ASC oligomer favors caspase-1CARD domain recruitment after intracellular potassium efflux

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Martín-Sánchez, Fátima | Compan, Vincent | Peñín-Franch, Alejandro | Tapia-Abellán, Ana | Gómez, Ana, I | Baños-Gregori, María, C | Schmidt, Florian, I | Pelegrin, Pablo

Edité par CCSD ; Rockefeller University Press -

International audience. Signaling through the inflammasome is important for the inflammatory response. Low concentrations of intracellular K + are associated with the specific oligomerization and activation of the NLRP3 inflammasome, a type of inflammasome involved in sterile inflammation. After NLRP3 oligomerization, ASC protein binds and forms oligomeric filaments that culminate in large protein complexes named ASC specks. ASC specks are also initiated from different inflammasome scaffolds, such as AIM2, NLRC4, or Pyrin. ASC oligomers recruit caspase-1 and then induce its activation through interactions between their respective caspase activation and recruitment domains (CARD). So far, ASC oligomerization and caspase-1 activation are K +-independent processes. Here, we found that when there is low intracellular K + , ASC oligomers change their structure independently of NLRP3 and make the ASC CARD domain more accessible for the recruitment of the pro-caspase-1 CARD domain. Therefore, conditions that decrease intracellular K + not only drive NLRP3 responses but also enhance the recruitment of the procaspase-1 CARD domain into the ASC specks. .

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