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AMR/R/sir.R

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# ==================================================================== #
# TITLE: #
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# AMR: An R Package for Working with Antimicrobial Resistance Data #
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# #
# SOURCE CODE: #
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# https://github.com/msberends/AMR #
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# #
# PLEASE CITE THIS SOFTWARE AS: #
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# Berends MS, Luz CF, Friedrich AW, Sinha BNM, Albers CJ, Glasner C #
# (2022). AMR: An R Package for Working with Antimicrobial Resistance #
# Data. Journal of Statistical Software, 104(3), 1-31. #
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# https://doi.org/10.18637/jss.v104.i03 #
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# #
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# Developed at the University of Groningen and the University Medical #
# Center Groningen in The Netherlands, in collaboration with many #
# colleagues from around the world, see our website. #
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# #
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# This R package is free software; you can freely use and distribute #
# it for both personal and commercial purposes under the terms of the #
# GNU General Public License version 2.0 (GNU GPL-2), as published by #
# the Free Software Foundation. #
# We created this package for both routine data analysis and academic #
# research and it was publicly released in the hope that it will be #
# useful, but it comes WITHOUT ANY WARRANTY OR LIABILITY. #
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# #
# Visit our website for the full manual and a complete tutorial about #
# how to conduct AMR data analysis: https://msberends.github.io/AMR/ #
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# ==================================================================== #
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#' Translate MIC and Disk Diffusion to SIR, or Clean Existing SIR Data
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#'
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#' @description Interpret minimum inhibitory concentration (MIC) values and disk diffusion diameters according to EUCAST or CLSI, or clean up existing SIR values. This transforms the input to a new class [`sir`], which is an ordered [factor] with levels `S < I < R`.
#'
#' Currently available **breakpoint guidelines** are EUCAST `r min(as.integer(gsub("[^0-9]", "", subset(AMR::clinical_breakpoints, guideline %like% "EUCAST")$guideline)))`-`r max(as.integer(gsub("[^0-9]", "", subset(AMR::clinical_breakpoints, guideline %like% "EUCAST")$guideline)))` and CLSI `r min(as.integer(gsub("[^0-9]", "", subset(AMR::clinical_breakpoints, guideline %like% "CLSI")$guideline)))`-`r max(as.integer(gsub("[^0-9]", "", subset(AMR::clinical_breakpoints, guideline %like% "CLSI")$guideline)))`, and available **breakpoint types** are `r vector_and(clinical_breakpoints$type)`.
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#'
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#' All breakpoints used for interpretation are publicly available in the [clinical_breakpoints] data set.
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#' @rdname as.sir
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#' @param x vector of values (for class [`mic`]: MIC values in mg/L, for class [`disk`]: a disk diffusion radius in millimetres)
#' @param mo any (vector of) text that can be coerced to valid microorganism codes with [as.mo()], can be left empty to determine it automatically
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#' @param ab any (vector of) text that can be coerced to a valid antimicrobial drug code with [as.ab()]
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#' @param uti (Urinary Tract Infection) A vector with [logical]s (`TRUE` or `FALSE`) to specify whether a UTI specific interpretation from the guideline should be chosen. For using [as.sir()] on a [data.frame], this can also be a column containing [logical]s or when left blank, the data set will be searched for a column 'specimen', and rows within this column containing 'urin' (such as 'urine', 'urina') will be regarded isolates from a UTI. See *Examples*.
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#' @inheritParams first_isolate
#' @param guideline defaults to EUCAST `r max(as.integer(gsub("[^0-9]", "", subset(AMR::clinical_breakpoints, guideline %like% "EUCAST")$guideline)))` (the latest implemented EUCAST guideline in the [AMR::clinical_breakpoints] data set), but can be set with the [package option][AMR-options] [`AMR_guideline`][AMR-options]. Currently supports EUCAST (`r min(as.integer(gsub("[^0-9]", "", subset(AMR::clinical_breakpoints, guideline %like% "EUCAST")$guideline)))`-`r max(as.integer(gsub("[^0-9]", "", subset(AMR::clinical_breakpoints, guideline %like% "EUCAST")$guideline)))`) and CLSI (`r min(as.integer(gsub("[^0-9]", "", subset(AMR::clinical_breakpoints, guideline %like% "CLSI")$guideline)))`-`r max(as.integer(gsub("[^0-9]", "", subset(AMR::clinical_breakpoints, guideline %like% "CLSI")$guideline)))`), see *Details*.
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#' @param conserve_capped_values a [logical] to indicate that MIC values starting with `">"` (but not `">="`) must always return "R" , and that MIC values starting with `"<"` (but not `"<="`) must always return "S"
#' @param add_intrinsic_resistance *(only useful when using a EUCAST guideline)* a [logical] to indicate whether intrinsic antibiotic resistance must also be considered for applicable bug-drug combinations, meaning that e.g. ampicillin will always return "R" in *Klebsiella* species. Determination is based on the [intrinsic_resistant] data set, that itself is based on `r format_eucast_version_nr(3.3)`.
#' @param include_screening a [logical] to indicate that clinical breakpoints for screening are allowed - the default is `FALSE`. Can also be set with the [package option][AMR-options] [`AMR_include_screening`][AMR-options].
#' @param include_PKPD a [logical] to indicate that PK/PD clinical breakpoints must be applied as a last resort - the default is `TRUE`. Can also be set with the [package option][AMR-options] [`AMR_include_PKPD`][AMR-options].
#' @param breakpoint_type the type of breakpoints to use, either `r vector_or(clinical_breakpoints$type)`. ECOFF stands for Epidemiological Cut-Off values. The default is `"human"`, which can also be set with the [package option][AMR-options] [`AMR_breakpoint_type`][AMR-options].
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#' @param reference_data a [data.frame] to be used for interpretation, which defaults to the [clinical_breakpoints] data set. Changing this argument allows for using own interpretation guidelines. This argument must contain a data set that is equal in structure to the [clinical_breakpoints] data set (same column names and column types). Please note that the `guideline` argument will be ignored when `reference_data` is manually set.
#' @param threshold maximum fraction of invalid antimicrobial interpretations of `x`, see *Examples*
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#' @param ... for using on a [data.frame]: names of columns to apply [as.sir()] on (supports tidy selection such as `column1:column4`). Otherwise: arguments passed on to methods.
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#' @details
#' *Note: The clinical breakpoints in this package were validated through and imported from [WHONET](https://whonet.org) and the public use of this `AMR` package has been endorsed by CLSI and EUCAST, please see [clinical_breakpoints] for more information.*
#'
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#' ### How it Works
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#'
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#' The [as.sir()] function works in four ways:
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#'
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#' 1. For **cleaning raw / untransformed data**. The data will be cleaned to only contain values S, I and R and will try its best to determine this with some intelligence. For example, mixed values with SIR interpretations and MIC values such as `"<0.25; S"` will be coerced to `"S"`. Combined interpretations for multiple test methods (as seen in laboratory records) such as `"S; S"` will be coerced to `"S"`, but a value like `"S; I"` will return `NA` with a warning that the input is unclear.
