Clostridioides difficile EF-Tu mutants conferring resistance to elfamycin

Accession ARO:3003357
CARD Short NameCdif_EFTu_ELF
DefinitionSequence variants of Clostridioides difficile elongation factor Tu that confer resistance to elfamycin antibiotics.
AMR Gene Familyelfamycin resistant EF-Tu
Drug Classelfamycin antibiotic
Resistance Mechanismantibiotic target alteration
Classification10 ontology terms | Show
Parent Term(s)3 ontology terms | Show
+ derives_from elongation factor Tu
+ elfamycin resistant EF-Tu [AMR Gene Family]
+ confers_resistance_to_antibiotic LFF571 [Antibiotic]
Publications

Leeds JA, et al. 2012. Antimicrob Agents Chemother 56(8): 4463-4465. Mechanism of action of and mechanism of reduced susceptibility to the novel anti-Clostridium difficile compound LFF571. (PMID 22644023)

Resistomes

Prevalence of Clostridioides difficile EF-Tu mutants conferring resistance to elfamycin among the sequenced genomes, plasmids, and whole-genome shotgun assemblies available at NCBI or IslandViewer for 413 important pathogens (see methodological details and complete list of analyzed pathogens). Values reflect percentage of genomes, plasmids, genome islands, or whole-genome shotgun assemblies that have at least one hit to the AMR detection model. Default view includes percentages calculated based on Perfect plus Strict RGI hits. Select the checkbox to view percentages based on only Perfect matches to AMR reference sequences curated in CARD (note: this excludes resistance via mutation as references in protein variant models are often wild-type, sensitive sequences).

Prevalence: protein variant model

SpeciesNCBI ChromosomeNCBI PlasmidNCBI WGSNCBI GI
No prevalence data


Detection Models

Model Type: protein variant model

Model Definition: Protein Variant Models (PVM) perform a similar search as Protein Homolog Models (PHM), i.e. detect protein sequences based on their similarity to a curated reference sequence, but secondarily screen query sequences for curated sets of mutations to differentiate them from antibiotic susceptible wild-type alleles. PVMs are designed to detect AMR acquired via mutation of house-keeping genes or antibiotic targets, e.g. a mutated gyrase resistant to aminocoumarin antibiotics. PVMs include a protein reference sequence (often from antibiotic susceptible wild-type alleles), a curated bit-score cut-off, and mapped resistance variants. Mapped resistance variants may include any or all of single point mutations, insertions, or deletions curated from the scientific literature. A Strict RGI match has a BLASTP bit-score above the curated BLASTP cutoff value and contains at least one curated mutation from amongst the mapped resistance variants, while a Loose RGI match has a bit-score less than the curated BLASTP bit-score cut-off but still contains at least one curated mutation from amongst the mapped resistance variants.

Bit-score Cut-off (blastP): 700

Legend:

  • discovered in clinical, agricultural, or environmental isolates

  • discovered via laboratory selection experiments

  • ReSeqTB https://platform.reseqtb.org

Published Variants:


>gb|AXU66539.1|+|Clostridioides difficile EF-Tu mutants conferring resistance to elfamycin [Clostridioides difficile]
MAKAKYERTKPHVNIGTIGHVDHGKTTLTAAITKTLYDRYQLGEAVDFANIDKAPEERER
GITISTAHVEYETPNRHYAHVDCPGHADYVKNMITGAAQMDGAILVCSATDGPMPQTREH
ILLSRQVGVPYIVVFLNKCDMVDDEELLELVEMEVRDLLTEYDFPGDDTPIVRGSALMAL
EDPKSEWGDKIVELFEQIDEYIPAPERDTDKPFLMPVEDVFSITGRGTVATGRVERGVLK
VQDEVELVGLTEAPRKVVVTGVEMFRKLLDQAQAGDNIGALLRGVQRNEIERGQVLAKTG
SVKAHTKFTAEVYVLKKEEGGRHTPFFDGYRPQFYFRTTDVTGACKLPEGIEMVMPGDNV
TMEVDLINSIVVEEGLRFSIREGGRTVASGVVATIIE



>gb|CP012325.1|+|109611-110804|Clostridioides difficile EF-Tu mutants conferring resistance to elfamycin [Clostridioides difficile]
ATGGCTAAAGCTAAATACGAAAGAACAAAACCTCATGTTAATATAGGGACAATAGGACACGTAGACCACGGTAAAACTACATTAACAGCA
GCAATAACAAAAACATTATATGACAGATATCAATTAGGAGAAGCAGTAGATTTCGCAAACATAGATAAAGCTCCAGAAGAAAGAGAAAGA
GGAATCACAATATCAACAGCACACGTTGAGTATGAAACACCAAATAGACACTATGCACACGTTGACTGCCCAGGGCATGCTGACTACGTT
AAGAACATGATAACAGGAGCAGCACAAATGGACGGAGCAATATTAGTTTGTTCAGCAACAGATGGACCAATGCCACAAACAAGAGAGCAT
ATACTATTATCAAGACAAGTTGGAGTACCATATATAGTAGTATTCTTAAATAAATGTGACATGGTAGATGATGAAGAGTTATTAGAGTTA
GTAGAGATGGAAGTAAGAGATTTATTAACAGAGTATGATTTCCCAGGAGATGACACTCCAATAGTAAGAGGATCAGCGTTAATGGCATTA
GAAGATCCAAAGAGTGAGTGGGGAGATAAGATAGTAGAATTATTCGAGCAAATAGATGAATATATACCAGCACCAGAGAGAGATACAGAT
AAGCCATTCTTAATGCCAGTAGAAGACGTATTCTCAATCACAGGAAGAGGAACAGTTGCAACAGGAAGAGTGGAAAGAGGAGTATTAAAA
GTACAAGACGAAGTAGAATTAGTAGGATTAACAGAAGCACCAAGAAAAGTAGTAGTAACAGGAGTAGAGATGTTCAGAAAATTATTAGAC
CAAGCACAAGCAGGGGATAATATAGGAGCATTATTAAGAGGAGTACAAAGAAACGAGATAGAAAGAGGACAAGTACTAGCAAAGACTGGA
TCAGTAAAGGCACACACAAAGTTTACAGCAGAAGTATATGTACTTAAAAAAGAAGAAGGTGGAAGACATACACCATTCTTTGATGGATAT
AGACCACAATTTTACTTCAGAACAACAGACGTAACAGGAGCTTGTAAGTTACCAGAAGGAATAGAGATGGTAATGCCTGGAGATAACGTA
ACAATGGAAGTAGACTTAATAAACTCAATAGTTGTAGAAGAGGGATTAAGATTCTCAATAAGAGAAGGTGGAAGAACAGTAGCTTCAGGA
GTTGTTGCTACAATAATAGAGTAA