Abstract

The International Paroxysmal Nocturnal Hemoglobinuria (PNH) Registry (NCT01374360) was initiated to optimize patient management by collecting data regarding disease burden, progression, and clinical outcomes. Herein, we report updated baseline demographics, clinical characteristics, disease burden data, and observed trends regarding clone size in the largest cohort of Registry patients. Patients with available data as of July 2017 were stratified by glycosylphosphatidylinositol (GPI)-deficient granulocyte clone size (< 10%, ≥ 10%–< 50%, and ≥ 50%). All patients were untreated with eculizumab at baseline, defined as date of eculizumab initiation or date of Registry enrollment (if never treated with eculizumab). Outcomes assessed in the current analysis included proportions of patients with high disease activity (HDA), history of major adverse vascular events (MAVEs; including thrombotic events [TEs]), bone marrow failure (BMF), red blood cell (RBC) transfusions, and PNH-related symptoms. A total of 4439 patients were included, of whom 2701 (60.8%) had available GPI-deficient granulocyte clone size data. Among these, median clone size was 31.8% (1002 had < 10%; 526 had ≥ 10%–< 50%; 1173 had ≥ 50%). There were high proportions of patients with HDA (51.6%), history of MAVEs (18.8%), BMF (62.6%), RBC transfusion (61.3%), and impaired renal function (42.8%). All measures except RBC transfusion history significantly correlated with GPI-deficient granulocyte clone size. A large proportion of patients with GPI-deficient granulocyte clone size < 10% had hemolysis (9.7%), MAVEs (10.2%), HDA (9.1%), and/or PNH-related symptoms. Although larger GPI-deficient granulocyte clone sizes were associated with higher disease burden, a substantial proportion of patients with smaller clone sizes had history of MAVEs/TEs.

Highlights

  • Paroxysmal nocturnal hemoglobinuria (PNH) is a rare, acquired, potentially life-threatening hematologic disorder characterized by chronic, intravascular hemolysis caused by uncontrolled activation of the terminal complement pathway [1,2,3]

  • PNH is a clinically heterogeneous disease; in addition to the primary clinical manifestation of chronic intravascular hemolysis, it is associated with bone marrow failure (BMF; e.g., aplastic anemia, myelodysplastic syndrome) and thrombophilia [4,5,6]

  • More than half of the patients (51.6%) had high disease activity (HDA) at baseline, and the proportion of patients with HDA at baseline correlated significantly with GPI-deficient granulocyte clone size category; higher proportions of patients with HDA were observed in subgroups with higher clone size (P < 0.0001)

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Summary

Introduction

Paroxysmal nocturnal hemoglobinuria (PNH) is a rare, acquired, potentially life-threatening hematologic disorder characterized by chronic, intravascular hemolysis caused by uncontrolled activation of the terminal complement pathway [1,2,3]. PNH occurs as a consequence of a somatic mutation in the phosphatidylinositol glycan class A gene in bone marrow stem cells, followed by clonal expansion of the mutated cells. This genetic mutation causes impaired glycosylphosphatidylinositol (GPI) biosynthesis and deficient GPI-anchored complement regulatory proteins on the surface of mature blood cells [4, 13]. Patients with larger GPIdeficient granulocyte clone size generally experience more debilitating symptoms and consequences of chronic complementmediated intravascular hemolysis, limited data suggest that smaller GPI-deficient granulocyte clones may confer significant disease burden [5, 6]. While larger GPI-deficient granulocyte clone size is associated with increased TE risk, all patients with PNH are at risk for a TE regardless of clone size [6, 11, 14, 15]

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