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#'
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#' 2. For **interpreting minimum inhibitory concentration (MIC) values** according to EUCAST or CLSI. You must clean your MIC values first using [as.mic()], that also gives your columns the new data class [`mic`]. Also, be sure to have a column with microorganism names or codes. It will be found automatically, but can be set manually using the `mo` argument.
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#' * Using `dplyr`, SIR interpretation can be done very easily with either:
#' ```
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#' your_data %>% mutate_if(is.mic, as.sir)
#' your_data %>% mutate(across(where(is.mic), as.sir))
#' ```
#' * Operators like "<=" will be stripped before interpretation. When using `conserve_capped_values = TRUE`, an MIC value of e.g. ">2" will always return "R", even if the breakpoint according to the chosen guideline is ">=4". This is to prevent that capped values from raw laboratory data would not be treated conservatively. The default behaviour (`conserve_capped_values = FALSE`) considers ">2" to be lower than ">=4" and might in this case return "S" or "I".
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#' 3. For **interpreting disk diffusion diameters** according to EUCAST or CLSI. You must clean your disk zones first using [as.disk()], that also gives your columns the new data class [`disk`]. Also, be sure to have a column with microorganism names or codes. It will be found automatically, but can be set manually using the `mo` argument.
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#' * Using `dplyr`, SIR interpretation can be done very easily with either:
#' ```
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#' your_data %>% mutate_if(is.disk, as.sir)
#' your_data %>% mutate(across(where(is.disk), as.sir))
#' ```
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#' 4. For **interpreting a complete data set**, with automatic determination of MIC values, disk diffusion diameters, microorganism names or codes, and antimicrobial test results. This is done very simply by running `as.sir(your_data)`.
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#'
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#' **For points 2, 3 and 4: Use [sir_interpretation_history()]** to retrieve a [data.frame] (or [tibble][tibble::tibble()] if the `tibble` package is installed) with all results of the last [as.sir()] call.
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#'
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#' ### Supported Guidelines
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#'
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#' For interpreting MIC values as well as disk diffusion diameters, currently implemented guidelines are EUCAST (`r min(as.integer(gsub("[^0-9]", "", subset(AMR::clinical_breakpoints, guideline %like% "EUCAST")$guideline)))`-`r max(as.integer(gsub("[^0-9]", "", subset(AMR::clinical_breakpoints, guideline %like% "EUCAST")$guideline)))`) and CLSI (`r min(as.integer(gsub("[^0-9]", "", subset(AMR::clinical_breakpoints, guideline %like% "CLSI")$guideline)))`-`r max(as.integer(gsub("[^0-9]", "", subset(AMR::clinical_breakpoints, guideline %like% "CLSI")$guideline)))`).
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#'
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#' Thus, the `guideline` argument must be set to e.g., ``r paste0('"', subset(AMR::clinical_breakpoints, guideline %like% "EUCAST")$guideline[1], '"')`` or ``r paste0('"', subset(AMR::clinical_breakpoints, guideline %like% "CLSI")$guideline[1], '"')``. By simply using `"EUCAST"` (the default) or `"CLSI"` as input, the latest included version of that guideline will automatically be selected. You can set your own data set using the `reference_data` argument. The `guideline` argument will then be ignored.
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#'
#' You can set the default guideline with the [package option][AMR-options] [`AMR_guideline`][AMR-options] (e.g. in your `.Rprofile` file), such as:
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#'
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#' ```
#' options(AMR_guideline = "CLSI")
#' options(AMR_guideline = "CLSI 2018")
#' options(AMR_guideline = "EUCAST 2020")
#' # or to reset:
#' options(AMR_guideline = NULL)
#' ```
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#'
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#' ### After Interpretation
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#'
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#' After using [as.sir()], you can use the [eucast_rules()] defined by EUCAST to (1) apply inferred susceptibility and resistance based on results of other antimicrobials and (2) apply intrinsic resistance based on taxonomic properties of a microorganism.
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#'
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#' ### Machine-Readable Clinical Breakpoints
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#'
#' The repository of this package [contains a machine-readable version](https://github.com/msberends/AMR/blob/main/data-raw/clinical_breakpoints.txt) of all guidelines. This is a CSV file consisting of `r format(nrow(AMR::clinical_breakpoints), big.mark = " ")` rows and `r ncol(AMR::clinical_breakpoints)` columns. This file is machine-readable, since it contains one row for every unique combination of the test method (MIC or disk diffusion), the antimicrobial drug and the microorganism. **This allows for easy implementation of these rules in laboratory information systems (LIS)**. Note that it only contains interpretation guidelines for humans - interpretation guidelines from CLSI for animals were removed.
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#'
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#' ### Other
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#'
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#' The function [is.sir()] detects if the input contains class `sir`. If the input is a [data.frame], it iterates over all columns and returns a [logical] vector.
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#'
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#' The function [is_sir_eligible()] returns `TRUE` when a columns contains at most 5% invalid antimicrobial interpretations (not S and/or I and/or R), and `FALSE` otherwise. The threshold of 5% can be set with the `threshold` argument. If the input is a [data.frame], it iterates over all columns and returns a [logical] vector.
#' @section Interpretation of SIR:
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#' In 2019, the European Committee on Antimicrobial Susceptibility Testing (EUCAST) has decided to change the definitions of susceptibility testing categories S, I, and R as shown below (<https://www.eucast.org/newsiandr>):
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#'
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#' - **S - Susceptible, standard dosing regimen**\cr
#' A microorganism is categorised as "Susceptible, standard dosing regimen", when there is a high likelihood of therapeutic success using a standard dosing regimen of the agent.
#' - **I - Susceptible, increased exposure** *\cr
#' A microorganism is categorised as "Susceptible, Increased exposure*" when there is a high likelihood of therapeutic success because exposure to the agent is increased by adjusting the dosing regimen or by its concentration at the site of infection.
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#' - **R = Resistant**\cr
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#' A microorganism is categorised as "Resistant" when there is a high likelihood of therapeutic failure even when there is increased exposure.
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#'
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#' * *Exposure* is a function of how the mode of administration, dose, dosing interval, infusion time, as well as distribution and excretion of the antimicrobial agent will influence the infecting organism at the site of infection.
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#'
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#' This AMR package honours this insight. Use [susceptibility()] (equal to [proportion_SI()]) to determine antimicrobial susceptibility and [count_susceptible()] (equal to [count_SI()]) to count susceptible isolates.
