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本文引用的文献

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Drug development: portals of discovery.药物研发:探索的门户。
Clin Cancer Res. 2012 Jan 1;18(1):23-32. doi: 10.1158/1078-0432.CCR-11-1001.
2
A sensitive and selective liquid chromatography/tandem mass spectrometry method for determination of MLN8237 in human plasma.一种用于测定人血浆中 MLN8237 的灵敏且选择性的液相色谱/串联质谱法。
J Chromatogr B Analyt Technol Biomed Life Sci. 2010 Sep 1;878(25):2369-73. doi: 10.1016/j.jchromb.2010.06.037. Epub 2010 Jul 3.
3
Aurora kinase A promotes ovarian tumorigenesis through dysregulation of the cell cycle and suppression of BRCA2.极光激酶 A 通过调控细胞周期和抑制 BRCA2 促进卵巢肿瘤发生。
Clin Cancer Res. 2010 Jun 15;16(12):3171-81. doi: 10.1158/1078-0432.CCR-09-3171. Epub 2010 Apr 27.
4
Initial testing of the aurora kinase A inhibitor MLN8237 by the Pediatric Preclinical Testing Program (PPTP).儿科临床前试验计划(PPTP)对极光激酶 A 抑制剂 MLN8237 的初步测试。
Pediatr Blood Cancer. 2010 Jul 15;55(1):26-34. doi: 10.1002/pbc.22430.
5
Stabilization of N-Myc is a critical function of Aurora A in human neuroblastoma.N-Myc的稳定是极光激酶A在人类神经母细胞瘤中的关键功能。
Cancer Cell. 2009 Jan 6;15(1):67-78. doi: 10.1016/j.ccr.2008.12.005.
6
Polo-like kinase-1 is activated by aurora A to promote checkpoint recovery.Polo样激酶-1由极光激酶A激活,以促进检查点恢复。
Nature. 2008 Sep 4;455(7209):119-23. doi: 10.1038/nature07185. Epub 2008 Jul 9.
7
Aurora kinase family: a new target for anticancer drug.极光激酶家族:抗癌药物的新靶点。
Recent Pat Anticancer Drug Discov. 2008 Jun;3(2):114-22. doi: 10.2174/157489208784638785.
8
Aurora kinases as anticancer drug targets.极光激酶作为抗癌药物靶点。
Clin Cancer Res. 2008 Mar 15;14(6):1639-48. doi: 10.1158/1078-0432.CCR-07-2179.
9
Targeted disruption of Aurora A causes abnormal mitotic spindle assembly, chromosome misalignment and embryonic lethality.极光激酶A的靶向破坏会导致有丝分裂纺锤体组装异常、染色体排列紊乱以及胚胎致死。
Oncogene. 2008 Jul 3;27(29):4122-7. doi: 10.1038/onc.2008.47. Epub 2008 Mar 17.
10
Shortening the timeline of pediatric phase I trials: the rolling six design.缩短儿科I期试验的时间线:滚动六设计。
J Clin Oncol. 2008 Jan 10;26(2):190-5. doi: 10.1200/JCO.2007.12.7712.

儿童肿瘤组 I 期联盟研究:一种研究性口服 Aurora 激酶 A 选择性小分子抑制剂 MLN8237 的儿科 I 期试验和药代动力学研究。

Pediatric phase I trial and pharmacokinetic study of MLN8237, an investigational oral selective small-molecule inhibitor of Aurora kinase A: a Children's Oncology Group Phase I Consortium study.

机构信息

Division of Oncology and Center for Childhood Cancer Research, Children's Hospital of Philadelphia, Department of Pediatrics, Perelman School of Medicine at the University of Pennsylvania, Philadelphia, Pennsylvania 19104, USA.

出版信息

Clin Cancer Res. 2012 Nov 1;18(21):6058-64. doi: 10.1158/1078-0432.CCR-11-3251. Epub 2012 Sep 17.

DOI:10.1158/1078-0432.CCR-11-3251
PMID:22988055
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4008248/
Abstract

PURPOSE

MLN8237, a selective small-molecule inhibitor of Aurora kinase A, has activity in a broad range of preclinical pediatric cancer models. We conducted a phase I trial in children with refractory/recurrent solid tumors to define the maximum-tolerated dose, toxicities, and pharmacokinetic properties of MLN8237.

EXPERIMENTAL DESIGN

MLN8237 was administered orally either once daily or divided twice daily for seven days, every 21 days. Using a rolling-six design, four dose levels (45, 60, 80, and 100 mg/m(2)/day) were evaluated on the once-daily schedule, and two dose levels (60 and 80 mg/m(2)/d) on the twice-daily schedule. Pharmacokinetic studies were conducted with the initial dose and trough drug concentrations also measured at the steady state.

RESULTS

Thirty-seven patients were enrolled. On the once-daily dosing schedule, myelosuppression was dose limiting in three of four patients at 100 mg/m(2), and one of six patients had dose-limiting mood alteration at 80 mg/m(2). At 45 mg/m(2), one of six patients experienced dose-limiting mucositis. Mucositis and myelosuppression were dose limiting at 80 mg/m(2) on the twice-daily schedule, and one of five patients at 60 mg/m(2) on the twice-daily schedule experienced a dose-limiting alkaline phosphatase. Five of 11 patients experienced hand-foot-skin syndrome with twice-daily dosing versus one of 21 after once-daily dosing. There was one partial response and six with prolonged stable disease among 33 evaluable subjects.

CONCLUSION

The twice-daily dose regimen is well tolerated in adults; however, children experienced a greater frequency of myelosuppression and hand-foot-skin syndrome on this schedule. Children tolerated a higher dose and the recommended pediatric phase II dose is 80 mg/m(2)/d once daily for seven days.

摘要

目的

MLN8237 是一种选择性的小分子 Aurora 激酶 A 抑制剂,在广泛的儿科癌症模型中具有活性。我们在患有难治性/复发性实体瘤的儿童中进行了一项 I 期试验,以确定 MLN8237 的最大耐受剂量、毒性和药代动力学特性。

实验设计

MLN8237 以口服方式给药,每日一次或每日两次分两次给药,连续 7 天,每 21 天一次。采用滚动六设计,在每日一次给药方案中评估了四个剂量水平(45、60、80 和 100mg/m2/天),在每日两次给药方案中评估了两个剂量水平(60 和 80mg/m2/d)。在初始剂量和稳态时还进行了药代动力学研究,测量了药物浓度的谷值。

结果

共纳入 37 例患者。在每日一次给药方案中,100mg/m2 时有 3/4 例患者出现骨髓抑制,80mg/m2 时有 1/6 例患者出现剂量限制的情绪改变。在 45mg/m2 时,1/6 例患者出现剂量限制的粘膜炎。在每日两次给药方案中,80mg/m2 时有粘膜炎和骨髓抑制,60mg/m2 时有 1/5 例患者出现剂量限制的碱性磷酸酶。与每日一次给药相比,每日两次给药时有 5/11 例患者出现手足皮肤综合征,而每日一次给药时有 1/21 例患者出现手足皮肤综合征。在 33 例可评价患者中,有 1 例部分缓解,6 例病情稳定延长。

结论

在成人中,每日两次给药方案耐受性良好;然而,儿童在该方案中出现骨髓抑制和手足皮肤综合征的频率更高。儿童耐受更高的剂量,推荐的儿科 II 期剂量为每日一次 80mg/m2/d,连续 7 天。