奥美拉唑与CYP2C19基因多态性:长期治疗对酸相关性疾病患者胃泌素、胃蛋白酶原I和嗜铬粒蛋白A的影响
Omeprazole and CYP2C19 polymorphism: effects of long-term treatment on gastrin, pepsinogen I, and chromogranin A in patients with acid related disorders.
作者信息
Sagar M, Bertilsson L, Stridsberg M, Kjellin A, Mârdh S, Seensalu R
机构信息
Center of Gastroenterology, Departments of Surgery and Medicine, Clinical Research Center, Sweden.
出版信息
Aliment Pharmacol Ther. 2000 Nov;14(11):1495-502. doi: 10.1046/j.1365-2036.2000.00835.x.
BACKGROUND
The polymorphic enzyme CYP2C19 is of importance for the metabolism and effects of omeprazole during short-term treatment.
AIM
To investigate the relationship between CYP2C19 genotype and the effects of long-term omeprazole treatment.
MATERIAL AND METHODS
A total of 180 patients with acid related disorders were genotyped for wild type and mutated CYP2C19 alleles by allele-specific PCR amplification. Gastrin and chromogranin A were assessed by radioimmunoassays, and pepsinogen I and H. pylori serology were assessed by ELISA methods.
RESULTS
In 108 of the patients, who received a single dose of 20 mg omeprazole, there was no difference in gastrin and chromogranin A concentrations between the three CYP2C19 genotypes. In 72 patients on long-term treatment (> 1 year) with 20 mg omeprazole daily, serum gastrin as well as plasma chromogranin A concentrations (mean +/- s.e.) were both about threefold higher in the wild type/mutated (52.1 +/- 7.6 pM and 7.3 +/- 1.3 nM (n=19), respectively) compared to wild type/wild type (14. 7 +/- 0.9 pM and 2.5 +/- 0.1 nM (n=52), respectively; both comparisons P=0.0001). In a single mutated/mutated patient on long-term treatment, both gastrin and chromogranin A were high (88 pM and 13.7 nM, respectively). Serum pepsinogen I concentration was significantly lower in wild type/mutated (n=19) patients on long-term treatment, compared with the corresponding wild type/wild type (n=49) group (147 +/- 19 microg/L vs. 193 +/- 12 microg/L, P=0. 04).
CONCLUSION
Patients with one (and probably also with two) mutated CYP2C19 allele(s) on long-term treatment with omeprazole had significantly affected serum gastrin and pepsinogen I and plasma chromogranin A concentrations compared with patients with two normal alleles. This indicates that changes in gastric mucosal morphology during omeprazole treatment might be dependent upon the degree of the individual's capacity to metabolize omeprazole.
背景
多态性酶CYP2C19在短期治疗期间对奥美拉唑的代谢及效应具有重要意义。
目的
研究CYP2C19基因型与长期奥美拉唑治疗效果之间的关系。
材料与方法
采用等位基因特异性PCR扩增技术,对180例酸相关性疾病患者的野生型和突变型CYP2C19等位基因进行基因分型。采用放射免疫分析法检测胃泌素和嗜铬粒蛋白A,采用ELISA法检测胃蛋白酶原I和幽门螺杆菌血清学。
结果
在108例接受单剂量20mg奥美拉唑治疗的患者中,三种CYP2C19基因型之间的胃泌素和嗜铬粒蛋白A浓度无差异。在72例每日接受20mg奥美拉唑长期治疗(>1年)的患者中,野生型/突变型患者(分别为52.1±7.6pM和7.3±1.3nM,n = 19)的血清胃泌素和血浆嗜铬粒蛋白A浓度(均值±标准误)均比野生型/野生型患者(分别为14.7±0.9pM和2.5±0.1nM,n = 52)高出约三倍(两组比较P = 0.0001)。在1例长期治疗的单突变型/突变型患者中,胃泌素和嗜铬粒蛋白A均升高(分别为88pM和13.7nM)。长期治疗的野生型/突变型患者(n = 19)的血清胃蛋白酶原I浓度显著低于相应的野生型/野生型患者(n = 49)组(147±19μg/L对193±12μg/L,P = 0.04)。
结论
与具有两个正常等位基因的患者相比,长期接受奥美拉唑治疗且携带一个(可能也携带两个)突变CYP2C19等位基因的患者,其血清胃泌素、胃蛋白酶原I和血浆嗜铬粒蛋白A浓度受到显著影响。这表明奥美拉唑治疗期间胃黏膜形态的变化可能取决于个体代谢奥美拉唑能力的程度。
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