Technical University of Denmark, National Food Institute, European Union Reference Laboratory for Antimicrobial Resistance, WHO Collaborating Centre for Antimicrobial Resistance in Foodborne Pathogens and Genomics, FAO Reference Laboratory for Antimicrobial Resistance, Kgs. Lyngby, Denmark.
Université de Paris, IAME, INSERM, Paris, France.
J Antimicrob Chemother. 2020 Dec 1;75(12):3491-3500. doi: 10.1093/jac/dkaa345.
WGS-based antimicrobial susceptibility testing (AST) is as reliable as phenotypic AST for several antimicrobial/bacterial species combinations. However, routine use of WGS-based AST is hindered by the need for bioinformatics skills and knowledge of antimicrobial resistance (AMR) determinants to operate the vast majority of tools developed to date. By leveraging on ResFinder and PointFinder, two freely accessible tools that can also assist users without bioinformatics skills, we aimed at increasing their speed and providing an easily interpretable antibiogram as output.
The ResFinder code was re-written to process raw reads and use Kmer-based alignment. The existing ResFinder and PointFinder databases were revised and expanded. Additional databases were developed including a genotype-to-phenotype key associating each AMR determinant with a phenotype at the antimicrobial compound level, and species-specific panels for in silico antibiograms. ResFinder 4.0 was validated using Escherichia coli (n = 584), Salmonella spp. (n = 1081), Campylobacter jejuni (n = 239), Enterococcus faecium (n = 106), Enterococcus faecalis (n = 50) and Staphylococcus aureus (n = 163) exhibiting different AST profiles, and from different human and animal sources and geographical origins.
Genotype-phenotype concordance was ≥95% for 46/51 and 25/32 of the antimicrobial/species combinations evaluated for Gram-negative and Gram-positive bacteria, respectively. When genotype-phenotype concordance was <95%, discrepancies were mainly linked to criteria for interpretation of phenotypic tests and suboptimal sequence quality, and not to ResFinder 4.0 performance.
WGS-based AST using ResFinder 4.0 provides in silico antibiograms as reliable as those obtained by phenotypic AST at least for the bacterial species/antimicrobial agents of major public health relevance considered.
基于 WGS 的抗菌药物敏感性测试(AST)对于几种抗菌药物/细菌组合的可靠性与表型 AST 相当。然而,由于需要具备生物信息学技能和抗菌药物耐药性(AMR)决定因素的知识来操作迄今为止开发的绝大多数工具,因此常规使用基于 WGS 的 AST 受到了阻碍。通过利用 ResFinder 和 PointFinder 这两个免费的工具,我们旨在提高它们的速度,并提供一个易于解释的抗生素谱作为输出,而无需生物信息学技能。
重写 ResFinder 代码以处理原始读数并使用基于 Kmer 的比对。修订和扩展了现有的 ResFinder 和 PointFinder 数据库。还开发了其他数据库,包括将每个 AMR 决定因素与抗菌化合物水平的表型相关联的基因型-表型键,以及用于计算抗生素谱的种特异性面板。使用具有不同 AST 谱的大肠杆菌(n=584)、沙门氏菌(n=1081)、空肠弯曲菌(n=239)、屎肠球菌(n=106)、屎肠球菌(n=50)和金黄色葡萄球菌(n=163)验证了 ResFinder 4.0,这些菌株来自不同的人类和动物来源和地理起源。
对于革兰氏阴性和革兰氏阳性细菌,分别有 46/51 和 25/32 种抗菌药物/细菌组合的基因型-表型一致性≥95%。当基因型-表型一致性<95%时,差异主要与表型测试解释标准和次优序列质量有关,而与 ResFinder 4.0 的性能无关。
使用 ResFinder 4.0 进行基于 WGS 的 AST 提供了与表型 AST 至少在主要公共卫生相关的细菌/抗菌药物方面一样可靠的计算抗生素谱。
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