Abstract

BackgroundFamilial hemophagocytosis (FHL) is a rare disease associated with defects in proteins involved in CD8+ T-cell cytotoxicity. Hyperactivation of immune cells results in a perilous, Th1-driven cytokine storm. We set out to explore the regulation of cytokines in an FHL patient who was clinically stable on low-dose immunosuppressive therapy after bone marrow transplantation over a six-month period. During this period, chimerism analyses showed that the fraction of host cells was between 1 and 10%. Both parents of the patient as well as healthy volunteers were studied for comparison.Methods/Principal FindingsUsing ELISA, quantitative real-time PCR, and clinical laboratory methods, we investigated constitutive and inducible cytokines, polymorphisms, and clinical parameters in whole blood and whole blood cultures. Although routine laboratory tests were within the normal range, the chemokines IP-10 and IL-8 as well as the cytokine IL-27p28 were increased up to 10-fold under constitutive and stimulated conditions compared to healthy controls. Moreover, high levels of IFNγ and TNFα were produced upon stimulation. Unexpectedly, IFNγ induction of IL-18 binding protein (IL-18BP) was markedly reduced (1.6-fold vs 5-fold in controls). The patient's mother featured intermediately increased cytokine levels, whereas levels in the father were similar to those in the controls.Conclusions/SignificanceSince IL-18 plays a major role in perpetuating hemophagocytosis, the failure of IFNγ to induce IL-18BP may constitute a fundamental pathogenetic mechanism. Furthermore, increased production of IL-8 and IL-27 appears to be associated with this disease. Such dysregulation of cytokines was also found in the heterozygous parents, providing a novel insight into genotype-phenotype correlation of FHL which may encourage future research of this rare disease.

Highlights

  • Hemophagocytic lymphohistiocytosis (HLH), called hemophagocytic or macrophage activation syndrome, is the name of a group of rare diseases characterized by a dysregulation of the immune system

  • Both IL-18 binding protein (IL18BP) and IP-10 were elevated in Whole Blood (WB) cultures from our patient under steady-state conditions, the near absent induction of the Th1 antagonist IL-18 binding protein (IL-18BP) by IFNc was striking

  • LPS-induced increases in the pro-inflammatory chemokines IP-10 (14-fold) and IL-8 (20-fold) were comparable to or even greater than in control subjects. This suggests the conclusion that, despite bone marrow transplantation (BMT) and immunosuppression, regulation of IL-18BP is severely impaired in the familial HLH (FHL) patient

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Summary

Introduction

Hemophagocytic lymphohistiocytosis (HLH), called hemophagocytic or macrophage activation syndrome, is the name of a group of rare diseases characterized by a dysregulation of the immune system. The group of inherited HLH comprises familial HLH (FHL) and the Chediak-Higashi and Griscelli syndromes, which are associated with various gene defects, but are nearly identical in clinical presentation. We set out to explore the regulation of cytokines in an FHL patient who was clinically stable on low-dose immunosuppressive therapy after bone marrow transplantation over a six-month period. During this period, chimerism analyses showed that the fraction of host cells was between 1 and 10%. Both parents of the patient as well as healthy volunteers were studied for comparison

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