Aiken Robert, Axelson Magnus, Harmenberg Johan, Klockare Maria, Larsson Olle, Wassberg Cecilia
Rutgers-Cancer Institute of New Jersey, New Brunswick, NJ, U.S.A.
Clinical Chemistry, Department of Molecular Medicine and Surgery, Karolinska University Hospital and Karolinska Institutet, Stockholm, Sweden.
Oncotarget. 2017 Sep 6;8(46):81501-81510. doi: 10.18632/oncotarget.20662. eCollection 2017 Oct 6.
Early phase I study of safety of AXL1717 in patients with recurrent or progressive malignant astrocytomas and evaluation of preliminary anti-tumor efficacy.
Nine patients fulfilling the set criteria were enrolled. Eight had recurrent glioblastoma and one gliosarcoma. Patients were treated with an oral suspension of AXL1717 (215-400 mg bid) cycle-by-cycle in 35-day cycles (28 days bid and 7 days off). Patients with progressive disease and/or toxicity-related dose delay of more than 14 days were withdrawn.
Four patients had tumor responses (44%) to AXL1717 treatment. Two of these had stable disease for 12 months (10 cycles at 215-300 mg bid). Due to MRI-detected progression they were then taken off the study. They died 8 and 12 months later, respectively. One patient was treated 8 months (6 cycles with 215 mg bid). He was withdrawn because of disease progression but died after another 25 months. The fourth patient having stable disease died of sepsis due to pancytopenia in the end of cycle 2 on 400 mg bid. A fifth patient underwent surgery after two cycles with 300 mg bid. Pathological analysis demonstrated abundant necrosis and small areas of viable tumor. After one more cycle with 300 mg bid he was withdrawn due to clinical and radiographic worsening and died 11 months later. The other 4 patients did not have any detectable responses and died within 3-13 months after trial entry. Neutropenia was the main adverse effect, which was easily detected and reversible in all but one patient.
This clinical phase I study indicates that AXL1717 as a single agent is capable of producing prolonged stable disease and survival of patients with relapsed malignant astrocytomas. The drug was well tolerated. A new formulation of the drug will be used in further investigations in order to better define the optimal dose.
对AXL1717在复发性或进展性恶性星形细胞瘤患者中的安全性进行I期早期研究,并评估其初步抗肿瘤疗效。
招募了9名符合既定标准的患者。其中8例为复发性胶质母细胞瘤,1例为胶质肉瘤。患者接受AXL1717口服混悬液(215 - 400mg,每日两次)治疗,每35天为一个周期(连续28天每日两次用药,停药7天)。疾病进展和/或毒性相关剂量延迟超过14天的患者退出研究。
4例患者对AXL1717治疗有肿瘤反应(44%)。其中2例疾病稳定达12个月(215 - 300mg,每日两次,共10个周期)。由于MRI检测到疾病进展,随后他们退出研究,分别在8个月和12个月后死亡。1例患者接受治疗8个月(215mg,每日两次,共6个周期)。因疾病进展退出研究,但在另外25个月后死亡。第4例疾病稳定的患者在第2周期结束时,每日两次服用400mg时因全血细胞减少导致败血症死亡。第5例患者在每日两次服用300mg,两个周期后接受了手术。病理分析显示有大量坏死和小面积存活肿瘤。在再进行一个每日两次服用300mg的周期后,因临床和影像学恶化退出研究,11个月后死亡。其他4例患者未出现任何可检测到的反应,在进入试验后3 - 13个月内死亡。中性粒细胞减少是主要不良反应,除1例患者外,在所有患者中均易于检测且可逆。
这项I期临床研究表明,AXL1717作为单一药物能够使复发性恶性星形细胞瘤患者产生长期疾病稳定并延长生存期。该药物耐受性良好。为了更好地确定最佳剂量,将在进一步研究中使用该药物的新制剂。
