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根据胃炎早期克拉霉素耐药 23S rRNA、rpl22 相关突变和 cyp2c19*1、*2、*3 基因模式评估幽门螺杆菌阳性感染患者。

Assessment of Helicobacter pylori positive infected patients according to Clarithromycin resistant 23S rRNA, rpl22 associated mutations and cyp2c19*1, *2, *3 genes pattern in the Early stage of Gastritis.

机构信息

Department of Bacteriology, Faculty of Medical Sciences, Tarbiat Modares University, Al-E Ahmad Exp., Tehran, Iran.

Foodborne and Waterborne Diseases Research Center, Research Institute for Gastroenterology and Liver Diseases, Shahid Beheshti University of Medical Sciences, Tehran, Iran.

出版信息

BMC Res Notes. 2022 Oct 25;15(1):335. doi: 10.1186/s13104-022-06227-5.

DOI:10.1186/s13104-022-06227-5
PMID:36284359
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9594930/
Abstract

OBJECTIVE

Clarithromycin resistant Helicobacter pylori (CAM-R) is the main cause of standard triple therapy eradicating failure. Proton pump inhibitors (PPIs) directly pose bacteriocidic activity and prepare the optimum condition for Clarithromycin's best function. In counter with Poor metabolizer subjects, Homozygote Extensive Metabolizers have well characterized by treatment failure. Eventually, determination of CAM-R profile and estimation of PPIs metabolization rate support clinicians in better prescription. So, we explored Helicobacter pylori'mutations in 23S rRNA and rpl22 resistant genes, and cyp2c19 *1, *2, *3 allele variations, and PPIs metabolization patterns in patients, consequently the results reported to the physician.

RESULTS

Sixteen out of 96 patients considered to be CAM-R Helicobacter pylori. A2143C (1/16), rpl22 insertion (16/16), and GTG deletion (2/16) recorded in CAM-R strains. P450 2C19 human genotyping demonstrated that the highest proportion of the H. pylori- positive strains infected patients 43/61(70.49%) categorized in Homozygote extensive metabolizer class. The rest (12/61)19.67% classified as Poor metabolizers, and 6/61(9.83%) distinct from Heterozygote extensive metabolizer group. Proportion of poor metabolizers and Heterozygote extensive metabolizer phenotypes between CAM-R strains mentioned to be 10/16(62.5%), and 6/16(37.5%). Cross points between the most frequently distributed allele in CAM-R strains indicated 81.25% for *2, and 2 for 18.75%.

摘要

目的

克拉霉素耐药幽门螺杆菌(CAM-R)是标准三联疗法根除失败的主要原因。质子泵抑制剂(PPIs)直接具有杀菌活性,并为克拉霉素的最佳功能准备最佳条件。与代谢不良者相比,纯合广泛代谢者的治疗失败特征明显。最终,确定 CAM-R 谱和估计 PPIs 代谢率有助于临床医生更好地处方。因此,我们探索了 23S rRNA 和 rpl22 耐药基因中的幽门螺杆菌突变,以及 CYP2C19 * 1、* 2、* 3等位基因变异和患者中的 PPIs 代谢模式,随后将结果报告给医生。

结果

在 96 名患者中,有 16 名被认为是 CAM-R 幽门螺杆菌。CAM-R 菌株中记录了 A2143C(1/16)、rpl22 插入(16/16)和 GTG 缺失(2/16)。P450 2C19 人类基因分型表明,最高比例的 H. pylori 阳性菌株感染患者 43/61(70.49%)归类为纯合广泛代谢者。其余(12/61)19.67%归类为代谢不良者,6/61(9.83%)与杂合广泛代谢者组不同。CAM-R 菌株中不良代谢者和杂合广泛代谢者表型的比例分别为 10/16(62.5%)和 6/16(37.5%)。CAM-R 菌株中最常见分布等位基因的交叉点表明,* 2为 81.25%,* 1 为 2%。

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