1st Department of Internal Medicine, Lung Cancer Group Cologne, Germany.
Clin Pharmacokinet. 2011 Jun;50(6):371-403. doi: 10.2165/11587020-000000000-00000.
The 4-anilinoquinazolines (gefitinib, erlotinib and lapatinib) are members of a class of potent and selective inhibitors of the human epidermal growth factor receptor (HER) family of tyrosine kinases that have been developed to treat patients with tumours with defined genetic alterations of the HER tyrosine kinase domain. They are characterized by a moderate rate of absorption after oral administration with peak plasma concentrations at several hours post-dose. Absolute bioavailability of gefitinib and erlotinib is about 60%. Low bioavailability is assumed for lapatinib. The drugs are extensively distributed in human tissues, including tumour tissues, have a large volume of distribution at least 3-fold exceeding the volume of body water and are extensively (about 95%) protein bound to α(1)-acid glycoprotein and albumin. Existing human data for gefitinib and erlotinib indicate that these substances penetrate into the central nervous system and accumulate in brain tumours, possibly due to leaks in the blood-brain barrier. Gefitinib, erlotinib and the absorbed fraction of lapatinib undergo extensive metabolism - mainly via hepatic and intestinal cytochrome P450 (CYP) 3A4 and also via CYP2D6 (gefitinib) and CYP1A2 (erlotinib) - and are primarily eliminated by biotransformation. The excretion of unchanged gefitinib, erlotinib, lapatinib and their metabolites occurs predominantly in the faeces and only a minor fraction is excreted in the urine. No relevant effects of age, sex, bodyweight or race on their pharmacokinetics have been reported to date. Limited available data indicate that genetic polymorphisms in enzymes and transporters involved in the pharmacokinetics of gefitinib (CYP2D6) and erlotinib (CYP3A4, CYP3A5 and ABCG2 [breast cancer resistance protein]) alter the exposure to these drugs. Modification of drug dose should be considered in patients with severe hepatic impairment receiving these tyrosine kinase inhibitors and in current smokers receiving erlotinib. Existing recommendations for dose adjustment (i.e. a dose decrement or increment for gefitinib, erlotinib and lapatinib in the presence of CYP3A4 inhibitors or inducers, respectively; a dose increase for erlotinib in smoking patients) need to be validated in clinical studies. Further investigations are required to explain the large interindividual variability in the pharmacokinetics of these drugs and to assess the clinical relevance of interaction potential and inhibitory effects on the metabolizing enzymes and transporters.
4-苯胺基喹唑啉(吉非替尼、厄洛替尼和拉帕替尼)是一类强效和选择性的人表皮生长因子受体(HER)家族酪氨酸激酶抑制剂,已被开发用于治疗具有 HER 酪氨酸激酶结构域明确遗传改变的肿瘤患者。这些药物的特点是口服吸收速度适中,给药后数小时达到血浆峰浓度。吉非替尼和厄洛替尼的绝对生物利用度约为 60%。拉帕替尼的生物利用度较低。这些药物广泛分布于人体组织,包括肿瘤组织,分布容积至少是人体水容积的 3 倍,与 α(1)-酸性糖蛋白和白蛋白广泛(约 95%)结合。现有的关于吉非替尼和厄洛替尼的人体数据表明,这些物质能够穿透血脑屏障进入中枢神经系统并在脑肿瘤中蓄积,这可能是由于血脑屏障的渗漏。吉非替尼、厄洛替尼和拉帕替尼的吸收部分主要通过肝和肠道细胞色素 P450(CYP)3A4 代谢,也通过 CYP2D6(吉非替尼)和 CYP1A2(厄洛替尼)代谢,并主要通过生物转化消除。未改变的吉非替尼、厄洛替尼、拉帕替尼及其代谢物主要通过粪便排泄,仅有少量通过尿液排泄。迄今为止,尚未报道年龄、性别、体重或种族对其药代动力学的相关影响。有限的可用数据表明,参与吉非替尼(CYP2D6)和厄洛替尼(CYP3A4、CYP3A5 和 ABCG2[乳腺癌耐药蛋白])药代动力学的酶和转运体的遗传多态性改变了这些药物的暴露量。接受这些酪氨酸激酶抑制剂治疗的严重肝损伤患者和接受厄洛替尼治疗的现吸烟者应考虑调整药物剂量。对于 CYP3A4 抑制剂或诱导剂存在时吉非替尼、厄洛替尼和拉帕替尼的剂量调整(即剂量减少或增加)以及吸烟患者厄洛替尼的剂量增加的现有建议需要在临床研究中验证。需要进一步研究来解释这些药物药代动力学的个体间差异很大的原因,并评估相互作用的潜力和对代谢酶和转运体的抑制作用的临床相关性。
