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抗癌药物 I 期临床试验中肌酸激酶与皮肤毒性的关系。

Association of creatine kinase and skin toxicity in phase I trials of anticancer agents.

机构信息

Drug Development Unit, Division of Cancer Therapeutics and Division of Clinical Studies, The Institute of Cancer Research, 15 Cotswold Road, Sutton SM2 5NG, UK.

出版信息

Br J Cancer. 2012 Nov 20;107(11):1797-800. doi: 10.1038/bjc.2012.482. Epub 2012 Oct 25.

Abstract

BACKGROUND

We investigated the association between skin rash and plasma creatine kinase (CK) levels in oncology phase I trials.

METHODS

We analysed data from 295 patients treated at our institution within 25 phase I trials which included CK measurements in the protocol. Trials involved drugs targeting EGFR/HER2, m-TOR, VEGFR, SRC/ABL, aurora kinase, BRAF/MEK, PARP, CDK, A5B1 integrin, as well as oncolytic viruses and vascular disrupting agents.

RESULTS

Creatine kinase measurements were available for 278 patients. The highest levels of plasma CK during the trial were seen among patients with Grade (G) 2/3 rash (median 249 U l(-1)) compared with G1 (median 81 U l(-1)) and no rash (median 55 U l(-1)) (P<0.001). There was a significant reduction in CK after the rash resolved (mean 264.2 vs 100.1; P=0.012) in 25 patients, where serial CK values were available. In vitro exposure of human keratinocytes to EGFR, MEK and a PI3Kinase/m-TOR inhibitor led to the increased expression of CK-brain and not CK-muscle or mitochondrial-CK.

CONCLUSION

Plasma CK elevation is associated with development of skin rash caused by novel anticancer agents. This should be studied further to characterise different isoforms as this will change the way we report adverse events in oncology phase I clinical trials.

摘要

背景

我们研究了肿瘤 I 期试验中皮疹与血浆肌酸激酶(CK)水平之间的关系。

方法

我们分析了在我们机构内进行的 25 项 I 期试验中 295 例患者的数据,这些试验的方案中包括 CK 测量。试验涉及针对 EGFR/HER2、m-TOR、VEGFR、SRC/ABL、极光激酶、BRAF/MEK、PARP、CDK、A5B1 整合素、溶瘤病毒和血管破坏剂的药物。

结果

278 例患者的 CK 测量值可用。在试验过程中,出现 G2/3 级皮疹的患者(中位值 249 U·l(-1)) 的血浆 CK 水平最高,而 G1 级皮疹患者(中位值 81 U·l(-1)) 和无皮疹患者(中位值 55 U·l(-1)) 的 CK 水平显著升高(P<0.001)。在 25 例可获得连续 CK 值的患者中,皮疹消退后 CK 显著降低(平均 264.2 比 100.1;P=0.012)。体外暴露于 EGFR、MEK 和 PI3K/m-TOR 抑制剂的人角质形成细胞导致 CK-脑而不是 CK-肌肉或线粒体-CK 的表达增加。

结论

新型抗癌药物引起的皮疹与血浆 CK 升高有关。应进一步研究这一点,以确定不同的同工酶,因为这将改变我们在肿瘤 I 期临床试验中报告不良事件的方式。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cf67/3504946/2607e11871be/bjc2012482f1.jpg

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