Literature DB >> 30459235

The inflammasome adapter ASC assembles into filaments with integral participation of its two Death Domains, PYD and CARD.

Reinard Jeffrey T Nambayan1, Suzanne I Sandin1,2, David A Quint3,4, David M Satyadi1, Eva de Alba5.   

Abstract

The inflammasome is a multiprotein complex necessary for the onset of inflammation. The adapter protein ASC assembles inflammasome components by acting as a molecular glue between danger-signal sensors and procaspase-1. The assembly is mediated by ASC self-association and protein interactions via its two Death Domains, PYD and CARD. Truncated versions of ASC have been shown to form filaments, but information on the filaments formed by full-length ASC is needed to construct a meaningful model of inflammasome assembly. To gain insights into this system, we used a combination of transmission EM, NMR, and computational analysis to investigate intact ASC structures. We show that ASC forms ∼6-7-nm-wide filaments that stack laterally to form bundles. The structural characteristics and dimensions of the bundles indicate that both PYD and CARD are integral parts of the filament. A truncated version of ASC with only the CARD domain (ASCCARD) forms different filaments (∼3-4-nm width), providing further evidence that both domains work in concert in filament assembly. Ring-shaped protein particles bound to pre-existing filaments match the size of ASC dimer structures generated by NMR-based protein docking, suggesting that the ASC dimer could be a basic building block for filament formation. Solution NMR binding studies identified the protein surfaces involved in the ASCCARD-ASCCARD interaction. These data provide new insights into the structural underpinnings of the inflammasome and should inform future efforts to interrogate this important biological system.
© 2019 Nambayan et al.

Entities:  

Keywords:  ASC; CARD; Death Domain; NMR; PYD; apoptosis; inflammasome; inflammation; protein assembly; transmission electron microscopy

Mesh:

Substances:

Year:  2018        PMID: 30459235      PMCID: PMC6333874          DOI: 10.1074/jbc.RA118.004407

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


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