基因分型
伊立替康
连锁不平衡
基因型
人口
生物
塔克曼
SNP基因分型
遗传学
单核苷酸多态性
医学
聚合酶链反应
癌症
结直肠癌
基因
环境卫生
作者
Adrián Bravo-Gómez,Sara Salvador‐Martín,Paula Zapata-Cobo,María Sanjurjo‐Sáez,Luis A. López‐Fernández
出处
期刊:Pharmaceutics
[Multidisciplinary Digital Publishing Institute]
日期:2022-09-29
卷期号:14 (10): 2082-2082
被引量:9
标识
DOI:10.3390/pharmaceutics14102082
摘要
The variant rs34983651 (UGT1A1*28) and its genotyping are used to prevent irinotecan-induced toxicity. Several variants are in close linkage disequilibrium. Our objective was to evaluate the potential correlation of genotyping UGT1A1*80 instead of UGT1A1*28 in different populations.We studied SNPs in linkage disequilibrium with UGT1A1*28 in several populations and selected rs887829 to develop an inexpensive and rapid genotyping method and compare it with the one we currently use for UGT1A1*28 genotyping. Samples from cancer patients (n = 701) already tested using PCR and electrophoresis prior to treatment with irinotecan for rs34983651 (UGT1A1*28) in a Spanish hospital were genotyped for rs887829 (UGT1A1*80) using real-time PCR with a TaqMan probe.We observed a complete match for both genotypes, except in one sample. This method was 100% efficient in correctly genotyping *28/*28 patients, 99.68% efficient for *1/*28, and 100% efficient for *1/*1. Linkage disequilibrium between populations showed the Iberian population to be the most suitable for the clinical use of UGT1A1*80. This method is less expensive and the time to decision is shorter.Genotyping of rs887829 using the proposed method may be used to substitute genotyping of rs34983651 as a pharmacogenetics test in cancer patients prior to starting irinotecan-based treatments, mainly in the Iberian population. In addition, it is less expensive than other conventional methods and easy to implement, with a shorter time to decision than UGT1A1*28.
科研通智能强力驱动
Strongly Powered by AbleSci AI