Immunophenotypic Parameters and RBC Alloimmunization in Children with Sickle Cell Disease on Chronic Transfusion

Overview

Journal Am J Hematol

Specialty Hematology

Date 2015 Sep 12

PMID 26361243

Citations 30

Authors

Robert S Nickel

John T Horan

Ross M Fasano

Erin Meyer

Cassandra D Josephson

Anne M Winkler

Marianne E M Yee

Leslie S Kean

Jeanne E Hendrickson

Affiliations

Soon will be listed here.

Abstract

Alloimmunization against red blood cell (RBC) antigens is a cause of morbidity and mortality in transfused patients with sickle cell disease (SCD). To investigate distinguishing characteristics of patients who develop RBC alloantibodies after transfusion (responders) versus those who do not (non-responders), a cross-sectional study of 90 children with SCD on chronic RBC transfusion therapy at a single institution was conducted in which 18 immune parameters (including T and B cell subsets) were tested via flow cytometry, and medical records were reviewed. RBC alloimmunization was present in 26/90 (29%) patients, with anti-E, K, and C among the most commonly detected alloantibodies despite prophylactic matching for these antigens at the study institution. In addition, RBC autoantibodies had been detected in 18/26 (69%) of alloimmunized versus 7/64 (11%) of non-alloimmunized patients (P < 0.0001). Alloimmunized patients were significantly older (median 13.0 years vs. 10.7 years, P = 0.010) and had more RBC unit exposures (median 148 U vs. 82 U, P = 0.020) than non-alloimmunized patients. Sex, age at initiation of chronic transfusion, splenectomy, stroke, and transfusion outside of the study institution were not significantly associated with RBC alloimmunization. Alloimmunized patients had a significantly increased percentage of CD4+ T memory cells compared to non-alloimmunized patients (57% vs. 49%, P = 0.0047), with no other significant differences in immune cell subsets or laboratory values detected between these groups. Additional research of RBC alloimmunization is needed to optimize transfusion therapy and to develop strategies to prevent alloimmunization.

Citing Articles

Adding hydroxyurea to chronic transfusion therapy for sickle cell anemia reduces transfusion burden.

Nickel R, Margulies S, Panchapakesan K, Chorvinsky E, Nino G, Gierdalski M Transfusion. 2024; 65(1):38-49.

PMID: 39580793 PMC: 11750600. DOI: 10.1111/trf.18073.

Increased memory phenotypes of CD4+ and CD8+ T cells in children with sickle cell anaemia in Tanzania.

Balandya E, Reynolds T, Aboud S, Obaro S, Makani J Tanzan J Health Res. 2024; 19(2).

PMID: 39211632 PMC: 11361362. DOI: 10.4314/thrb.v19i2.3.

Post-transfusion biotin-labeled red blood cell survival studies in pediatric sickle cell disease with antibodies of uncertain significance.

Yee M, Zerra P, McCoy J, Covington M, Stowell S, Joiner C Transfusion. 2024; 64(5):800-807.

PMID: 38506450 PMC: 11088511. DOI: 10.1111/trf.17800.

Proinflammatory state promotes red blood cell alloimmunization in pediatric patients with sickle cell disease.

Zheng Y, Gossett J, Chen P, Barton M, Ryan M, Yu J Blood Adv. 2023; 7(17):4799-4808.

PMID: 37023228 PMC: 10469551. DOI: 10.1182/bloodadvances.2022008647.

The Development and Consequences of Red Blood Cell Alloimmunization.

Arthur C, Stowell S Annu Rev Pathol. 2022; 18:537-564.

PMID: 36351365 PMC: 10414795. DOI: 10.1146/annurev-pathol-042320-110411.