as.mo {AMR} | R Documentation |
Transform Arbitrary Input to Valid Microbial Taxonomy
Description
Use this function to get a valid microorganism code (mo
) based on arbitrary user input. Determination is done using intelligent rules and the complete taxonomic tree of the kingdoms Animalia, Archaea, Bacteria, and Protozoa, and most microbial species from the kingdom Fungi (see Source). The input can be almost anything: a full name (like "Staphylococcus aureus"
), an abbreviated name (such as "S. aureus"
), an abbreviation known in the field (such as "MRSA"
), or just a genus. See Examples.
Usage
as.mo(
x,
Becker = FALSE,
Lancefield = FALSE,
minimum_matching_score = NULL,
keep_synonyms = getOption("AMR_keep_synonyms", FALSE),
reference_df = get_mo_source(),
ignore_pattern = getOption("AMR_ignore_pattern", NULL),
cleaning_regex = getOption("AMR_cleaning_regex", mo_cleaning_regex()),
language = get_AMR_locale(),
info = interactive(),
...
)
is.mo(x)
mo_uncertainties()
mo_renamed()
mo_failures()
mo_reset_session()
mo_cleaning_regex()
Arguments
x |
a character vector or a data.frame with one or two columns |
Becker |
a logical to indicate whether staphylococci should be categorised into coagulase-negative staphylococci ("CoNS") and coagulase-positive staphylococci ("CoPS") instead of their own species, according to Karsten Becker et al. (see Source). Please see Details for a full list of staphylococcal species that will be converted. This excludes Staphylococcus aureus at default, use |
Lancefield |
a logical to indicate whether a beta-haemolytic Streptococcus should be categorised into Lancefield groups instead of their own species, according to Rebecca C. Lancefield (see Source). These streptococci will be categorised in their first group, e.g. Streptococcus dysgalactiae will be group C, although officially it was also categorised into groups G and L. . Please see Details for a full list of streptococcal species that will be converted. This excludes enterococci at default (who are in group D), use |
minimum_matching_score |
a numeric value to set as the lower limit for the MO matching score. When left blank, this will be determined automatically based on the character length of |
keep_synonyms |
a logical to indicate if old, previously valid taxonomic names must be preserved and not be corrected to currently accepted names. The default is |
reference_df |
a data.frame to be used for extra reference when translating |
ignore_pattern |
a Perl-compatible regular expression (case-insensitive) of which all matches in |
cleaning_regex |
a Perl-compatible regular expression (case-insensitive) to clean the input of |
language |
language to translate text like "no growth", which defaults to the system language (see |
info |
a logical to indicate if a progress bar should be printed if more than 25 items are to be coerced - the default is |
... |
other arguments passed on to functions |
Details
A microorganism (MO) code from this package (class: mo
) is human readable and typically looks like these examples:
Code Full name --------------- -------------------------------------- B_KLBSL Klebsiella B_KLBSL_PNMN Klebsiella pneumoniae B_KLBSL_PNMN_RHNS Klebsiella pneumoniae rhinoscleromatis | | | | | | | | | | | \---> subspecies, a 3-5 letter acronym | | \----> species, a 3-6 letter acronym | \----> genus, a 4-8 letter acronym \----> taxonomic kingdom: A (Archaea), AN (Animalia), B (Bacteria), F (Fungi), PL (Plantae), P (Protozoa)
Values that cannot be coerced will be considered 'unknown' and will be returned as the MO code UNKNOWN
with a warning.
Use the mo_*
functions to get properties based on the returned code, see Examples.
The as.mo()
function uses a novel matching score algorithm (see Matching Score for Microorganisms below) to match input against the available microbial taxonomy in this package. This will lead to the effect that e.g. "E. coli"
(a microorganism highly prevalent in humans) will return the microbial ID of Escherichia coli and not Entamoeba coli (a microorganism less prevalent in humans), although the latter would alphabetically come first.