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#' @return Ordered [factor] with new class `sir`
#' @aliases sir
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#' @export
#' @seealso [as.mic()], [as.disk()], [as.mo()]
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#' @source
#' For interpretations of minimum inhibitory concentration (MIC) values and disk diffusion diameters:
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#'
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#' - **M39 Analysis and Presentation of Cumulative Antimicrobial Susceptibility Test Data**, `r min(as.integer(gsub("[^0-9]", "", subset(AMR::clinical_breakpoints, guideline %like% "CLSI")$guideline)))`-`r max(as.integer(gsub("[^0-9]", "", subset(AMR::clinical_breakpoints, guideline %like% "CLSI")$guideline)))`, *Clinical and Laboratory Standards Institute* (CLSI). <https://clsi.org/standards/products/microbiology/documents/m39/>.
#' - **M100 Performance Standard for Antimicrobial Susceptibility Testing**, `r min(as.integer(gsub("[^0-9]", "", subset(AMR::clinical_breakpoints, guideline %like% "CLSI")$guideline)))`-`r max(as.integer(gsub("[^0-9]", "", subset(AMR::clinical_breakpoints, guideline %like% "CLSI")$guideline)))`, *Clinical and Laboratory Standards Institute* (CLSI). <https://clsi.org/standards/products/microbiology/documents/m100/>.
#' - **Breakpoint tables for interpretation of MICs and zone diameters**, `r min(as.integer(gsub("[^0-9]", "", subset(AMR::clinical_breakpoints, guideline %like% "EUCAST")$guideline)))`-`r max(as.integer(gsub("[^0-9]", "", subset(AMR::clinical_breakpoints, guideline %like% "EUCAST")$guideline)))`, *European Committee on Antimicrobial Susceptibility Testing* (EUCAST). <https://www.eucast.org/clinical_breakpoints>.
#' @inheritSection AMR Reference Data Publicly Available
#' @examples
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#' example_isolates
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#' summary(example_isolates) # see all SIR results at a glance
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#'
#' # For INTERPRETING disk diffusion and MIC values -----------------------
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#'
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#' # a whole data set, even with combined MIC values and disk zones
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#' df <- data.frame(
#' microorganism = "Escherichia coli",
#' AMP = as.mic(8),
#' CIP = as.mic(0.256),
#' GEN = as.disk(18),
#' TOB = as.disk(16),
#' ERY = "R"
#' )
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#' as.sir(df)
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#'
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#' # return a 'logbook' about the results:
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#' sir_interpretation_history()
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#'
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#' # for single values
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#' as.sir(
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#' x = as.mic(2),
#' mo = as.mo("S. pneumoniae"),
#' ab = "AMP",
#' guideline = "EUCAST"
#' )
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#'
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#' as.sir(
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#' x = as.disk(18),
#' mo = "Strep pneu", # `mo` will be coerced with as.mo()
#' ab = "ampicillin", # and `ab` with as.ab()
#' guideline = "EUCAST"
#' )
#'
#' \donttest{
#' # the dplyr way
#' if (require("dplyr")) {
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#' df %>% mutate_if(is.mic, as.sir)
#' df %>% mutate_if(function(x) is.mic(x) | is.disk(x), as.sir)
#' df %>% mutate(across(where(is.mic), as.sir))
#' df %>% mutate_at(vars(AMP:TOB), as.sir)
#' df %>% mutate(across(AMP:TOB, as.sir))
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#'
#' df %>%
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#' mutate_at(vars(AMP:TOB), as.sir, mo = .$microorganism)
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#'
#' # to include information about urinary tract infections (UTI)
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#' data.frame(
#' mo = "E. coli",
#' NIT = c("<= 2", 32),
#' from_the_bladder = c(TRUE, FALSE)
#' ) %>%
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#' as.sir(uti = "from_the_bladder")
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#'
#' data.frame(
#' mo = "E. coli",
#' NIT = c("<= 2", 32),
#' specimen = c("urine", "blood")
#' ) %>%
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#' as.sir() # automatically determines urine isolates
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#'
#' df %>%
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#' mutate_at(vars(AMP:TOB), as.sir, mo = "E. coli", uti = TRUE)
#' }
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#'
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#' # For CLEANING existing SIR values ------------------------------------
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#'
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#' as.sir(c("S", "I", "R", "A", "B", "C"))
#' as.sir("<= 0.002; S") # will return "S"
#' sir_data <- as.sir(c(rep("S", 474), rep("I", 36), rep("R", 370)))
#' is.sir(sir_data)
#' plot(sir_data) # for percentages
#' barplot(sir_data) # for frequencies
#'
#' # the dplyr way
#' if (require("dplyr")) {
#' example_isolates %>%
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#' mutate_at(vars(PEN:RIF), as.sir)
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#' # same:
#' example_isolates %>%
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#' as.sir(PEN:RIF)
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#'
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#' # fastest way to transform all columns with already valid AMR results to class `sir`:
#' example_isolates %>%
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#' mutate_if(is_sir_eligible, as.sir)
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#'
#' # since dplyr 1.0.0, this can also be:
#' # example_isolates %>%
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#' # mutate(across(where(is_sir_eligible), as.sir))
#' }
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#' }
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as.sir <- function(x, ...) {
UseMethod("as.sir")
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}
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#' @rdname as.sir
#' @details `NA_sir_` is a missing value of the new `sir` class, analogous to e.g. base \R's [`NA_character_`][base::NA].
#' @export
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NA_sir_ <- set_clean_class(factor(NA_character_, levels = c("S", "I", "R"), ordered = TRUE),
new_class = c("sir", "ordered", "factor")
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)
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#' @rdname as.sir
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#' @export
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is.sir <- function(x) {
if (inherits(x, "data.frame")) {
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unname(vapply(FUN.VALUE = logical(1), x, is.sir))
} else {
rsi <- inherits(x, "rsi")
sir <- inherits(x, "sir")
if (isTRUE(rsi) && message_not_thrown_before("is.sir-rsi")) {
deprecation_warning(extra_msg = "The 'rsi' class has been replaced with 'sir'. Transform your 'rsi' columns to 'sir' with `as.sir()`, e.g.:\n your_data %>% mutate_if(is.rsi, as.sir)")
}
isTRUE(rsi) || isTRUE(sir)
}
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}
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#' @rdname as.sir
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#' @export
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is_sir_eligible <- function(x, threshold = 0.05) {
meet_criteria(threshold, allow_class = "numeric", has_length = 1)
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if (inherits(x, "data.frame")) {
# iterate this function over all columns
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return(unname(vapply(FUN.VALUE = logical(1), x, is_sir_eligible)))
}
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stop_if(NCOL(x) > 1, "`x` must be a one-dimensional vector.")
