Barosi Giovanni, Tefferi Ayalew, Gangat Naseema, Szuber Natasha, Rambaldi Alessandro, Odenike Olatoyosi, Kröger Nicolaus, Gagelmann Nico, Talpaz Moshe, Kantarjian Hagop, Gale Robert Peter
Center for the Study of Myelofibrosis, IRCCS Policlinico S Matteo Foundation, Pavia, Italy.
Division of Hematology, Department of Medicine, Mayo Clinic, Rochester, MN, USA.
Lancet Haematol. 2024 May;11(5):e383-e389. doi: 10.1016/S2352-3026(24)00067-X. Epub 2024 Apr 8.
Myelofibrosis is a myeloid neoplasm characterised by the presence of JAK2, CALR, or MPL mutations (with a 90% mutation frequency) and trilineage myeloid proliferation with prominent megakaryocyte atypia. People with myelofibrosis have a lower survival rate and poorer quality of life than healthy individuals. Therapy for myelofibrosis uses Janus kinase inhibitors, which reduce splenomegaly and alleviate symptoms. Regulatory approvals for Janus kinase inhibitors have focused on this dual endpoint. In this Viewpoint, we discuss the validity of using spleen reduction as a surrogate endpoint for the disease-modifying activity of candidate drugs for myelofibrosis. We suggest alternative endpoints addressing unmet patient needs, including progression-free survival and overall survival. Moreover, we highlight the importance of selecting a core set of crucial outcomes with which we can individualise clinical decision making and standardise reporting of clinical trials results. We propose selecting patient-reported outcomes and anaemia response. We also suggest integrating economic considerations in the process of evaluating new drugs for myelofibrosis.
骨髓纤维化是一种髓系肿瘤,其特征为存在JAK2、CALR或MPL突变(突变频率为90%)以及伴有显著巨核细胞异型性的三系髓系增殖。与健康个体相比,骨髓纤维化患者的生存率较低,生活质量较差。骨髓纤维化的治疗使用Janus激酶抑制剂,这类药物可减轻脾肿大并缓解症状。Janus激酶抑制剂的监管批准主要集中在这一双重终点上。在本观点文章中,我们讨论了将脾脏缩小作为骨髓纤维化候选药物疾病修饰活性替代终点的有效性。我们建议采用能够满足未满足的患者需求的替代终点,包括无进展生存期和总生存期。此外,我们强调选择一组核心关键结局的重要性,通过这些结局我们可以实现临床决策的个体化,并使临床试验结果的报告标准化。我们建议选择患者报告结局和贫血反应。我们还建议在评估骨髓纤维化新药的过程中纳入经济考量因素。