With Becker = TRUE
, the following 85 staphylococci will be converted to the coagulase-negative group: S. argensis, S. arlettae, S. auricularis, S. borealis, S. caeli, S. caledonicus, S. canis, S. capitis, S. capitis capitis, S. capitis urealyticus, S. capitis ureolyticus, S. caprae, S. carnosus, S. carnosus carnosus, S. carnosus utilis, S. casei, S. caseolyticus, S. chromogenes, S. cohnii, S. cohnii cohnii, S. cohnii urealyticum, S. cohnii urealyticus, S. condimenti, S. croceilyticus, S. debuckii, S. devriesei, S. durrellii, S. edaphicus, S. epidermidis, S. equorum, S. equorum equorum, S. equorum linens, S. felis, S. fleurettii, S. gallinarum, S. haemolyticus, S. hominis, S. hominis hominis, S. hominis novobiosepticus, S. jettensis, S. kloosii, S. lentus, S. lloydii, S. lugdunensis, S. massiliensis, S. microti, S. muscae, S. nepalensis, S. pasteuri, S. petrasii, S. petrasii croceilyticus, S. petrasii jettensis, S. petrasii petrasii, S. petrasii pragensis, S. pettenkoferi, S. piscifermentans, S. pragensis, S. pseudoxylosus, S. pulvereri, S. ratti, S. rostri, S. saccharolyticus, S. saprophyticus, S. saprophyticus bovis, S. saprophyticus saprophyticus, S. schleiferi, S. schleiferi schleiferi, S. sciuri, S. sciuri carnaticus, S. sciuri lentus, S. sciuri rodentium, S. sciuri sciuri, S. simulans, S. stepanovicii, S. succinus, S. succinus casei, S. succinus succinus, S. taiwanensis, S. urealyticus, S. ureilyticus, S. veratri, S. vitulinus, S. vitulus, S. warneri, and S. xylosus.
The following 16 staphylococci will be converted to the coagulase-positive group: S. agnetis, S. argenteus, S. coagulans, S. cornubiensis, S. delphini, S. hyicus, S. hyicus chromogenes, S. hyicus hyicus, S. intermedius, S. lutrae, S. pseudintermedius, S. roterodami, S. schleiferi coagulans, S. schweitzeri, S. simiae, and S. singaporensis.
With Lancefield = TRUE
, the following streptococci will be converted to their corresponding Lancefield group: S. agalactiae (Group B), S. anginosus anginosus (Group F), S. anginosus whileyi (Group F), S. anginosus (Group F), S. canis (Group G), S. dysgalactiae dysgalactiae (Group C), S. dysgalactiae equisimilis (Group C), S. dysgalactiae (Group C), S. equi equi (Group C), S. equi ruminatorum (Group C), S. equi zooepidemicus (Group C), S. equi (Group C), S. pyogenes (Group A), S. salivarius salivarius (Group K), S. salivarius thermophilus (Group K), S. salivarius (Group K), and S. sanguinis (Group H).
Coping with Uncertain Results
Results of non-exact taxonomic input are based on their matching score. The lowest allowed score can be set with the minimum_matching_score
argument. At default this will be determined based on the character length of the input, and the taxonomic kingdom and human pathogenicity of the taxonomic outcome. If values are matched with uncertainty, a message will be shown to suggest the user to evaluate the results with mo_uncertainties()
, which returns a data.frame with all specifications.
To increase the quality of matching, the cleaning_regex
argument can be used to clean the input (i.e., x
). This must be a regular expression that matches parts of the input that should be removed before the input is matched against the available microbial taxonomy. It will be matched Perl-compatible and case-insensitive. The default value of cleaning_regex
is the outcome of the helper function mo_cleaning_regex()
.
There are three helper functions that can be run after using the as.mo()
function:
Use
mo_uncertainties()
to get a data.frame that prints in a pretty format with all taxonomic names that were guessed. The output contains the matching score for all matches (see Matching Score for Microorganisms below).Use
mo_failures()
to get a character vector with all values that could not be coerced to a valid value.Use
mo_renamed()
to get a data.frame with all values that could be coerced based on old, previously accepted taxonomic names.
Microbial Prevalence of Pathogens in Humans
The coercion rules consider the prevalence of microorganisms in humans, which is available as the prevalence
column in the microorganisms data set. The grouping into human pathogenic prevalence is explained in the section Matching Score for Microorganisms below.