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if (any(c(
"numeric",
"integer",
"mo",
"ab",
"Date",
"POSIXt",
"raw",
"hms",
"mic",
"disk"
)
%in% class(x))) {
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# no transformation needed
return(FALSE)
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} else if (all(x %in% c("S", "I", "R", NA)) & !all(is.na(x))) {
return(TRUE)
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} else if (!any(c("S", "I", "R") %in% x, na.rm = TRUE) & !all(is.na(x))) {
return(FALSE)
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} else {
x <- x[!is.na(x) & !is.null(x) & !x %in% c("", "-", "NULL")]
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if (length(x) == 0) {
# no other values than empty
cur_col <- get_current_column()
if (!is.null(cur_col)) {
ab <- suppressWarnings(as.ab(cur_col, fast_mode = TRUE, info = FALSE))
if (!is.na(ab)) {
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# this is a valid antibiotic drug code
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message_(
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"Column '", font_bold(cur_col), "' is SIR eligible (despite only having empty values), since it seems to be ",
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ab_name(ab, language = NULL, tolower = TRUE), " (", ab, ")"
)
return(TRUE)
}
}
# all values empty and no antibiotic col name - return FALSE
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return(FALSE)
}
# transform all values and see if it meets the set threshold
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checked <- suppressWarnings(as.sir(x))
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outcome <- sum(is.na(checked)) / length(x)
outcome <= threshold
}
}
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#' @export
# extra param: warn (logical, to never throw a warning)
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as.sir.default <- function(x, ...) {
if (inherits(x, "sir")) {
return(x)
}
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x.bak <- x
x <- as.character(x) # this is needed to prevent the vctrs pkg from throwing an error
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if (inherits(x.bak, c("integer", "numeric", "double")) && all(x %in% c(1:3, NA))) {
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# support haven package for importing e.g., from SPSS - it adds the 'labels' attribute
lbls <- attributes(x.bak)$labels
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if (!is.null(lbls) && all(c("S", "I", "R") %in% names(lbls)) && all(c(1:3) %in% lbls)) {
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x[x.bak == 1] <- names(lbls[lbls == 1])
x[x.bak == 2] <- names(lbls[lbls == 2])
x[x.bak == 3] <- names(lbls[lbls == 3])
} else {
x[x.bak == 1] <- "S"
x[x.bak == 2] <- "I"
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x[x.bak == 3] <- "R"
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}
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} else if (inherits(x.bak, "character") && all(x %in% c("1", "2", "3", "S", "I", "R", NA_character_))) {
x[x.bak == "1"] <- "S"
x[x.bak == "2"] <- "I"
x[x.bak == "3"] <- "R"
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} else if (!all(is.na(x)) && !identical(levels(x), c("S", "I", "R")) && !all(x %in% c("S", "I", "R", NA))) {
if (all(x %unlike% "(R|S|I)", na.rm = TRUE)) {
# check if they are actually MICs or disks
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if (all_valid_mics(x)) {
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warning_("in `as.sir()`: the input seems to contain MIC values. You can transform them with `as.mic()` before running `as.sir()` to interpret them.")
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} else if (all_valid_disks(x)) {
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warning_("in `as.sir()`: the input seems to contain disk diffusion values. You can transform them with `as.disk()` before running `as.sir()` to interpret them.")
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}
}
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# trim leading and trailing spaces, new lines, etc.
x <- trimws2(as.character(unlist(x)))
x[x %in% c(NA, "", "-", "NULL")] <- NA_character_
x.bak <- x
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na_before <- length(x[is.na(x)])
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# correct for translations
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trans_R <- unlist(TRANSLATIONS[
which(TRANSLATIONS$pattern == "Resistant"),
LANGUAGES_SUPPORTED[LANGUAGES_SUPPORTED %in% colnames(TRANSLATIONS)]
])
trans_S <- unlist(TRANSLATIONS[
which(TRANSLATIONS$pattern == "Susceptible"),
LANGUAGES_SUPPORTED[LANGUAGES_SUPPORTED %in% colnames(TRANSLATIONS)]
])
trans_I <- unlist(TRANSLATIONS[
which(TRANSLATIONS$pattern %in% c("Incr. exposure", "Susceptible, incr. exp.", "Intermediate")),
LANGUAGES_SUPPORTED[LANGUAGES_SUPPORTED %in% colnames(TRANSLATIONS)]
])
x <- gsub(paste0(unique(trans_R[!is.na(trans_R)]), collapse = "|"), "R", x, ignore.case = TRUE)
x <- gsub(paste0(unique(trans_S[!is.na(trans_S)]), collapse = "|"), "S", x, ignore.case = TRUE)
x <- gsub(paste0(unique(trans_I[!is.na(trans_I)]), collapse = "|"), "I", x, ignore.case = TRUE)
# replace all English textual input
x[x %like% "([^a-z]|^)res(is(tant)?)?"] <- "R"
x[x %like% "([^a-z]|^)sus(cep(tible)?)?"] <- "S"
x[x %like% "([^a-z]|^)int(er(mediate)?)?|incr.*exp"] <- "I"
# remove other invalid characters
# set to capitals
x <- toupper(x)
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x <- gsub("[^A-Z]+", "", x, perl = TRUE)
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# CLSI uses SDD for "susceptible dose-dependent"
x <- gsub("SDD", "I", x, fixed = TRUE)
# some labs now report "H" instead of "I" to not interfere with EUCAST prior to 2019
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x <- gsub("H", "I", x, fixed = TRUE)
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# MIPS uses D for Dose-dependent (which is I, but it will throw a note)
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x <- gsub("D", "I", x, fixed = TRUE)
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# MIPS uses U for "susceptible urine"
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x <- gsub("U", "S", x, fixed = TRUE)
# in cases of "S;S" keep S, but in case of "S;I" make it NA
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x <- gsub("^S+$", "S", x)
x <- gsub("^I+$", "I", x)
x <- gsub("^R+$", "R", x)
x[!x %in% c("S", "I", "R")] <- NA_character_
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na_after <- length(x[is.na(x) | x == ""])
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if (!isFALSE(list(...)$warn)) { # so as.sir(..., warn = FALSE) will never throw a warning
if (na_before != na_after) {
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list_missing <- x.bak[is.na(x) & !is.na(x.bak) & x.bak != ""] %pm>%
unique() %pm>%
sort() %pm>%
vector_and(quotes = TRUE)
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cur_col <- get_current_column()
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warning_("in `as.sir()`: ", na_after - na_before, " result",
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ifelse(na_after - na_before > 1, "s", ""),
ifelse(is.null(cur_col), "", paste0(" in column '", cur_col, "'")),
" truncated (",
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round(((na_after - na_before) / length(x)) * 100),
"%) that were invalid antimicrobial interpretations: ",
list_missing,
call = FALSE
)
}
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if (any(toupper(x.bak[!is.na(x.bak)]) == "U") && message_not_thrown_before("as.sir", "U")) {
warning_("in `as.sir()`: 'U' was interpreted as 'S', following some laboratory systems")
}
