Relling M V, Ayers D, Heideman R L
Pharmaceutical Division, St Jude Children's Research Hospital, Memphis, TN 38105.
Pharmacogenetics. 1991 Oct;1(1):42-9. doi: 10.1097/00008571-199110000-00007.
Mephenytoin is the prototype substrate for the genetically regulated, polymorphically distributed cytochrome P450, mephenytoin hydroxylase. Mephenytoin is an anticonvulsant which has been associated with leukopenia when used chronically. The haematologic effects of a single dose of oral mephenytoin, as is typically used to determine drug metabolism phenotype for this polymorphism, have not been reported. We administered 100 mg oral racemic mephenytoin to 30 healthy male volunteers and measured complete blood count three times weekly for 23 days. The time dependency of the urinary ratio of S to R mephenytoin in five serial urine samples (0-4, 4-8, 8-16, 16-24 and 24-32 h after the dose) was evaluated. There were no significant decreases from baseline in any subject in leukocyte count, haematocrit or platelet count. Two of the 30 subjects both of Indian extraction, were poor metabolizers of mephenytoin. The S:R ratio decreased with time (p = 0.001). Using the 0-4 h urine, one subject would have been misphenotyped as a poor metabolizer; phenotype assignments were in agreement with each other based on all subsequent urine collections. We conclude that there is no evidence that single dose mephenytoin is associated with haematologic toxicity in healthy male volunteers, and that the 4-8 h post-dose urine is as reliable as the 24-32 h collection for assignment of phenotype.
美芬妥英是由基因调控、呈多态性分布的细胞色素P450(美芬妥英羟化酶)的原型底物。美芬妥英是一种抗惊厥药,长期使用时与白细胞减少有关。单次口服美芬妥英(通常用于确定该多态性的药物代谢表型)的血液学效应尚未见报道。我们给30名健康男性志愿者口服100mg消旋美芬妥英,并在23天内每周三次测量全血细胞计数。评估了五个连续尿液样本(给药后0 - 4、4 - 8、8 - 16、16 - 24和24 - 32小时)中美芬妥英S型与R型尿排泄率的时间依赖性。所有受试者的白细胞计数、血细胞比容或血小板计数均未出现相对于基线的显著下降。30名受试者中有两名均为印度裔,是美芬妥英的慢代谢者。S:R比值随时间下降(p = 0.001)。使用给药后0 - 4小时的尿液,一名受试者会被误判为慢代谢者;基于所有后续尿液收集结果,表型判定相互一致。我们得出结论,没有证据表明单次剂量的美芬妥英会对健康男性志愿者产生血液学毒性,并且给药后4 - 8小时的尿液与24 - 32小时收集的尿液在表型判定方面同样可靠。
