1370:一流的DRD2/ clpp靶向吡普利酮ONC201的ADME和毒理学分析

S. Morrow, R. Tarapore, A. Guo, Magdalena Nej, Yunlan Fang, Gina Theerman, Leah Lake, M. Stogniew, V. Prabhu, J. Allen
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引用次数: 0

摘要

Imipridone ONC201是一种一流的DRD2拮抗剂和ClpP激动剂,在H3 k27m突变胶质瘤患者中耐受性良好,每周给药一次,可诱导持久的肿瘤消退。我们评估了ONC201在动物体内的毒理学、吸收、分布、代谢和排泄。在大鼠和狗中每周口服ONC201的28天重复剂量研究显示,NOAELs(分别为75和60 mg/kg)比临床剂量625 mg/kg更高。遗传毒性(AMES,体外和体内微核试验)分析表明,ONC201在暴露于RP2D和患者平均Cmax 2 μ M以上时不具有致突变性。3T3神经红色摄取试验显示ONC201不是光毒素(光刺激因子1.1)。在胚胎发育研究中,ONC201在大鼠或家兔中未引起母性效应,在3/61只兔胎儿中(从妊娠7-17或19天开始)每日剂量分别为62.5和25 mg/kg,导致胎儿畸形。一剂量[14C]-ONC201对大鼠进行的定量全身放射自显影研究显示,在大多数组织中,组织分布迅速,在1h达到峰值,血浆终末半衰期为5.6h。内分泌、代谢/排泄、眼部和胃肠道组织中ONC201的分布最高[14C]。[14C]-ONC201均匀分布在CNS亚结构中,包括中线区域。与均匀分布一致,ONC201具有高通透性(23-31×10-6 cm/s, 7-700 μM),并不是Caco-2细胞外排转运体的底物(外排比0.46-0.79)。ONC201在200μM时对MDR1-和bcrp介导的转运有抑制作用。ONC201的临床试验限制了诱导或抑制CYP酶的合用药物的使用,但一些支持性药物可以影响这些酶。体外研究表明,ONC201不是7种主要人类CYP酶的诱导剂,但抑制CYP 2B6、2C8、2C9、2C19、2D6和3A4的底物(IC50 20-90µM)。地塞米松是一种已知的CYP3A4诱导剂,在H3 k27m突变胶质瘤患者(n=22)中,对地塞米松的分析未显示基线剂量水平与ONC201血浆浓度之间的相关性。人肝细胞的代谢分析显示,只有一种代谢物ONC207丰度>10%。ONC207在癌细胞活力和DRD2拮抗试验中未达到IC50。通过LC-MS/MS对onc201治疗的H3 k27m突变胶质瘤患者(n=20)的血浆样本进行分析,证实ONC207是主要代谢物。一剂量[14C]-ONC201对大鼠进行的物质平衡研究显示,主要的排泄途径是胆汁(61.18%),通过粪便(69.78%)排泄,尿液(24.99%)也有助于整体恢复。总之,这些数据为ONC201治疗晚期癌症患者提供了信息,这些患者通常需要一系列药物治疗和合并症。引文格式:Sara Morrow, Rohinton Tarapore, Ailan Guo, Magdalena Nej, Yunlan Fang, Gina Theerman, Leah Lake, Martin Stogniew, Varun V. Prabhu, Joshua E. Allen一流的DRD2/ clpp靶向吡普利酮ONC201的ADME和毒理学分析[摘要]。见:美国癌症研究协会2021年年会论文集;2021年4月10日至15日和5月17日至21日。费城(PA): AACR;癌症杂志,2021;81(13 -增刊):1370。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Abstract 1370: ADME and toxicology profiles of first-in-class DRD2/ClpP-targeted imipridone ONC201
Imipridone ONC201 is a first-in-class DRD2 antagonist and ClpP agonist that is well tolerated and induces durable tumor regressions in H3 K27M-mutant glioma patients with once weekly dosing. We evaluated the toxicology, absorption, distribution, metabolism and excretion of ONC201 in animals. Repeat-dose 28-day studies with weekly oral ONC201 in rats and dogs revealed NOAELs (75 and 60 mg/kg, respectively) that represent higher dose levels compared to the 625 mg clinical dose. Genotoxicity (AMES, in vitro and in vivo micronucleus assays) assays demonstrated that ONC201 is not mutagenic at exposures above the RP2D and 2µM average Cmax in patients. The 3T3 neural red uptake assay showed ONC201 is not a phototoxin (photo-irritant factor 1.1). In embryofetal development studies, ONC201 did not lead to maternal effects in rats or rabbits and caused fetal malformations in 3/61 rabbit fetuses with daily dosing (from gestation day 7-17 or 19) at 62.5 and 25 mg/kg, respectively. A quantitative whole-body autoradiography study conducted in rats with one dose of [14C]-ONC201 showed rapidly tissue distribution peaking at 1h in most tissues and exhibiting a plasma terminal half-life of 5.6h. The endocrine, metabolic/excretory, ocular and GI tract tissues contained the highest distribution of [14C]ONC201. [14C]-ONC201 was distributed evenly across CNS substructures, including the midline region. Consistent with the uniform distribution, ONC201 displayed high permeability (23-31×10-6 cm/s, 7-700 μM) and was not a substrate of efflux transporters in Caco-2 cells (efflux ratio 0.46-0.79). ONC201 exerted inhibitory potential on MDR1- and BCRP-mediated transport at 200μM. Clinical trials with ONC201 restrict use of concomitant medications that induce or inhibit CYP enzymes, but several supportive medications can affect these enzymes. In vitro studies revealed that ONC201 is not an inducer of 7 major human CYP enzymes but does inhibit and is a substrate of CYP 2B6, 2C8, 2C9, 2C19, 2D6 and 3A4 (IC50 20-90µM). Analysis of dexamethasone, a known inducer of CYP3A4, did not show a correlation between baseline dose level and ONC201 plasma concentrations in H3 K27M-mutant glioma patients (n=22). Metabolic profiling in human hepatocytes revealed only one metabolite, ONC207, that was >10% in abundance. ONC207 did not achieve an IC50 in cancer cell viability and DRD2 antagonism assays. Assaying by LC-MS/MS of plasma samples obtained from ONC201-treated H3 K27M-mutant glioma patients (n=20) confirmed the presence of ONC207 as the major metabolite. A mass balance study conducted in rats with one dose of [14C]-ONC201 showed that the main route of excretion was biliary (61.18%) via the feces (69.78%), with urine (24.99%) also contributing to overall recovery. Together, these data inform the administration of ONC201 to advanced cancer patients who often require a range of comedications and comorbidities. Citation Format: Sara Morrow, Rohinton Tarapore, Ailan Guo, Magdalena Nej, Yunlan Fang, Gina Theerman, Leah Lake, Martin Stogniew, Varun V. Prabhu, Joshua E. Allen. ADME and toxicology profiles of first-in-class DRD2/ClpP-targeted imipridone ONC201 [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2021; 2021 Apr 10-15 and May 17-21. Philadelphia (PA): AACR; Cancer Res 2021;81(13_Suppl):Abstract nr 1370.
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