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if (any(toupper(x.bak[!is.na(x.bak)]) == "D") && message_not_thrown_before("as.sir", "D")) {
warning_("in `as.sir()`: 'D' (dose-dependent) was interpreted as 'I', following some laboratory systems")
}
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if (any(toupper(x.bak[!is.na(x.bak)]) == "SDD") && message_not_thrown_before("as.sir", "SDD")) {
warning_("in `as.sir()`: 'SDD' (susceptible dose-dependent, coined by CLSI) was interpreted as 'I' to comply with EUCAST's 'I'")
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}
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if (any(toupper(x.bak[!is.na(x.bak)]) == "H") && message_not_thrown_before("as.sir", "H")) {
warning_("in `as.sir()`: 'H' was interpreted as 'I', following some laboratory systems")
}
}
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}
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set_clean_class(factor(x, levels = c("S", "I", "R"), ordered = TRUE),
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new_class = c("sir", "ordered", "factor")
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)
}
2018-08-23 00:40:36 +02:00
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#' @rdname as.sir
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#' @export
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as.sir.mic <- function(x,
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mo = NULL,
ab = deparse(substitute(x)),
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guideline = getOption("AMR_guideline", "EUCAST"),
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uti = NULL,
conserve_capped_values = FALSE,
add_intrinsic_resistance = FALSE,
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reference_data = AMR::clinical_breakpoints,
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include_screening = getOption("AMR_include_screening", FALSE),
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include_PKPD = getOption("AMR_include_PKPD", TRUE),
breakpoint_type = getOption("AMR_breakpoint_type", "human"),
...) {
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as_sir_method(
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method_short = "mic",
method_long = "MIC values",
x = x,
mo = mo,
ab = ab,
guideline = guideline,
uti = uti,
conserve_capped_values = conserve_capped_values,
add_intrinsic_resistance = add_intrinsic_resistance,
reference_data = reference_data,
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include_screening = include_screening,
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include_PKPD = include_PKPD,
breakpoint_type = breakpoint_type,
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...
)
2019-05-10 16:44:59 +02:00
}
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#' @rdname as.sir
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#' @export
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as.sir.disk <- function(x,
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mo = NULL,
ab = deparse(substitute(x)),
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guideline = getOption("AMR_guideline", "EUCAST"),
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uti = NULL,
add_intrinsic_resistance = FALSE,
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reference_data = AMR::clinical_breakpoints,
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include_screening = getOption("AMR_include_screening", FALSE),
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include_PKPD = getOption("AMR_include_PKPD", TRUE),
breakpoint_type = getOption("AMR_breakpoint_type", "human"),
...) {
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as_sir_method(
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method_short = "disk",
method_long = "disk diffusion zones",
x = x,
mo = mo,
ab = ab,
guideline = guideline,
uti = uti,
conserve_capped_values = FALSE,
add_intrinsic_resistance = add_intrinsic_resistance,
reference_data = reference_data,
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include_screening = include_screening,
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include_PKPD = include_PKPD,
breakpoint_type = breakpoint_type,
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...
)
2020-02-20 13:19:23 +01:00
}
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#' @rdname as.sir
2020-02-20 13:19:23 +01:00
#' @export
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as.sir.data.frame <- function(x,
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...,
col_mo = NULL,
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guideline = getOption("AMR_guideline", "EUCAST"),
uti = NULL,
conserve_capped_values = FALSE,
add_intrinsic_resistance = FALSE,
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reference_data = AMR::clinical_breakpoints,
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include_screening = getOption("AMR_include_screening", FALSE),
include_PKPD = getOption("AMR_include_PKPD", TRUE),
breakpoint_type = getOption("AMR_breakpoint_type", "human")) {
meet_criteria(x, allow_class = "data.frame") # will also check for dimensions > 0
meet_criteria(col_mo, allow_class = "character", is_in = colnames(x), allow_NULL = TRUE)
meet_criteria(guideline, allow_class = "character", has_length = 1)
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meet_criteria(uti, allow_class = c("logical", "character"), allow_NULL = TRUE, allow_NA = TRUE)
meet_criteria(conserve_capped_values, allow_class = "logical", has_length = 1)
meet_criteria(add_intrinsic_resistance, allow_class = "logical", has_length = 1)
meet_criteria(reference_data, allow_class = "data.frame")
meet_criteria(include_screening, allow_class = "logical", has_length = 1)
meet_criteria(include_PKPD, allow_class = "logical", has_length = 1)
meet_criteria(breakpoint_type, allow_class = "character", is_in = reference_data$type, has_length = 1)
2022-08-28 10:31:50 +02:00
2020-12-22 00:51:17 +01:00
x.bak <- x
for (i in seq_len(ncol(x))) {
# don't keep factors, overwriting them is hard
if (is.factor(x[, i, drop = TRUE])) {
x[, i] <- as.character(x[, i, drop = TRUE])
}
}
2022-08-28 10:31:50 +02:00
2020-10-20 21:00:57 +02:00
# -- MO
col_mo.bak <- col_mo
if (is.null(col_mo)) {
col_mo <- search_type_in_df(x = x, type = "mo", info = FALSE)
}
2022-08-28 10:31:50 +02:00
2020-02-20 13:19:23 +01:00
# -- UTIs
col_uti <- uti
if (is.null(col_uti)) {
col_uti <- search_type_in_df(x = x, type = "uti")
}
if (!is.null(col_uti)) {
if (is.logical(col_uti)) {
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# already a [logical] vector as input
2020-02-20 13:19:23 +01:00
if (length(col_uti) == 1) {
uti <- rep(col_uti, NROW(x))
} else {
uti <- col_uti
}
} else {
# column found, transform to logical
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stop_if(
length(col_uti) != 1 | !col_uti %in% colnames(x),
"argument `uti` must be a [logical] vector, of must be a single column name of `x`"
)
2020-02-20 13:19:23 +01:00
uti <- as.logical(x[, col_uti, drop = TRUE])
}
} else {
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# col_uti is still NULL - look for specimen column and make logicals of the urines
2020-02-20 13:19:23 +01:00
col_specimen <- suppressMessages(search_type_in_df(x = x, type = "specimen"))
if (!is.null(col_specimen)) {
uti <- x[, col_specimen, drop = TRUE] %like% "urin"
values <- sort(unique(x[uti, col_specimen, drop = TRUE]))
if (length(values) > 1) {
plural <- c("s", "", "")
} else {
plural <- c("", "s", "a ")
}
2022-08-28 10:31:50 +02:00
message_(
"Assuming value", plural[1], " ",
vector_and(values, quotes = TRUE),
" in column '", font_bold(col_specimen),
"' reflect", plural[2], " ", plural[3], "urinary tract infection", plural[1],
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".\n Use `as.sir(uti = FALSE)` to prevent this."
