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高危骨髓恶性肿瘤的分化治疗:伴随的II期研究结果

Differentiation therapy in poor risk myeloid malignancies: Results of companion phase II studies.

作者信息

Norsworthy Kelly J, Cho Eunpi, Arora Jyoti, Kowalski Jeanne, Tsai Hua-Ling, Warlick Erica, Showel Margaret, Pratz Keith W, Sutherland Lesley A, Gore Steven D, Ferguson Anna, Sakoian Sarah, Greer Jackie, Espinoza-Delgado Igor, Jones Richard J, Matsui William H, Smith B Douglas

机构信息

Johns Hopkins University, Sidney Kimmel Comprehensive Cancer Center, Baltimore, MD, United States.

Biostatistics and Bioinformatics Shared Resource, Winship Cancer Institute of Emory University, Atlanta, GA, United States.

出版信息

Leuk Res. 2016 Oct;49:90-7. doi: 10.1016/j.leukres.2016.09.003. Epub 2016 Sep 3.

DOI:10.1016/j.leukres.2016.09.003
PMID:27619199
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8829813/
Abstract

Pre-clinical data in non-M3 AML supports the use of differentiation therapy, but clinical activity has been limited. Myeloid growth factors can enhance anti-leukemic activity of differentiating agents in vitro. We conducted companion phase II trials investigating sargramostim (GM-CSF) 125μg/m(2)/day plus 1) bexarotene (BEX) 300mg/m(2)/day or 2) entinostat (ENT) 4-8mg/m(2)/week in patients with MDS or relapsed/refractory AML. Primary endpoints were response after at least two treatment cycles and toxicity. 26 patients enrolled on the BEX trial had a median of 2 prior treatments and 24 enrolled on the ENT trial had a median of 1. Of 13 response-evaluable patients treated with BEX, the best response noted was hematologic improvement in neutrophils (HI-N) seen in 4 (31%) patients; none achieved complete (CR) or partial remission (PR). Of 10 treated with ENT, there was 1 (10%) partial remission (PR) and 2 (20%) with HI-N. The secondary endpoint responses of HI-N with each combination were accompanied by a numerical increase in ANC (BEX: 524 to 931 cells/mm(3), p=0.096; ENT: 578 to 1 137 cells/mm(3), p=0.15) without increasing marrow blasts. Shared grade 3-4 non-hematologic toxicities included febrile neutropenia, bone pain, fatigue, and dyspnea. GM-CSF plus either BEX or ENT are well tolerated in resistant and refractory MDS and AML and showed modest clinical and biologic activity, most commonly HI-N.

摘要

非M3型急性髓系白血病的临床前数据支持使用分化疗法,但临床活性有限。髓系生长因子可在体外增强分化剂的抗白血病活性。我们开展了两项伴随的II期试验,研究沙格司亭(GM-CSF)125μg/m²/天加1)贝沙罗汀(BEX)300mg/m²/天或2)恩替诺特(ENT)4 - 8mg/m²/周用于骨髓增生异常综合征(MDS)或复发/难治性急性髓系白血病患者。主要终点是至少两个治疗周期后的反应和毒性。参加BEX试验的26例患者既往治疗的中位数为2次,参加ENT试验的24例患者既往治疗的中位数为1次。在接受BEX治疗的13例可评估反应的患者中,观察到的最佳反应是4例(31%)患者出现中性粒细胞血液学改善(HI-N);无患者达到完全缓解(CR)或部分缓解(PR)。在接受ENT治疗的10例患者中,有1例(10%)部分缓解(PR),2例(20%)出现HI-N。每种联合用药的HI-N次要终点反应均伴随绝对中性粒细胞计数(ANC)数值增加(BEX:524至931个细胞/mm³,p = 0.096;ENT:578至1137个细胞/mm³,p = 0.15),且未增加骨髓原始细胞。共同的3 - 4级非血液学毒性包括发热性中性粒细胞减少、骨痛、疲劳和呼吸困难。GM-CSF加BEX或ENT在耐药和难治性MDS和急性髓系白血病中耐受性良好,并显示出适度的临床和生物学活性,最常见的是HI-N。