Cooper Todd M, Sison Edward Allan Racela, Baker Sharyn D, Li Lie, Ahmed Amina, Trippett Tanya, Gore Lia, Macy Margaret E, Narendran Aru, August Keith, Absalon Michael J, Boklan Jessica, Pollard Jessica, Magoon Daniel, Brown Patrick A
Seattle Children's Cancer and Blood Disorders Center, University of Washington, Seattle, Washington.
Texas Children's Cancer and Hematology Centers, Baylor College of Medicine, Houston, Texas.
Pediatr Blood Cancer. 2017 Aug;64(8). doi: 10.1002/pbc.26414. Epub 2017 Apr 14.
Plerixafor, a reversible CXCR4 antagonist, inhibits interactions between leukemic blasts and the bone marrow stromal microenvironment and may enhance chemosensitivity. A phase 1 trial of plerixafor in combination with intensive chemotherapy in children and young adults with relapsed or refractory acute lymphoblastic leukemia (ALL), acute myeloid leukemia (AML), and myelodysplastic syndrome (MDS) was performed to determine a tolerable and biologically active dose.
Plerixafor was administered daily for 5 days at four dose levels (6, 9, 12, and 15 mg/m /dose) followed 4 hr later by high-dose cytarabine (every 12 hr) and etoposide (daily).
Nineteen patients (13 with AML, 5 with ALL, 1 with MDS) were treated. The most common grade 3 or greater nonhematologic toxicities attributable to plerixafor were febrile neutropenia and hypokalemia. There were no dose-limiting toxicities (DLTs). Plerixafor exposure increased with increasing dose levels and clearance was similar on days 1 and 5. Eighteen patients were evaluable for response. Two patients achieved complete remission (CR) and one patient achieved CR with incomplete hematologic recovery (CRi): all three had AML. No responses were seen in patients with ALL or MDS. Plerixafor mobilized leukemic blasts into the peripheral blood in 14 of 16 evaluable patients (median 3.4-fold increase), and the degree of mobilization correlated with surface CXCR4 expression.
Plerixafor, in combination with high-dose cytarabine and etoposide, was well tolerated in children and young adults with relapsed/refractory acute leukemias and MDS. While biologic responses were observed, clinical responses in this heavily pretreated cohort were modest.
普乐沙福是一种可逆的CXCR4拮抗剂,可抑制白血病原始细胞与骨髓基质微环境之间的相互作用,并可能增强化疗敏感性。开展了一项普乐沙福联合强化化疗用于复发或难治性急性淋巴细胞白血病(ALL)、急性髓系白血病(AML)和骨髓增生异常综合征(MDS)儿童及年轻成人患者的1期试验,以确定可耐受且具有生物活性的剂量。
普乐沙福按四个剂量水平(6、9、12和15mg/m²/剂量)每日给药5天,4小时后给予大剂量阿糖胞苷(每12小时一次)和依托泊苷(每日一次)。
19例患者(13例AML、5例ALL、1例MDS)接受了治疗。普乐沙福所致最常见的3级或更高级别的非血液学毒性为发热性中性粒细胞减少和低钾血症。未出现剂量限制性毒性(DLT)。普乐沙福的暴露量随剂量水平增加而增加,第1天和第5天的清除率相似。18例患者可评估疗效。2例患者达到完全缓解(CR),1例患者达到血液学未完全恢复的CR(CRi):这3例均为AML。ALL或MDS患者未见缓解。16例可评估患者中有14例普乐沙福使白血病原始细胞动员至外周血(中位增加3.4倍),动员程度与表面CXCR4表达相关。
普乐沙福联合大剂量阿糖胞苷和依托泊苷在复发/难治性急性白血病和MDS儿童及年轻成人患者中耐受性良好。虽然观察到生物学反应,但在这个经过大量预处理的队列中临床反应有限。
