Platelet response to romiplostim amongst patients with newly diagnosed, persistent, and chronic immune thrombocytopenia in routine clinical practice in Denmark, Sweden, and Norway

Author:

Christiansen Christian Fynbo1ORCID,Risbo Nickolaj1,Ghanima Waleed23ORCID,Linder Marie4,Bahmanyar Shahram4,Seesaghur Anouchka56,Clouser Mary56,Nørgaard Mette1,Sørensen Henrik Toft1

Affiliation:

1. Department of Clinical Epidemiology Aarhus University Hospital and Aarhus University Aarhus Denmark

2. Department of Medicine Østfold Hospital Trust Grålum Norway

3. Department of Hematology Oslo University Hospital and Institute of Clinical Medicine, University of Oslo Oslo Norway

4. Clinical Epidemiology Division and Centre for Pharmacoepidemiology, Department of Medicine Karolinska Institutet Stockholm Sweden

5. Center for Observational Research, Amgen Uxbridge UK

6. Center for Observational Research, Amgen Thousand Oaks California USA

Abstract

SummaryPatient characteristics and platelet responses at romiplostim initiation according to the duration of immune thrombocytopenia (ITP) are poorly understood. Amongst romiplostim‐exposed adults with ITP lasting ≥6 months during 2009–2018 in Denmark, Sweden, and Norway, we examined characteristics at romiplostim initiation, romiplostim dosage, and durable platelet response (≥75% of measurements ≥50 × 109/L at 14–24 weeks) for subcohorts with newly diagnosed (duration <3 months), persistent (3–12 months), or chronic (>12 months) ITP initiating romiplostim. The 285 romiplostim initiators comprised 81 (28%) with newly diagnosed, 47 (16%) with persistent, and 157 (55%) with chronic ITP. More patients with newly diagnosed ITP than longer ITP duration, had low comorbidity levels, two or more prior ITP therapies, and previous bleeding requiring hospitalisation. The median romiplostim doses were similar across subcohorts. During treatment, median platelet counts were similar across subcohorts (75–76 × 109/L), and the durable platelet response was 64.6%, 52.9%, and 52.7% for newly diagnosed, persistent, and chronic ITP, respectively. After treatment cessation, the median platelet count was 138 × 109/L, 68 × 109/L, and 71 × 109/L, respectively. In conclusion, newly diagnosed patients, compared with romiplostim initiators with longer disease duration, had more severe ITP, higher frequency of durable platelet response, and higher median platelet count after cessation.

Funder

Amgen

Publisher

Wiley

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