Rusotinibe comprimidos (ruxolitinibe / Jakafi) para o tratamento de fibrose da medula óssea com risco moderado ou alto, incluindo fibrose da medula óssea primária, mielofibrose após policitemia vera e mielofibrose após paciente com trombocitose idiopática. Pacientes com fibrose da medula óssea de risco moderado ou alto referem-se a pacientes com mais de 65 anos de idade ou têm uma das seguintes condições: anemia, sintomas físicos, diminuição da contagem de leucócitos, diminuição da contagem de células embrionárias ou diminuição da contagem de plaquetas. 80% a 90% dos casos.
Rusotinib tablets (ruxolitinib / Jakafi) are currently marketed in the United States, Europe and other places, but are still not marketed in mainland China. Rusolitinib is the first Janus associated kinase (JAK) inhibitor approved in the world so far, and the first specific myelofibrosis treatment drug approved by the FDA and the world. Rusotinib is available in 5 doses of 5, 10, 15, 20, and 25 mg / tablet, and is administered as an oral regimen twice a day. Bone marrow fibrosis is a progressive and potentially life-threatening rare blood system disease, which is a myeloproliferative tumor and is estimated to affect 1.60-18.5 million people in the United States. Bone marrow fibrosis patients are gradually replaced by scar tissue, so that blood cell production has to be carried out in organs such as liver and spleen. Anemia, leukopenia, and thrombocytopenia occur. Patients with bone marrow fibrosis are characterized by bone marrow failure and splenomegaly, as well as fatigue, musculoskeletal pain, abdominal discomfort, severe itching, night sweating, and satiety, which seriously impair the quality of life. Splenomegaly and systemic symptoms in patients with myelofibrosis are associated with JAK pathway signaling dysfunction. Rusotinib is an oral JAK1 and JAK2 inhibitor, and JAK1 and JAK2 are involved in the regulation of blood and immune function.
Certificação The decision to approve the above lusotinib was mainly based on data from two phase III randomized, double-blind, and controlled clinical trials with two codenames, COMFORT-I and COMPORT-Ⅱ. The COMFORT-I study included a total of 309 patients with uncomfortable or resistant allogeneic bone marrow transplantation, or relapsed primary bone marrow fibrosis, myelofibrosis after polycythemia and idiopathic thrombocythemia, and the results showed The proportion of patients who achieved the primary end point after 24 weeks of treatment with lusotinib or placebo, even if the spleen volume decreased by ≥35%, was 41.9% and O. respectively. 7% (P <0.000 1). In addition, the proportion of patients with an improvement of ≥50% in the improved Myelofibrosis Symptom Assessment Form Total Symptom Score (MFSAF TSS) in the two groups of lusotinib or placebo was 45.9% and 5.3% (P <0.001), and the median time to response was less than 4 weeks. The C0MPORT-11 study included 219 patients with uncomfortable or allogeneic bone marrow transplantation, or relapsed primary bone marrow fibrosis, myelofibrosis after polycythemia and idiopathic thrombocytosis, and the results showed that The proportion of patients with sotinib or the best therapy hydroxyurea (hydroxyurea) or glucocorticoid after 48 weeks of treatment to reduce the spleen volume ≥35% was 28.5% and 0 (P <0.001). Os efeitos colaterais hematológicos mais comuns do tratamento com lusotinibe observados no C0MPORT-I e no COMPORT-11 foram trombocitopenia e anemia relacionadas à dose, mas esses dois efeitos colaterais são fáceis de controlar e raramente levam os pacientes a interromper o tratamento; os efeitos colaterais mais comuns não relacionados ao sistema sanguíneo são diarreia, tontura, dor de cabeça, fadiga e náusea.
