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通过药敏试验和耐药分离株突变特征分析鉴定人胃内幽门螺杆菌异质性。

Evidence of Helicobacter pylori heterogeneity in human stomachs by susceptibility testing and characterization of mutations in drug-resistant isolates.

机构信息

Department of Medical Laboratory Sciences, Health, and Sciences, International University of Health and Welfare Graduate School, Chiba, Japan.

Kochi Medical School, Kochi Community Medical Support Center, Kochi, Japan.

出版信息

Sci Rep. 2024 May 27;14(1):12066. doi: 10.1038/s41598-024-62200-1.

Abstract

Heterogeneity of Helicobacter pylori communities contributes to its pathogenicity and diverse clinical outcomes. We conducted drug-susceptibility tests using four antibiotics, clarithromycin (CLR), amoxicillin (AMX), metronidazole and sitafloxacin, to examine H. pylori population diversity. We also analyzed genes associated with resistance to CLR and AMX. We examined multiple isolates from 42 Japanese patients, including 28 patients in whom primary eradication with CLR and AMX had failed, and 14 treatment-naïve patients. We identified some patients with coexistence of drug resistant- and sensitive-isolates (drug-heteroR/S-patients). More than 60% of patients were drug-heteroR/S to all four drugs, indicating extensive heterogeneity. For the four drugs except AMX, the rates of drug-heteroR/S-patients were higher in treatment-naïve patients than in primary eradication-failure patients. In primary eradication-failure patients, isolates multi-resistant to all four drugs existed among other isolates. In primary eradication-failure drug-heteroR/S-patients, CLR- and AMX-resistant isolates were preferentially distributed to the corpus and antrum with different minimum inhibitory concentrations, respectively. We found two mutations in PBP1A, G591K and A480V, and analyzed these in recombinants to directly demonstrate their association with AMX resistance. Assessment of multiple isolates from different stomach regions will improve accurate assessment of H. pylori colonization status in the stomach.

摘要

幽门螺杆菌群落的异质性与其致病性和多样化的临床结果有关。我们使用四种抗生素(克拉霉素 [CLR]、阿莫西林 [AMX]、甲硝唑和司他沙星)进行了药敏试验,以检查幽门螺杆菌种群的多样性。我们还分析了与 CLR 和 AMX 耐药相关的基因。我们检查了来自 42 名日本患者的多个分离株,包括 28 名首次接受 CLR 和 AMX 治疗失败的患者和 14 名未经治疗的患者。我们发现一些患者同时存在耐药和敏感分离株(药物异质性/R/S-患者)。超过 60%的患者对所有四种药物均为药物异质性/R/S,表明存在广泛的异质性。对于除 AMX 以外的四种药物,在未经治疗的患者中,药物异质性/R/S-患者的比例高于首次治疗失败的患者。在首次治疗失败的患者中,除其他分离株外,还存在对所有四种药物均耐药的分离株。在首次治疗失败的药物异质性/R/S-患者中,CLR 和 AMX 耐药分离株分别优先分布在具有不同最小抑菌浓度的胃体和胃窦。我们发现 PBP1A 中的两个突变,G591K 和 A480V,并在重组体中分析了这些突变,以直接证明它们与 AMX 耐药性有关。对来自不同胃区的多个分离株进行评估将提高对胃内幽门螺杆菌定植状态的准确评估。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0c73/11130178/25a9893eab98/41598_2024_62200_Fig1_HTML.jpg

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