ATPergic signaling disruption in human sepsis as a potential source of biomarkers for clinical use

Author:

Leite Rafael Olivé1,de Souza Priscila Oliveira2,Haas Clarissa Branco2,Silveira Fernando da3,Mohr Kauan3,Bertoni Ana Paula Santin2,Soares Mayara S. Pereira1,Azambuja Juliana H.2,Prá Morgana Dal2,Cruz Lorraynne Letycia Prado da2,Gelsleichter Nicolly Espindola2,Begnini Karine4,Haskó George5,Wink Márcia R.2,Spanevello Roselia M.1,Braganhol Elizandra2

Affiliation:

1. Universidade Federal de Pelotas

2. Universidade Federal de Ciências da Saúde de Porto Alegre

3. Hospital Nossa Senhora da Conceição

4. Federal University of Rio Grande do Sul

5. Columbia University

Abstract

Abstract Sepsis is a life-threatening organ dysfunction caused by a dysregulated inflammatory response to infection. To date, there is no specific treatment established for sepsis. In the extracellular compartment, purines such as adenosine triphosphate (ATP) and adenosine play essential roles in the immune/inflammatory responses during sepsis and septic shock. The balance of extracellular levels among ATP and adenosine are intimately involved in the signals related to immune stimulation/immunosuppression balance. Specialized enzymes, including CD39, CD73, and adenosine deaminase (ADA), are responsible to metabolize ATP to adenosine which will further sensitize the P2 and P1 purinoceptors, respectively. Disruption of the purinergic pathway had been described in the sepsis pathophysiology. Although purinergic signaling has been suggested as a potential target for sepsis treatment, the majority of data available was obtained using pre-clinical approaches. We hypothesized that, as a reflection of deregulation on purinergic signaling, septic patients exhibit differential measurements of serum, neutrophils and monocytes purinergic pathway markers when compared to two types of controls (ward and healthy). It was observed that ATP and ADP serum levels were increased in septic patients, as well as the A2a mRNA expression in neutrophils and monocytes. Both ATPase/ADPase activities were increased during sepsis. Serum ATP and ADP levels, and both ATPase and ADPase activities were associated with the diagnosis of sepsis, representing potential biomarkers candidates. In conclusion, our results advance the translation of purinergic signaling from pre-clinical models into the clinical setting opening opportunities for so much needed new strategies for sepsis and septic shock diagnostics and treatment.

Publisher

Research Square Platform LLC

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