2022-08-28 10:31:50 +02:00
)
2020-02-20 13:19:23 +01:00
} else {
# no data about UTI's found
2022-10-29 14:15:23 +02:00
uti <- NULL
2020-02-20 13:19:23 +01:00
}
}
2022-08-28 10:31:50 +02:00
2020-02-20 13:19:23 +01:00
i <- 0
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if (tryCatch(length(list(...)) > 0, error = function(e) TRUE)) {
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sel <- colnames(pm_select(x, ...))
2021-12-05 23:11:10 +01:00
} else {
sel <- colnames(x)
}
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if (!is.null(col_mo)) {
sel <- sel[sel != col_mo]
}
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ab_cols <- colnames(x)[vapply(FUN.VALUE = logical(1), x, function(y) {
2020-02-20 13:19:23 +01:00
i <<- i + 1
check <- is.mic(y) | is.disk(y)
ab <- colnames(x)[i]
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if (!is.null(col_mo) && ab == col_mo) {
return(FALSE)
}
if (!is.null(col_uti) && ab == col_uti) {
return(FALSE)
}
2020-09-24 12:38:13 +02:00
if (length(sel) == 0 || (length(sel) > 0 && ab %in% sel)) {
ab_coerced <- suppressWarnings(as.ab(ab))
if (is.na(ab_coerced) || (length(sel) > 0 & !ab %in% sel)) {
2020-09-24 12:38:13 +02:00
# not even a valid AB code
return(FALSE)
} else {
return(TRUE)
}
2020-02-20 13:19:23 +01:00
} else {
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return(FALSE)
2020-02-20 13:19:23 +01:00
}
})]
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stop_if(
length(ab_cols) == 0,
"no columns with MIC values, disk zones or antibiotic column names found in this data set. Use as.mic() or as.disk() to transform antimicrobial columns."
)
2020-02-20 13:19:23 +01:00
# set type per column
types <- character(length(ab_cols))
types[vapply(FUN.VALUE = logical(1), x.bak[, ab_cols, drop = FALSE], is.disk)] <- "disk"
types[vapply(FUN.VALUE = logical(1), x.bak[, ab_cols, drop = FALSE], is.mic)] <- "mic"
types[types == "" & vapply(FUN.VALUE = logical(1), x[, ab_cols, drop = FALSE], all_valid_disks)] <- "disk"
types[types == "" & vapply(FUN.VALUE = logical(1), x[, ab_cols, drop = FALSE], all_valid_mics)] <- "mic"
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types[types == "" & !vapply(FUN.VALUE = logical(1), x.bak[, ab_cols, drop = FALSE], is.sir)] <- "sir"
if (any(types %in% c("mic", "disk"), na.rm = TRUE)) {
2020-10-20 21:00:57 +02:00
# now we need an mo column
stop_if(is.null(col_mo), "`col_mo` must be set")
# if not null, we already found it, now find again so a message will show
if (is.null(col_mo.bak)) {
col_mo <- search_type_in_df(x = x, type = "mo")
}
x_mo <- as.mo(x[, col_mo, drop = TRUE])
}
2022-08-28 10:31:50 +02:00
2020-02-20 13:19:23 +01:00
for (i in seq_len(length(ab_cols))) {
if (types[i] == "mic") {
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x[, ab_cols[i]] <- x %pm>%
pm_pull(ab_cols[i]) %pm>%
as.character() %pm>%
as.mic() %pm>%
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as.sir(
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mo = x_mo,
mo.bak = x[, col_mo, drop = TRUE],
ab = ab_cols[i],
guideline = guideline,
uti = uti,
conserve_capped_values = conserve_capped_values,
add_intrinsic_resistance = add_intrinsic_resistance,
reference_data = reference_data,
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include_screening = include_screening,
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include_PKPD = include_PKPD,
breakpoint_type = breakpoint_type,
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is_data.frame = TRUE
)
2020-02-20 13:19:23 +01:00
} else if (types[i] == "disk") {
2023-02-09 13:07:39 +01:00
x[, ab_cols[i]] <- x %pm>%
pm_pull(ab_cols[i]) %pm>%
as.character() %pm>%
as.disk() %pm>%
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as.sir(
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mo = x_mo,
mo.bak = x[, col_mo, drop = TRUE],
ab = ab_cols[i],
guideline = guideline,
uti = uti,
add_intrinsic_resistance = add_intrinsic_resistance,
reference_data = reference_data,
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include_screening = include_screening,
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include_PKPD = include_PKPD,
breakpoint_type = breakpoint_type,
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is_data.frame = TRUE
)
2023-01-21 23:47:20 +01:00
} else if (types[i] == "sir") {
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show_message <- FALSE
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ab <- ab_cols[i]
ab_coerced <- suppressWarnings(as.ab(ab))
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if (!all(x[, ab_cols[i], drop = TRUE] %in% c("S", "I", "R", NA), na.rm = TRUE)) {
2020-12-22 00:51:17 +01:00
show_message <- TRUE
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# only print message if values are not already clean
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message_("=> Cleaning values in column '", font_bold(ab), "' (",
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ifelse(ab_coerced != toupper(ab), paste0(ab_coerced, ", "), ""),
ab_name(ab_coerced, tolower = TRUE), ")... ",
appendLF = FALSE,
as_note = FALSE
)
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} else if (!is.sir(x.bak[, ab_cols[i], drop = TRUE])) {
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show_message <- TRUE
# only print message if class not already set
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message_("=> Assigning class 'sir' to already clean column '", font_bold(ab), "' (",
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ifelse(ab_coerced != toupper(ab), paste0(ab_coerced, ", "), ""),
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ab_name(ab_coerced, tolower = TRUE, language = NULL), ")... ",
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appendLF = FALSE,
as_note = FALSE
)
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}
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x[, ab_cols[i]] <- as.sir.default(x = as.character(x[, ab_cols[i], drop = TRUE]))
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if (show_message == TRUE) {
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message_(" OK.", add_fn = list(font_green), as_note = FALSE)
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}
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}
}
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x
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}
get_guideline <- function(guideline, reference_data) {
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if (!identical(reference_data, AMR::clinical_breakpoints)) {
return(guideline)
}
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guideline_param <- toupper(guideline)