Value
A character vector with additional class mo
Source
Berends MS et al. (2022). AMR: An R Package for Working with Antimicrobial Resistance Data. Journal of Statistical Software, 104(3), 1-31; doi:10.18637/jss.v104.i03
Becker K et al. (2014). Coagulase-Negative Staphylococci. Clin Microbiol Rev. 27(4): 870-926; doi:10.1128/CMR.00109-13
Becker K et al. (2019). Implications of identifying the recently defined members of the S. aureus complex, S. argenteus and S. schweitzeri: A position paper of members of the ESCMID Study Group for staphylococci and Staphylococcal Diseases (ESGS). Clin Microbiol Infect; doi:10.1016/j.cmi.2019.02.028
Becker K et al. (2020). Emergence of coagulase-negative staphylococci. Expert Rev Anti Infect Ther. 18(4):349-366; doi:10.1080/14787210.2020.1730813
Lancefield RC (1933). A serological differentiation of human and other groups of hemolytic streptococci. J Exp Med. 57(4): 571-95; doi:10.1084/jem.57.4.571
Berends MS et al. (2022). Trends in Occurrence and Phenotypic Resistance of Coagulase-Negative Staphylococci (CoNS) Found in Human Blood in the Northern Netherlands between 2013 and 2019/ Micro.rganisms 10(9), 1801; doi:10.3390/microorganisms10091801
Parte, AC et al. (2020). List of Prokaryotic names with Standing in Nomenclature (LPSN) moves to the DSMZ. International Journal of Systematic and Evolutionary Microbiology, 70, 5607-5612; doi:10.1099/ijsem.0.004332. Accessed from https://lpsn.dsmz.de on December 11th, 2022.
GBIF Secretariat (2022). GBIF Backbone Taxonomy. Checklist dataset doi:10.15468/39omei. Accessed from https://www.gbif.org on December 11th, 2022.
Reimer, LC et al. (2022). BacDive in 2022: the knowledge base for standardized bacterial and archaeal data. Nucleic Acids Res., 50(D1):D741-D74; doi:10.1093/nar/gkab961. Accessed from https://bacdive.dsmz.de on May 12th, 2023.
Public Health Information Network Vocabulary Access and Distribution System (PHIN VADS). US Edition of SNOMED CT from 1 September 2020. Value Set Name 'Microorganism', OID 2.16.840.1.114222.4.11.1009 (v12). URL: https://phinvads.cdc.gov
Bartlett A et al. (2022). A comprehensive list of bacterial pathogens infecting humans Microbiology 168:001269; doi:10.1099/mic.0.001269
Matching Score for Microorganisms
With ambiguous user input in as.mo()
and all the mo_*
functions, the returned results are chosen based on their matching score using mo_matching_score()
. This matching score m
, is calculated as:
where:
-
x
is the user input; -
n
is a taxonomic name (genus, species, and subspecies); -
l_n
is the length ofn
; -
lev
is the Levenshtein distance function (counting any insertion as 1, and any deletion or substitution as 2) that is needed to changex
inton
; -
p_n
is the human pathogenic prevalence group ofn
, as described below; -
k_n
is the taxonomic kingdom ofn
, set as Bacteria = 1, Fungi = 1.25, Protozoa = 1.5, Archaea = 2, others = 3.
The grouping into human pathogenic prevalence p
is based on recent work from Bartlett et al. (2022, doi:10.1099/mic.0.001269) who extensively studied medical-scientific literature to categorise all bacterial species into these groups:
-
Established, if a taxonomic species has infected at least three persons in three or more references. These records have
prevalence = 1.0
in the microorganisms data set; -
Putative, if a taxonomic species has fewer than three known cases. These records have
prevalence = 1.25
in the microorganisms data set.
