CD38high/HLA‐DR+CD8+ T lymphocytes display pathogen‐specific expansion regardless of hemophagocytic lymphohistiocytosis

Author:

Lodi Lorenzo12,Sarli Walter Maria12,Ricci Silvia12,Pisano Laura2,Boscia Silvia2,Mastrolia Maria Vincenza3ORCID,Malinconi Sara1,Fusco Eleonora1,Sieni Elena4,Indolfi Giuseppe56,Simonini Gabriele36,Galli Luisa17,Azzari Chiara12

Affiliation:

1. Department of Health Sciences University of Florence Florence Italy

2. Immunology Unit Meyer Children's Hospital IRCCS Florence Italy

3. Rheumatology Unit Meyer Children's Hospital IRCCS Florence Italy

4. Pediatric Hematology‐Oncology Department Meyer Children's Hospital IRCCS Florence Italy

5. Hepatology Unit Meyer Children's Hospital IRCCS Florence Italy

6. Department NEUROFARBA University of Florence Florence Italy

7. Infectious Disease Unit Meyer Children's Hospital IRCCS Florence Italy

Abstract

AbstractThe characteristic expansion of T CD38high/HLA‐DR+CD8+ lymphocytes observed in hemophagocytic lymphohistiocytosis (HLH) and macrophage activation syndrome (MAS) proved able to distinguish HLH/MAS from sepsis and systemic juvenile idiopathic arthritis. However, the performance of this marker in differentiating HLH/MAS from other pediatric febrile conditions with similar clinical onset and yet entirely different treatments remains unexplored. CD38high/HLA‐DR+CD8+ frequencies measured in the peripheral fresh blood of pediatric patients attended for suspicion of HLH/MAS were retrospectively recorded and clinical characteristics were retrieved. CD38high/HLA‐DR+CD8+ frequencies in HLH/MAS patients (15 patients; median: 22.0%, IQR: 11.0–49.0%) were compared with those who presented febrile conditions other‐than‐HLH (28 patients; median: 13.0%, IQR: 3.9–28.7%; p = 0.24). HLH and non‐HLH patients were subsequently regrouped based on the presence of an identified infection (22 patients; median: 27.0%, IQR: 15.2‐72.1%) and compared with those without infections (21 patients; median: 7.6%, IQR: 3.7–24.3%; p = 0.0035). CD38high/HLA‐DR+CD8+ percentages were significantly higher only in the infection group compared with the noninfection one, with a patent pathogen‐specific expansion in Epstein–Barr virus primoinfection and visceral leishmaniasis regardless of the presence of HLH. CD38high/HLA‐DR+CD8+ frequencies do not appear as an HLH‐specific marker as they naturally expand in other clinical situations that are common in childhood and may mimic HLH initial presentation.

Publisher

Wiley

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