Barranco-Lampón Gilberto, Martínez-Castro Raúl, Arana-Luna Luara, Álvarez-Vera José Luis, Rojas-Castillejos Flavio, Peñaloza-Ramírez Rosalinda, Carballo-Zarate Adrián Alejandro, Olarte-Carrillo Irma, Minamy Jaime Israel-García, López-Salazar Javier, Navarrete Juan José, Espinosa-Partida Arturo, Ventura-Enríquez Yanet, Ruiz-Contreras Josué Isel, Aguirre-Reyes Oyuky Gissell, Anaya-Cuéllar Irene, Aguilar-Luévano Jocelyn, Díaz-Ramírez Hugo Francisco, Herrera-Olivares Wilfrido, Aguilar-Hidalgo José Antonio, Alcívar-Cedeño Luisa Ma, Hernández-Caballero Álvaro, Galaz-Cordero Lourdes Elena, Peña-Celaya José Antonio de la, Báez-Islas Pamela Elena, Bates-Martín Ramón Alberto, Cano-León Ana Ma de la Luz, Espitia-Ríos Ma Eugenia, Barbosa Diego, Morales-Adrián Javier, Pacheco Martín Jacobo, Delgado-López Nancy, Neme-Yunes Yvette, Moralws-Hernández Alba Edna, Mújica-Martínez Aldo, Pérez-Lizardi Alejandra Betsabé, Pérez-Gómez Karen Daniela, Barragán-Ibáñez Gabriel, Martínez Adolfo, Flores-Ordúñez Karen, Ramírez-Hoyos Paulina, Rosales-López Ma de Los Ángeles, Acosta-Maldonado Brenda Lizeth, Jiménez-Ochoa Marco Alejandro, Garzón-Velásquez Katheryn Betsabé, Hernández-Ruiz Eleazar, McNally-Guillén Bosco Martín, Saucedo-Montes Erick Eduardo, Aguilar-Andrade Carolina, Vivas-Arteaga Cindy Lissette, Guerra-Alarcón Lidia Virginia, Milán-Salvatierra Andrea Iracema, Campa-Monroy Dafne Itzel, Cota-Rangel Xóchitl, Estrada-Domínguez Patricia, García-Camacho Alinka Socorro, García-Castillo Carolina, Banda-García Luisa Iztacihuatl, Rodríguez-Sánchez Vania, Meillón-García Luis Antonio, Urbina-Escalante Elizabeth, Martínez-Ramírez Mario Alberto, Loera-Fragoso Sergio José, Martínez-Coronel Jorge, Zapata-Canto Nidia, Gómez-Cortés Sue Cynthia, Medina-Coral Jesús Emanuel, Mójica-Balderas Liliana, Pérez-Zúñiga Juan Manuel, Pérez Fernando Jacobo, López-Arroyo José Luis, Zazueta-Pozos Juan Francisco, Romero-Martínez Eduardo, Romero-Rodelo Hilda, Tapia-Enríquez Ana Laura, Soriano-Mercedes Emely Johanny, Salazar-Ramírez Óscar, Vilchis-González Shendel Paulina, Tepepa-Flores Fredy, Alvarado-Ibarra Martha
Servicio de Hematología, Hospital General de México, Ciudad de México, México.
Servicio de Hematología, Instituto Nacional de Cancerología, Ciudad de México, México.
Gac Med Mex. 2022;158(Supl 1):26-37. doi: 10.24875/GMM.M22000804.
Myelofibrosis (MF) is a BCR-ABL1-negative myeloproliferative neoplasm characterized by clonal myeloproliferation, dysregulated kinase signaling, and release of abnormal cytokines. In recent years, important progress has been made in the knowledge of the molecular biology and the prognostic assessment of MF. Conventional treatment has limited impact on the patients' survival; it includes a wait-and-see approach for asymptomatic patients, erythropoiesis-stimulating agents, androgens, or immunomodulatory agents for anemia, cytoreductive drugs such as hydroxyurea for the splenomegaly and constitutional symptoms, and splenectomy or radiotherapy in selected patients. The discovery of the Janus kinase (JAK) 2 mutation triggered the development of molecular targeted therapy of MF. The JAK inhibitors are effective in both JAK2-positive and JAK2-negative MF; one of them, ruxolitinib, is the current best available therapy for MF splenomegaly and constitutional symptoms. Although ruxolitinib has changed the therapeutic scenario of MF, there is no clear indication of a disease-modifying effect. Allogeneic stem cell transplantation remains the only curative therapy of MF, but due to its associated morbidity and mortality, it is usually restricted to eligible high- and intermediate-2-risk MF patients. To improve current therapeutic results, the combination of JAK inhibitors with other agents is currently being tested, and newer drugs are being investigated.
骨髓纤维化(MF)是一种BCR-ABL1阴性骨髓增殖性肿瘤,其特征为克隆性骨髓增殖、激酶信号失调以及异常细胞因子的释放。近年来,在MF的分子生物学知识和预后评估方面取得了重要进展。传统治疗对患者生存的影响有限;对于无症状患者采取观察等待的方法,对于贫血患者使用促红细胞生成剂、雄激素或免疫调节剂,对于脾肿大和全身症状使用羟基脲等细胞减灭药物,对于部分患者进行脾切除术或放疗。Janus激酶(JAK)2突变的发现推动了MF分子靶向治疗的发展。JAK抑制剂对JAK2阳性和JAK2阴性MF均有效;其中一种,鲁索替尼,是目前治疗MF脾肿大和全身症状的最佳可用疗法。尽管鲁索替尼改变了MF的治疗局面,但尚无明确迹象表明其具有改善疾病的效果。异基因干细胞移植仍然是MF的唯一治愈性疗法,但由于其相关的发病率和死亡率,通常仅限于符合条件的高危和中危2级MF患者。为了改善当前的治疗效果,目前正在测试JAK抑制剂与其他药物的联合使用,并且正在研究更新的药物。
