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Platelet ITGA2B inhibits caspase-8 and Rip3/Mlkl-dependent platelet death though PTPN6 during sepsis

Jiang Jiang, Wei Li, Lu Zhou, Dengping Liu, Yuanyuan Wang, Jianzhong An, Shigang Qiao, Zhanli Xie

2023iScience13 citationsDOIOpen Access PDF

Abstract

Platelets play an important role in the pathogenesis of sepsis and platelet transfusion is a therapeutic option for sepsis patients, although the exact mechanisms have not been elucidated so far. ITGA2B encodes the αIIb protein in platelets, and its upregulation in sepsis is associated with increased mortality rate. Here, we generated a Itga2b (Q887X) knockin mouse, which significantly reduced ITGA2B expression of platelet and megakaryocyte. The decrease of ITGA2B level aggravated the death of septic mice. We analyzed the transcriptomic profiles of the platelets using RNA sequencing. Our findings suggest that ITGA2B upregulates PTPN6 in megakaryocytes via the transcription factors Nfkb1 and Rel. Furthermore, PTPN6 inhibits platelet apoptosis and necroptosis during sepsis by targeting the Ripk1/Ripk3/Mlkl and caspase-8 pathways. This prevents Kupffer cells from rapidly clearing activated platelets, and eventually maintains vascular integrity during sepsis. Our findings indicate a new function of ITGA2B in the regulation of platelet death during sepsis.

Topics & Concepts

SepsisPlateletNecroptosisMegakaryocyteDownregulation and upregulationImmunologyPlatelet activationRIPK1Septic shockCell biologyBiologyApoptosisProgrammed cell deathGeneGeneticsStem cellHaematopoiesisNeutrophil, Myeloperoxidase and Oxidative MechanismsImmune Response and InflammationSepsis Diagnosis and Treatment
Platelet ITGA2B inhibits caspase-8 and Rip3/Mlkl-dependent platelet death though PTPN6 during sepsis | Litcius