Ubch7, in host cells, thereby enhancing its own kinase activity and preventing the ubiquitination and degradation of phosphorylated IκBα.…”

Section: Shigella Flexnerimentioning

confidence: 99%

The ubiquitin system: a critical regulator of innate immunity and pathogen–host interactions

Chai

Liu

2016

Cell Mol Immunol

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The ubiquitin system comprises enzymes that are responsible for ubiquitination and deubiquitination, as well as ubiquitin receptors that are capable of recognizing and deciphering the ubiquitin code, which act in coordination to regulate almost all host cellular processes, including host-pathogen interactions. In response to pathogen infection, the host innate immune system launches an array of distinct antimicrobial activities encompassing inflammatory signaling, phagosomal maturation, autophagy and apoptosis, all of which are fine-tuned by the ubiquitin system to eradicate the invading pathogens and to reduce concomitant host damage. By contrast, pathogens have evolved a cohort of exquisite strategies to evade host innate immunity by usurping the ubiquitin system for their own benefits. Here, we present recent advances regarding the ubiquitin system-mediated modulation of host-pathogen interplay, with a specific focus on host innate immune defenses and bacterial pathogen immune evasion.

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“…The mechanism by which IpaH7.8 induced macrophage cell death is via IpaH7.8 E3 ligasemediated proteasome-dependent GLMN degradation in a cell model of BMDMs and peritoneal macrophages isolated from BALB/c mice. GLMN is polyubiquitinated in the presence of IpaH7.8 [139]. In this context, Wang et al, showed that the production and secretion of IpaH4.5 by Shigella interacts with p65 inhibiting the transcriptional activity of NF-κB through the NTR domain of IpaH4.5 and the p65 region spanning from amino acids 1-190.…”

Section: • • Inflammation Induced By Eiecmentioning

confidence: 99%

Role of Virulence Factors on Host Inflammatory Response Induced by Diarrheagenic Escherichia Coli pathotypes

Sanchez-Villamil

Navarro-Garcı́a

2015

Future Microbiol.

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Pathogens are able to breach the intestinal barrier, and different bacterial species can display different abilities to colonize hosts and induce inflammation. Inflammatory response studies induced by enteropathogens as Escherichia coli are interesting since it has acquired diverse genetic mobile elements, leading to different E. coli pathotypes. Diarrheagenic E. coli secrete toxins, effectors and virulence factors that exploit the host cell functions to facilitate the bacterial colonization. Many bacterial proteins are delivered to the host cell for subverting the inflammatory response. Hereby, we have highlighted the specific processes used by E. coli pathotypes, by that subvert the inflammatory pathways. These mechanisms include an arrangement of pro- and anti-inflammatory responses to favor the appropriate environmental niche for the bacterial survival and growth.

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Shigella IpaH7.8 E3 ubiquitin ligase targets glomulin and activates inflammasomes to demolish macrophages

Cited by 91 publications

References 57 publications

Regulation of inflammasomes by ubiquitination

Regulation of inflammasomes by ubiquitination

The ubiquitin system: a critical regulator of innate immunity and pathogen–host interactions

Role of Virulence Factors on Host Inflammatory Response Induced by Diarrheagenic Escherichia Coli pathotypes

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