The PYRIN Domain-only Protein POP1 Inhibits Inflammasome Assembly and Ameliorates Inflammatory Disease

Almeida, Lúcia de; Khare, Shruti; Misharin, Alexander V.; Patel, Rajul A.; Ratsimandresy, Rojo A.; Wallin, Melissa; Perlman, Harris; Greaves, David R.; Hoffman, Hal M.; Dorfleutner, Andrea; Stehlik, Christian

doi:10.1016/j.immuni.2015.07.018

Cited by 106 publications

(190 citation statements)

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“…30 A20-driven ubiquitination of NLRP3, PYRIN domain-only protein POP1-dependent inhibition of inflammasome assembly, or reactive oxygen species-driven suppression of caspase-1 are just three such regulatory mechanisms. [31][32][33] Figure 2. Inflammasome activation in dendritic cells and macrophages involves numerous elements.…”

Section: Il-1bmentioning

confidence: 99%

Of Inflammasomes and Alarmins: IL-1β and IL-1α in Kidney Disease

Anders

2016

JASN

209

152

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Kidney injury implies danger signaling and a response by the immune system. The inflammasome is a central danger recognition platform that triggers local and systemic inflammation. In immune cells, inflammasome activation causes the release of mature IL-1b and of the alarmin IL-1a. Dying cells release IL-1a also, independently of the inflammasome. Both IL-1a and IL-1b ligate the same IL-1 receptor (IL-1R) that is present on nearly all cells inside and outside the kidney, further amplifying cytokine and chemokine release. Thus, the inflammasome-IL-1a/IL-b-IL-1R system is a central element of kidney inflammation and the systemic consequences. Seminal discoveries of recent years have expanded this central paradigm of inflammation. This review gives an overview of arising concepts of inflammasome and IL-1a/b regulation in renal cells and in experimental kidney disease models. There is a pipeline of compounds that can interfere with the inflammasome-IL-1a/IL-b-IL-1R system, ranging from recently described small molecule inhibitors of NLRP3, a component of the inflammasome complex, to regulatory agency-approved IL-1-neutralizing biologic drugs. Based on strong theoretic and experimental rationale, the potential therapeutic benefits of using such compounds to block the inflammasome-IL-1a/IL-b-IL-1R system in kidney disease should be further explored.

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Section: Il-1bmentioning

confidence: 99%

Of Inflammasomes and Alarmins: IL-1β and IL-1α in Kidney Disease

Anders

2016

JASN

209

152

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“…Inhibiting AIM2 inflammasome activity using synthetic inhibitors, such as synthetic Oligodeoxynucleotides (ODN) containing suppressive TTAGGG Motifs (Kaminski et al, 2013) or taking advantage of endogenous AIM2 inhibitors, such as the pyrin-containing proteins, recently described by (Khare et al, 2014;de Almeida et al, 2015), or antimicrobial cathelicidin peptides, reported by Schauber and colleagues , could certainly be explored and studied for their potential to limit undesired inflammation (Man et al, 2016). Still, further research aiming at the discovery of new small-molecules to inhibit AIM2 inflammasome would certainly be of benefit to the development of effective drugs to treat chronic diseases, in which inflammation is the key player.…”

Section: Therapeutic Implications Of Aim2 Inflammasomementioning

confidence: 99%

The Duality of AIM2 Inflammasome: A Focus on its Role in Autoimmunity and Skin Diseases

Canavese¹

2016

American Journal of Pharmacology and Toxicology

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Understanding the inflammasome biology is one of the most exciting challenges in immuno-pharmacology. The role of the inflammasomes has been recognized in the host defense mechanism against invading pathogens and in the development of several conditions, such as cancer, auto-inflammatory, autoimmune, metabolic and neurodegenerative disorders. DNA recognition by the cells is a crucial immunological step leading to the initiation of an innate immune response. Absent in Melanoma 2 (AIM2) is a cytoplasmic sensor that perceives double-stranded DNA of microbial or host origin. Once the DNA is bound, AIM2 assembles a multiprotein complex named inflammasome, which drives pyroptosis and proteolytic cleavage of pro-IL-1β and pro-IL-18 pro-inflammatory cytokines, leading to a protective inflammasome-mediated host response. However, improper recognition of self-DNA by AIM2 triggers deleterious inflammatory responses, leading to systemic inflammation and several pathological conditions. Therefore, understanding the mechanisms of AIM2-inflammasome-mediated inflammation will provide an essential knowledge base to develop new successful therapeutic strategies to cure the outlined pathologies in which AIM2-inflammasome activation plays a key role, as well as to guide clinical practice. This mini-review provides an overview on the latest research findings on AIM2 inflammasome, with particular focus on its role in autoimmunity and skin disorders. An update on its therapeutic implications has also been documented.

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“…In this issue of Immunity, de Almeida et al (2015) report that the PYRIN domain-only protein (POP1) efficiently inhibits inflammasome activation, identifying it as a pan-inflammasome inhibitor.…”

mentioning

confidence: 99%

“…In the article by de Almeida et al (2015) appearing in this issue of Immunity, the authors have identified PYRIN (PYD) only protein (POP1) as a negative regulator of inflammasome activation. Although the POP family of proteins was identified in humans more than 10 years ago (they are not found in mice) and includes POP1 (also known as ASC2), POP2, POP3, and POP4 (Stehlik et al, 2003), their functions have been unclear.…”

mentioning

confidence: 99%

“…Furthermore, the authors found that POP1 overexpression inhibited ASC particle release, thereby preventing secondary inflammasome activation after engulfment by macrophages. de Almeida et al (2015) generated transgenic mice expressing human POP1 under the macrophagespecific CD68 promoter and showed that NLRP3 inflammasome autoactivation by CAPS mutation was significantly inhibited. More importantly, these mice were protected against LPS-induced peritonitis.…”

mentioning

confidence: 99%

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