RED BLOOD CELL SENESCENCE IN INFLAMMATORY CHRONIC DISEASES

STAMPONE, ROCÍO; PACINI, ANTONELLA; ENSINCK, ALEJANDRA; TANNO, FEDERICO; DINATALE,BRENDA; LEIVA, RODOLFO; RAMOS, KARINA; BESSONE, FERNANDO; REGGIARDO, VIRGINIA; PEREZ, ANA ROSA; COTORRUELO, CARLOS; VILLAR, SILVINA

Mar del Plata

Congreso; Reunión anual de Sociedades de Biociencias (SAIC, SAB, AAFE, AACyTAL); 2023

SAIC, SAB, AAFE, AACyTAL

RED BLOOD CELL SENESCENCE IN INFLAMMATORY CHRONIC DISEASESRocío Stampone1, Antonella Pacini1, Alejandra Ensinck2, Federico Tanno3, Brenda Dinatale1, Rodolfo Leiva4, Karina Ramos4, Fernando Bessone3, M. Virginia Reggiardo3, Ana Rosa Pérez1, Carlos Cotorruelo1, Silvina Villar11Instituto de Inmunología Clínica y Experimental Rosario (IDICER-CONICET-UNR), Rosario, Argentina2Área de Inmunología. Facultad de Ciencias Bioquímicas y Farmacéuticas, UNR, Rosario, Argentina3Servicio de gastroenterología y hepatología del Hospital Provincial del Centenario, Rosario, Argentina4Servicio y Cátedra de Cardiología, Hospital Provincial del Centenario y Fac. de Cs. Médicas, UNR, Rosario, ArgentinaE-mail: rociostampone@gmail.com Chronic inflammatory diseases, regardless of their nature, could impact various physiological processes, including the senescence of blood cells. While it is known that the average lifespan of red blood cells (RBCs) is 120 days, there is evidence to support that chronic inflammatory processes could accelerate the erythrocyte aging. Thus, it is possible that RBCs may have a shorter half-life in pathologies like Chagas disease (CD) and autoimmune hepatitis (AIH). This study aims to identify changes in aging markers of RBCs, such as an increase in autologous IgG antibodies on the RBCs membrane that bind to band 3, stimulating C3b deposition and erythrophagocytosis, and a decrease in the expression of CD47, a transmembrane protein which acts as a “don’t eat me” signal. In both cases, the removal of RBCs by macrophages is promoted. For this, we recruited individuals infected with Trypanosoma Cruzi who developed Chronic Chagas Cardiomyopathy (CCC, n=7) and those without cardiac pathology (Indeterminate form (IND), n=18), as well as patients with AIH (n=10). Healthy volunteers were matched according to sex and age (Co, n=10). Flow cytometry has been applied for detection of CD47 and RBCs-bound IgG. CD47 expression was lower in both AIH, IND vs. Co, as indicated by the Median Fluorescence Intensity values (*p