if (guideline_param %in% c("CLSI", "EUCAST")) {
guideline_param <- rev(sort(subset(reference_data, guideline %like% guideline_param)$guideline))[1L]
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}
if (guideline_param %unlike% " ") {
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# like 'EUCAST2020', should be 'EUCAST 2020'
guideline_param <- gsub("([a-z]+)([0-9]+)", "\\1 \\2", guideline_param, ignore.case = TRUE)
}
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stop_ifnot(guideline_param %in% reference_data$guideline,
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"invalid guideline: '", guideline,
"'.\nValid guidelines are: ", vector_and(reference_data$guideline, quotes = TRUE, reverse = TRUE),
call = FALSE
)
guideline_param
}
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as_sir_method <- function(method_short,
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method_long,
x,
mo,
ab,
guideline,
uti,
conserve_capped_values,
add_intrinsic_resistance,
reference_data,
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include_screening,
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include_PKPD,
breakpoint_type,
...) {
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meet_criteria(x, allow_NA = TRUE, .call_depth = -2)
meet_criteria(mo, allow_class = c("mo", "character"), allow_NULL = TRUE, .call_depth = -2)
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meet_criteria(ab, allow_class = c("ab", "character"), has_length = 1, .call_depth = -2)
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meet_criteria(guideline, allow_class = "character", has_length = 1, .call_depth = -2)
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meet_criteria(uti, allow_class = "logical", has_length = c(1, length(x)), allow_NULL = TRUE, allow_NA = TRUE, .call_depth = -2)
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meet_criteria(conserve_capped_values, allow_class = "logical", has_length = 1, .call_depth = -2)
meet_criteria(add_intrinsic_resistance, allow_class = "logical", has_length = 1, .call_depth = -2)
meet_criteria(reference_data, allow_class = "data.frame", .call_depth = -2)
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meet_criteria(include_screening, allow_class = "logical", has_length = 1, .call_depth = -2)
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meet_criteria(include_PKPD, allow_class = "logical", has_length = 1, .call_depth = -2)
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check_reference_data(reference_data, .call_depth = -2)
meet_criteria(breakpoint_type, allow_class = "character", is_in = reference_data$type, has_length = 1, .call_depth = -2)
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guideline_coerced <- get_guideline(guideline, reference_data)
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if (message_not_thrown_before("as.sir", "sir_interpretation_history")) {
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message_("Run `sir_interpretation_history()` afterwards to retrieve a logbook with all the details of the breakpoint interpretations. Note that some microorganisms might not have breakpoints for each antimicrobial drug in ", guideline_coerced, ".\n\n")
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}
# for dplyr's across()
cur_column_dplyr <- import_fn("cur_column", "dplyr", error_on_fail = FALSE)
if (!is.null(cur_column_dplyr) && tryCatch(is.data.frame(get_current_data("ab", call = 0)), error = function(e) FALSE)) {
# try to get current column, which will only be available when in across()
ab <- tryCatch(cur_column_dplyr(),
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error = function(e) ab
)
}
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# for auto-determining mo
mo_var_found <- ""
if (is.null(mo)) {
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tryCatch(
{
df <- get_current_data(arg_name = "mo", call = -3) # will return an error if not found
mo <- NULL
try(
{
mo <- suppressMessages(search_type_in_df(df, "mo"))
},
silent = TRUE
)
if (!is.null(df) && !is.null(mo) && is.data.frame(df)) {
mo_var_found <- paste0(" based on column '", font_bold(mo), "'")
mo <- df[, mo, drop = TRUE]
}
},
error = function(e) {
mo <- NULL
}
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)
}
if (is.null(mo)) {
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stop_("No information was supplied about the microorganisms (missing argument `mo` and no column of class 'mo' found). See ?as.sir.\n\n",
"To transform certain columns with e.g. mutate(), use `data %>% mutate(across(..., as.sir, mo = x))`, where x is your column with microorganisms.\n",
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"To transform all ", method_long, " in a data set, use `data %>% as.sir()` or `data %>% mutate_if(is.", method_short, ", as.sir)`.",
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call = FALSE
)
}
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if (length(ab) == 1 && ab %like% paste0("as.", method_short)) {
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stop_("No unambiguous name was supplied about the antibiotic (argument `ab`). See ?as.sir.", call = FALSE)
}
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ab.bak <- ab
ab <- suppressWarnings(as.ab(ab))
if (!is.null(list(...)$mo.bak)) {
mo.bak <- list(...)$mo.bak
} else {
mo.bak <- mo
}
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# be sure to take current taxonomy, as the 'clinical_breakpoints' data set only contains current taxonomy
mo <- suppressWarnings(suppressMessages(as.mo(mo, keep_synonyms = FALSE, info = FALSE)))
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if (is.na(ab)) {
message_("Returning NAs for unknown antibiotic: '", font_bold(ab.bak),
"'. Rename this column to a valid name or code, and check the output with `as.ab()`.",
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add_fn = font_red,
as_note = FALSE
)
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return(as.sir(rep(NA, length(x))))
}
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if (length(mo) == 1) {
mo <- rep(mo, length(x))
}
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if (is.null(uti)) {
uti <- NA
}
if (length(uti) == 1) {
uti <- rep(uti, length(x))
}
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if (isTRUE(add_intrinsic_resistance) && guideline_coerced %unlike% "EUCAST") {
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if (message_not_thrown_before("as.sir", "intrinsic")) {
warning_("in `as.sir()`: using 'add_intrinsic_resistance' is only useful when using EUCAST guidelines, since the rules for intrinsic resistance are based on EUCAST.")
