Litcius/Paper detail

An ACE inhibitor reduces bactericidal activity of human neutrophils in vitro and impairs mouse neutrophil activity in vivo

Duo‐Yao Cao, Jorge F. Giani, Luciana C. Veiras, Ellen A. Bernstein, Derick Okwan‐Duodu, Faizan Ahmed, Catherine Bresee, Warren G. Tourtellotte, S. Ananth Karumanchi, Kenneth E. Bernstein, Zakir Khan

2021Science Translational Medicine39 citationsDOIOpen Access PDF

Abstract

in vitro. In vivo, ACEI-treated mice infected with MRSA had increased bacteremia and tissue bacteria counts compared to mice treated with an ARB or with no drug. Similarly, ACEIs, but not ARBs, increased the incidence of MRSA-induced infective endocarditis in mice with aortic valve injury. Neutrophils from ACE knockout (KO) mice or mice treated with an ACEI produced less leukotriene B4 (LTB4) upon stimulation with MRSA or lipopolysaccharide, whereas neutrophils overexpressing ACE produced more LTB4 compared to wild-type neutrophils. As a result of reduced LTB4 production, ACE KO neutrophils showed decreased survival signaling and increased apoptosis. In contrast, neutrophils overexpressing ACE had an enhanced survival phenotype. Last, in a cohort of human volunteers receiving the ACEI ramipril for 1 week, ACEI administration reduced neutrophil superoxide and reactive oxygen species production and neutrophils isolated from volunteers during ramipril treatment had reduced bactericidal activity. Together, these data demonstrate that ACEI treatment, but not ARB treatment, can reduce the bacterial killing ability of neutrophils.

Topics & Concepts

In vivoIn vitroNeutrophil extracellular trapsNeutrophileMicrobiologyPharmacologyChemistryImmunologyInflammationBiologyBiochemistryBiotechnologyNeutrophil, Myeloperoxidase and Oxidative MechanismsS100 Proteins and AnnexinsImmune Response and Inflammation