| Literature DB >> 25763868 |
Benoît Vingert1,2, Marie Tamagne1,2, Anoosha Habibi2,3, Sadaf Pakdaman1,2, Julie Ripa1,2, Rahma Elayeb1,2, Frédéric Galacteros2,3,4, Philippe Bierling1,2, Hélène Ansart-Pirenne1, Pablo Bartolucci2,3,4, France Noizat-Pirenne1,2,4.
Abstract
Alloimmunization against red blood cells (RBCs) is the main immunological risk associated with transfusion in patients with sickle cell disease (SCD). However, about 50-70% of SCD patients never get immunized despite frequent transfusion. In murine models, CD4(+) T cells play a key role in RBC alloimmunization. We therefore explored and compared the CD4(+) T-cell phenotypes and functions between a group of SCD patients (n = 11) who never became immunized despite a high transfusion regimen and a group of SCD patients (n = 10) who had become immunized (at least against Kidd antigen b) after a low transfusion regimen. We studied markers of CD4(+) T-cell function, including TLR, that directly control lymphocyte function, and their spontaneous cytokine production. We also tested responders for the cytokine profile in response to Kidd antigen b peptides. Low TLR2/TLR3 expression and, unexpectedly, strong expression of CD40 on CD4(+) T cells were associated with the nonresponder status, whereas spontaneous expression of IL-10 by CD4(+) T cells and weak Tbet expression were associated with the responder status. A Th17 profile was predominant in responders when stimulated by Jb(k) . These findings implicate CD4(+) T cells in alloimmunization in humans and suggest that they may be exploited to differentiate responders from nonresponders.Entities:
Keywords: Alloimmunization; CD4+ T cells; Jkb; Sickle cell disease; Th17
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Year: 2015 PMID: 25763868 DOI: 10.1002/eji.201445187
Source DB: PubMed Journal: Eur J Immunol ISSN: 0014-2980 Impact factor: 5.532