Abstract

Abstract Acute inflammation in response to both exogenous and endogenous danger signals can lead to the assembly of cytoplasmic inflammasomes that stimulate the activation of caspase-1. Subsequently, caspase-1 facilitates the maturation and release of cytokines and also, under some circumstances, the induction of cell death by pyroptosis. Using a mouse line lacking expression of NLRP1, we show that assembly of this inflammasome in cells is triggered by a toxin from anthrax and that it initiates caspase-1 activation and release of IL-1β. Furthermore, NLRP1 inflammasome activation also leads to cell death, which escalates over 3 d following exposure to the toxin and culminates in acute lung injury and death of the mice. We show that these events are not dependent on production of IL-1β by the inflammasome but are dependent on caspase-1 expression. In contrast, muramyl dipeptide-mediated inflammasome formation is not dependent on NLRP1 but NLRP3. Taken together, our findings show that assembly of the NLRP1 inflammasome is sufficient to initiate pyroptosis, which subsequently leads to a self-amplifying cascade of cell injury within the lung from which the lung cannot recover, eventually resulting in catastrophic consequences for the organism.

Keywords

PyroptosisInflammasomeNLRP1Caspase 1Programmed cell deathMuramyl dipeptideInflammationCell biologyCaspaseApoptosisBiologyImmunologyChemistryImmune systemBiochemistry

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Year
2012
Type
article
Volume
189
Issue
4
Pages
2006-2016
Citations
269
Access
Closed

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Martina Kovářová, Pamela R. Hesker, Leigh A. Jania et al. (2012). NLRP1-Dependent Pyroptosis Leads to Acute Lung Injury and Morbidity in Mice. The Journal of Immunology , 189 (4) , 2006-2016. https://doi.org/10.4049/jimmunol.1201065

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DOI
10.4049/jimmunol.1201065