TNF-α impairs platelet function by inhibiting autophagy and disrupting metabolism via syntaxin 17 downregulation
Guadalupe Rojas-Sanchez, Jorge Calzada-Martinez, Brandon McMahon, Aaron C. Petrey, Gabriela Dveksler, Gerardo P. Espino-Solis, Orlando Esparza, Giovanny Hernandez, Dennis Le, Eric P. Wartchow, Ken Jones, Lucas H. Ting, Catherine Jankowski, Marguerite R. Kelher, Marilyn Manco-Johnson, Marie L. Feser, Kevin D. Deane, Travis Nemkov, Angelo D’Alessandro, Andrew Thorburn, Paola Maycotte, José A. López, Pavel Davizon-Castillo
Guadalupe Rojas-Sanchez, Jorge Calzada-Martinez, Brandon McMahon, Aaron C. Petrey, Gabriela Dveksler, Gerardo P. Espino-Solis, Orlando Esparza, Giovanny Hernandez, Dennis Le, Eric P. Wartchow, Ken Jones, Lucas H. Ting, Catherine Jankowski, Marguerite R. Kelher, Marilyn Manco-Johnson, Marie L. Feser, Kevin D. Deane, Travis Nemkov, Angelo D’Alessandro, Andrew Thorburn, Paola Maycotte, José A. López, Pavel Davizon-Castillo
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Research Article Hematology Metabolism

TNF-α impairs platelet function by inhibiting autophagy and disrupting metabolism via syntaxin 17 downregulation

Abstract

Platelets play a dual role in hemostasis and inflammation-associated thrombosis and hemorrhage. Although the mechanisms linking inflammation to platelet dysfunction remain poorly understood, our previous work demonstrated that TNF-α alters mitochondrial mass, platelet activation, and autophagy-related pathways in megakaryocytes. Here, we hypothesized that TNF-α impairs platelet function by disrupting autophagy, a process critical for mitochondrial health and cellular metabolism. Using human and murine models of TNF-α–driven diseases, including myeloproliferative neoplasms and rheumatoid arthritis, we found that TNF-α downregulates syntaxin 17 (STX17), a key mediator of autophagosome-lysosome fusion. This disruption inhibited autophagy, leading to the accumulation of dysfunctional mitochondria and reduced mitochondrial respiration. These metabolic alterations compromised platelet-driven clot contraction, a process linked to thrombotic and hemorrhagic complications. Our findings reveal a mechanism by which TNF-α disrupts hemostasis through autophagy inhibition, highlighting TNF-α as a critical regulator of platelet metabolism and function. This study provides potentially new insights into inflammation-associated pathologies and suggests autophagy-targeting strategies as potential therapeutic avenues to restore hemostatic balance.

Authors

Guadalupe Rojas-Sanchez, Jorge Calzada-Martinez, Brandon McMahon, Aaron C. Petrey, Gabriela Dveksler, Gerardo P. Espino-Solis, Orlando Esparza, Giovanny Hernandez, Dennis Le, Eric P. Wartchow, Ken Jones, Lucas H. Ting, Catherine Jankowski, Marguerite R. Kelher, Marilyn Manco-Johnson, Marie L. Feser, Kevin D. Deane, Travis Nemkov, Angelo D’Alessandro, Andrew Thorburn, Paola Maycotte, José A. López, Pavel Davizon-Castillo

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Figure 6

Inhibition of autophagic pathways in platelets from mice with rheumatoid arthritis and inflammatory bowel disease is linked to low STX17 levels.

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Inhibition of autophagic pathways in platelets from mice with rheumatoid...
(A) Spatial RNA transcriptomics of bone marrow megakaryocytes (MKs); littermate controls (n = 1) and TNFdARE (n = 1) mice. Immunofluorescence for CD41, ACTA2, PECAM1, and DNA; the circles represent the regions of interest (ROIs) selected for the transcriptomic analysis. Scale bar: 2 mm. KEGG analysis of differentially expressed genes in the control (n = 9) and TNFdARE (n = 12) groups. (B) Immunoblot analysis of LC3B-II and TOM20 in platelets from control (n = 5) and TNFdARE (n = 4) mice treated with vehicle (PBS) or CQ (50 μM), before-and-after graph; 2-way ANOVA, Šídák’s test. Noncontiguous gel lanes are indicated. (C) Immunoblot analysis of STX17 in platelets from Ctrl (n = 3) and TNFdARE (n = 3) mice, before-and-after graph; 2-way ANOVA, Šídák’s test. (D and E) Immunoblot analysis of LC3B-II from HCs (n = 8) and patients with RA (n = 5) and TOM20 from HCs (n = 6) and patients with RA (n = 5) treated with vehicle (PBS) or CQ (50 μM). Before-and-after graph; 2-way ANOVA, Šídák’s test, Šídák’s test. (F) Summary of autophagic flux, accumulation of damaged mitochondria, and platelet hemostasis in TNFdARE mice and patients with RA. (G) Summary of autophagic flux.