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首页> 外文期刊>Neuro-Oncology >Pharmacokinetics, safety, and tolerability of olaparib and temozolomide for recurrent glioblastoma: results of the phase Ⅰ OPARATIC trial
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Pharmacokinetics, safety, and tolerability of olaparib and temozolomide for recurrent glioblastoma: results of the phase Ⅰ OPARATIC trial

机译:用于复发性胶质细胞瘤的药代动力学,安全性和替替唑胺的耐受性:Ⅰ阶段oMaratic试验的结果

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Background. The poly(ADP-ribose) polymerase (PARP) inhibitor olaparib potentiated radiation and temozolomide (TMZ) chemotherapy in preclinical glioblastoma models but brain penetration was poor. Clinically, PARP inhibitors exacerbate the hematological side effects of TMZ. The OPARATIC trial was conducted to measure penetration of recurrent glioblastoma by olaparib and assess the safety and tolerability of its combination with TMZ.Methods. Preclinical pharmacokinetic studies evaluated olaparib tissue distribution in rats and tumor-bearing mice. Adult patients with recurrent glioblastoma received various doses and schedules of olaparib and low-dose TMZ in a 3 + 3 design. Suitable patients received olaparib prior to neurosurgical resection; olaparib concentrations in plasma, tumor core and tumor margin specimens were measured by mass spectrometry. A dose expansion cohort tested tolerability and efficacy of the recommended phase II dose (RP2D). Radiosensitizing effects of olaparib were measured by clonogenic survival in glioblastoma cell lines.Results. Olaparib was a substrate for multidrug resistance protein 1 and showed no brain penetration in rats but was detected in orthotopic glioblastoma xenografts. Clinically, olaparib was detected in 71/71 tumor core specimens (27 patients; median, 496 nM) and 21/21 tumor margin specimens (9 patients; median, 512.3 nM). Olaparib exacerbated TMZ-related hematological toxicity, necessitating intermittent dosing. RP2D was olaparib 150 mg (3 days/week) with TMZ 75 mg/m2 daily for 42 days. Fourteen (36%) of 39 evaluable patients were progression free at 6 months. Olaparib radiosensitized 6 glioblastoma cell lines at clinically relevant concentrations of 100 and 500 nM.Conclusion. Olaparib reliably penetrates recurrent glioblastoma at radiosensitizing concentrations, supporting further clinical development and highlighting the need for better preclinical models.
机译:背景。聚(ADP-核糖)聚合酶(PARP)抑制剂Olaparib促进辐射和替替莫唑胺(TMZ)化疗呈临床前胶质母细胞瘤模型,但脑渗透差。临床上,PARP抑制剂加剧了TMZ的血液副作用。进行了Olaparib的渗透胶质母细胞瘤的渗透,并评估其与TMZ.Methods的安全性和耐受性的渗透。临床前药代动力学研究评估了大鼠和肿瘤小鼠的奥拉帕里布组织分布。成年患者在3 + 3设计中接受了奥拉帕里布和低剂量TMZ的各种剂量和时间表。合适的患者在神经外切除之前接受奥拉帕布;通过质谱法测量血浆,肿瘤核心和肿瘤缘标本中的奥拉帕里布浓度。剂量膨胀队列测试的耐受性和推荐的第二阶段剂量(RP2D)的疗效。通过胶质母细胞瘤细胞系中的克隆灭性存活来测量olaparib的辐射敏化作用。结果。 Olaparib是用于多药抗性蛋白1的底物,并且在大鼠中没有显示出脑渗透,但在原位胶质母细胞瘤异种移植物中检测到。临床上,在71/71肿瘤核心标本(27例患者,496nm)和21/21肿瘤边缘标本(9例患者中,中位数,512.3nm)中检测到奥拉帕里布。奥拉帕里布与TMZ相关的血液毒性,需要间歇计量剂。 RP2D是Olaparib 150毫克(3天/周),每日TMZ 75 mg / m2为42天。 39名可评估患者的39名(36%)在6个月内自由进展。奥拉帕里布在临床相关浓度为100和500nm的临床相关浓度的辐射敏化瘤细胞系。结论。奥拉帕里布可靠地穿透辐射敏化浓度的复发胶质母细胞瘤,支持进一步的临床开发,并突出需要更好的临床前模型。

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