Furthermore,
Any genus present in the established list also has
prevalence = 1.0
in the microorganisms data set;Any other genus present in the putative list has
prevalence = 1.25
in the microorganisms data set;Any other species or subspecies of which the genus is present in the two aforementioned groups, has
prevalence = 1.5
in the microorganisms data set;Any non-bacterial genus, species or subspecies of which the genus is present in the following list, has
prevalence = 1.25
in the microorganisms data set: Absidia, Acanthamoeba, Acremonium, Aedes, Alternaria, Amoeba, Ancylostoma, Angiostrongylus, Anisakis, Anopheles, Apophysomyces, Aspergillus, Aureobasidium, Basidiobolus, Beauveria, Blastocystis, Blastomyces, Candida, Capillaria, Chaetomium, Chrysonilia, Cladophialophora, Cladosporium, Conidiobolus, Contracaecum, Cordylobia, Cryptococcus, Curvularia, Demodex, Dermatobia, Dientamoeba, Diphyllobothrium, Dirofilaria, Echinostoma, Entamoeba, Enterobius, Exophiala, Exserohilum, Fasciola, Fonsecaea, Fusarium, Giardia, Haloarcula, Halobacterium, Halococcus, Hendersonula, Heterophyes, Histomonas, Histoplasma, Hymenolepis, Hypomyces, Hysterothylacium, Leishmania, Malassezia, Malbranchea, Metagonimus, Meyerozyma, Microsporidium, Microsporum, Mortierella, Mucor, Mycocentrospora, Necator, Nectria, Ochroconis, Oesophagostomum, Oidiodendron, Opisthorchis, Pediculus, Penicillium, Phlebotomus, Phoma, Pichia, Piedraia, Pithomyces, Pityrosporum, Pneumocystis, Pseudallescheria, Pseudoterranova, Pulex, Rhizomucor, Rhizopus, Rhodotorula, Saccharomyces, Sarcoptes, Scolecobasidium, Scopulariopsis, Scytalidium, Spirometra, Sporobolomyces, Stachybotrys, Strongyloides, Syngamus, Taenia, Talaromyces, Toxocara, Trichinella, Trichobilharzia, Trichoderma, Trichomonas, Trichophyton, Trichosporon, Trichostrongylus, Trichuris, Tritirachium, Trombicula, Trypanosoma, Tunga, or Wuchereria;All other records have
prevalence = 2.0
in the microorganisms data set.
When calculating the matching score, all characters in x
and n
are ignored that are other than A-Z, a-z, 0-9, spaces and parentheses.
All matches are sorted descending on their matching score and for all user input values, the top match will be returned. This will lead to the effect that e.g., "E. coli"
will return the microbial ID of Escherichia coli (m = 0.688
, a highly prevalent microorganism found in humans) and not Entamoeba coli (m = 0.381
, a less prevalent microorganism in humans), although the latter would alphabetically come first.
Reference Data Publicly Available
All data sets in this AMR
package (about microorganisms, antibiotics, SIR interpretation, EUCAST rules, etc.) are publicly and freely available for download in the following formats: R, MS Excel, Apache Feather, Apache Parquet, SPSS, SAS, and Stata. We also provide tab-separated plain text files that are machine-readable and suitable for input in any software program, such as laboratory information systems. Please visit our website for the download links. The actual files are of course available on our GitHub repository.
See Also
microorganisms for the data.frame that is being used to determine ID's.
The mo_*
functions (such as mo_genus()
, mo_gramstain()
) to get properties based on the returned code.
Examples
# These examples all return "B_STPHY_AURS", the ID of S. aureus:
as.mo(c(
"sau", # WHONET code
"stau",
"STAU",
"staaur",
"S. aureus",
"S aureus",
"Sthafilokkockus aureus", # handles incorrect spelling
"Staphylococcus aureus (MRSA)",
"MRSA", # Methicillin Resistant S. aureus
"VISA", # Vancomycin Intermediate S. aureus
"VRSA", # Vancomycin Resistant S. aureus
115329001 # SNOMED CT code
))
# Dyslexia is no problem - these all work:
as.mo(c(
"Ureaplasma urealyticum",
"Ureaplasma urealyticus",
"Ureaplasmium urealytica",
"Ureaplazma urealitycium"
))
# input will get cleaned up with the input given in the `cleaning_regex` argument,
# which defaults to `mo_cleaning_regex()`:
cat(mo_cleaning_regex(), "\n")
as.mo("Streptococcus group A")
as.mo("S. epidermidis") # will remain species: B_STPHY_EPDR
as.mo("S. epidermidis", Becker = TRUE) # will not remain species: B_STPHY_CONS
as.mo("S. pyogenes") # will remain species: B_STRPT_PYGN
as.mo("S. pyogenes", Lancefield = TRUE) # will not remain species: B_STRPT_GRPA
# All mo_* functions use as.mo() internally too (see ?mo_property):
mo_genus("E. coli")
mo_gramstain("ESCO")
mo_is_intrinsic_resistant("ESCCOL", ab = "vanco")