Literature DB >> 25316332

High red blood cell nitric oxide synthase activation is not associated with improved vascular function and red blood cell deformability in sickle cell anaemia.

Marijke Grau1, Anaïs Mozar, Keyne Charlot, Yann Lamarre, Linda Weyel, Frank Suhr, Bianca Collins, Stéphane Jumet, Marie-Dominique Hardy-Dessources, Marc Romana, Nathalie Lemonne, Maryse Etienne-Julan, Sophie Antoine-Jonville, Wilhelm Bloch, Philippe Connes.   

Abstract

Human red blood cells (RBC) express an active and functional endothelial-like nitric oxide (NO) synthase (RBC-NOS). We report studies on RBC-NOS activity in sickle cell anaemia (SCA), a genetic disease characterized by decreased RBC deformability and vascular dysfunction. Total RBC-NOS content was not significantly different in SCA patients compared to healthy controls; however, using phosphorylated RBC-NOS-Ser(1177) as a marker, RBC-NOS activation was higher in SCA patients as a consequence of the greater activation of Akt (phosphorylated Akt-Ser(473) ). The higher RBC-NOS activation in SCA led to higher levels of S-nitrosylated α- and β-spectrins, and greater RBC nitrite and nitrotyrosine levels compared to healthy controls. Plasma nitrite content was not different between the two groups. Laser Doppler flowmetric experiments demonstrated blunted microcirculatory NO-dependent response under hyperthermia in SCA patients. RBC deformability, measured by ektacytometry, was reduced in SCA in contrast to healthy individuals, and pre-shearing RBC in vitro did not improve deformability despite an increase of RBC-NOS activation. RBC-NOS activation is high in freshly drawn blood from SCA patients, resulting in high amounts of NO produced by RBC. However, this does not result in improved RBC deformability and vascular function: higher RBC-NO is not sufficient to counterbalance the enhanced oxidative stress in SCA.
© 2014 John Wiley & Sons Ltd.

Entities:  

Keywords:  blood rheology; microcirculation; nitric oxide synthase; sickle cell anaemia

Mesh:

Substances:

Year:  2014        PMID: 25316332     DOI: 10.1111/bjh.13185

Source DB:  PubMed          Journal:  Br J Haematol        ISSN: 0007-1048            Impact factor:   6.998


  15 in total

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