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}
}
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agent_formatted <- paste0("'", font_bold(ab.bak), "'")
agent_name <- ab_name(ab, tolower = TRUE, language = NULL)
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if (generalise_antibiotic_name(ab.bak) == generalise_antibiotic_name(agent_name)) {
agent_formatted <- paste0(
agent_formatted,
" (", ab, ")"
)
} else if (generalise_antibiotic_name(ab) != generalise_antibiotic_name(agent_name)) {
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agent_formatted <- paste0(
agent_formatted,
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" (", ifelse(ab.bak == ab, "",
paste0(ab, ", ")
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), agent_name, ")"
)
}
# this intro text will also be printed in the progress bar in the `progress` package is installed
intro_txt <- paste0("Interpreting ", method_long, ": ", ifelse(isTRUE(list(...)$is_data.frame), "column ", ""),
agent_formatted,
mo_var_found,
ifelse(identical(reference_data, AMR::clinical_breakpoints),
paste0(", ", font_bold(guideline_coerced)),
""),
"... ")
message_(intro_txt, appendLF = FALSE, as_note = FALSE)
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msg_note <- function(messages) {
messages <- unique(messages)
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for (i in seq_len(length(messages))) {
messages[i] <- word_wrap(extra_indent = 5, messages[i])
}
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message(
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font_yellow_bg(paste0(" NOTE", ifelse(length(messages) > 1, "S", ""), " \n")),
paste0(" ", font_black(AMR_env$bullet_icon), " ", font_black(messages, collapse = NULL), collapse = "\n")
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)
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}
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method <- method_short
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metadata_mo <- get_mo_uncertainties()
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df <- data.frame(
values = x,
mo = mo,
result = NA_sir_,
uti = uti,
stringsAsFactors = FALSE
)
if (method == "mic") {
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# when as.sir.mic is called directly
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df$values <- as.mic(df$values)
} else if (method == "disk") {
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# when as.sir.disk is called directly
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df$values <- as.disk(df$values)
}
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df_unique <- unique(df[ , c("mo", "uti"), drop = FALSE])
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rise_warning <- FALSE
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rise_note <- FALSE
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method_coerced <- toupper(method)
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ab_coerced <- as.ab(ab)
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if (identical(reference_data, AMR::clinical_breakpoints)) {
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breakpoints <- reference_data %pm>%
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subset(guideline == guideline_coerced & method == method_coerced & ab == ab_coerced)
if (ab_coerced == "AMX" && nrow(breakpoints) == 0) {
ab_coerced <- "AMP"
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breakpoints <- reference_data %pm>%
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subset(guideline == guideline_coerced & method == method_coerced & ab == ab_coerced)
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}
} else {
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breakpoints <- reference_data %pm>%
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subset(method == method_coerced & ab == ab_coerced)
}
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breakpoints <- breakpoints %pm>%
subset(type == breakpoint_type)
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if (isFALSE(include_screening)) {
# remove screening rules from the breakpoints table
breakpoints <- breakpoints %pm>%
subset(site %unlike% "screen" & ref_tbl %unlike% "screen")
}
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if (isFALSE(include_PKPD)) {
# remove PKPD rules from the breakpoints table
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breakpoints <- breakpoints %pm>%
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subset(mo != "UNKNOWN" & ref_tbl %unlike% "PK.*PD")
}
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msgs <- character(0)
if (nrow(breakpoints) == 0) {
# apparently no breakpoints found
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message(
paste0(font_rose_bg(" WARNING "), "\n"),
font_black(paste0(" ", AMR_env$bullet_icon, " No ", method_coerced, " breakpoints available for ",
suppressMessages(suppressWarnings(ab_name(ab_coerced, language = NULL, tolower = TRUE))),
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" (", ab_coerced, ").")))
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load_mo_uncertainties(metadata_mo)
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return(rep(NA_sir_, nrow(df)))
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}
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if (guideline_coerced %like% "EUCAST") {
any_is_intrinsic_resistant <- FALSE
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add_intrinsic_resistance_to_AMR_env()
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}
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p <- progress_ticker(n = nrow(df_unique), n_min = 10, title = font_blue(intro_txt), only_bar_percent = TRUE)
has_progress_bar <- !is.null(import_fn("progress_bar", "progress", error_on_fail = FALSE)) && nrow(df_unique) >= 10
on.exit(close(p))
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# run the rules
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for (i in seq_len(nrow(df_unique))) {
p$tick()
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mo_current <- df_unique[i, "mo", drop = TRUE]
uti_current <- df_unique[i, "uti", drop = TRUE]
if (is.na(uti_current)) {
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# no preference, so no filter on UTIs
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rows <- which(df$mo == mo_current)
} else {
rows <- which(df$mo == mo_current & df$uti == uti_current)
}
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values <- df[rows, "values", drop = TRUE]
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new_sir <- rep(NA_sir_, length(rows))
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# find different mo properties, as fast as possible
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mo_current_genus <- AMR_env$MO_lookup$mo[match(AMR_env$MO_lookup$genus[match(mo_current, AMR_env$MO_lookup$mo)], AMR_env$MO_lookup$fullname)]
mo_current_family <- AMR_env$MO_lookup$mo[match(AMR_env$MO_lookup$family[match(mo_current, AMR_env$MO_lookup$mo)], AMR_env$MO_lookup$fullname)]
mo_current_order <- AMR_env$MO_lookup$mo[match(AMR_env$MO_lookup$order[match(mo_current, AMR_env$MO_lookup$mo)], AMR_env$MO_lookup$fullname)]
mo_current_class <- AMR_env$MO_lookup$mo[match(AMR_env$MO_lookup$class[match(mo_current, AMR_env$MO_lookup$mo)], AMR_env$MO_lookup$fullname)]
mo_current_rank <- AMR_env$MO_lookup$rank[match(mo_current, AMR_env$MO_lookup$mo)]
mo_current_name <- AMR_env$MO_lookup$fullname[match(mo_current, AMR_env$MO_lookup$mo)]
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if (mo_current %in% AMR::microorganisms.groups$mo) {
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# get the species group (might be more than 1 entry)
mo_current_species_group <- AMR::microorganisms.groups$mo_group[which(AMR::microorganisms.groups$mo == mo_current)]
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} else {
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mo_current_species_group <- NULL
}
mo_current_other <- structure("UNKNOWN", class = c("mo", "character"))
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# formatted for notes
mo_formatted <- mo_current_name
if (!mo_current_rank %in% c("kingdom", "phylum", "class", "order")) {
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mo_formatted <- font_italic(mo_formatted)
}
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ab_formatted <- paste0(
suppressMessages(suppressWarnings(ab_name(ab_coerced, language = NULL, tolower = TRUE))),
" (", ab_coerced, ")"
)
# gather all available breakpoints for current MO and sort on taxonomic rank
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# (this will prefer species breakpoints over order breakpoints)
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breakpoints_current <- breakpoints %pm>%
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subset(mo %in% c(
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mo_current, mo_current_genus, mo_current_family,
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mo_current_order, mo_current_class,
mo_current_species_group,
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mo_current_other
))
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if (is.na(unique(uti_current))) {
breakpoints_current <- breakpoints_current %pm>%
# this will put UTI = FALSE first, then UTI = TRUE, then UTI = NA
pm_arrange(rank_index, uti) # 'uti' is a column in data set 'clinical_breakpoints'
} else if (unique(uti_current) == TRUE) {
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breakpoints_current <- breakpoints_current %pm>%
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subset(uti == TRUE) %pm>%
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# be as specific as possible (i.e. prefer species over genus):
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pm_arrange(rank_index)
} else if (unique(uti_current) == FALSE) {
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breakpoints_current <- breakpoints_current %pm>%
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subset(uti == FALSE) %pm>%
# be as specific as possible (i.e. prefer species over genus):
pm_arrange(rank_index)
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}
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# throw notes for different body sites
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site <- breakpoints_current[1L, "site", drop = FALSE] # this is the one we'll take
if (is.na(site)) {
site <- paste0("an unspecified body site")
} else {
site <- paste0("body site '", site, "'")
}
if (nrow(breakpoints_current) == 1 && all(breakpoints_current$uti == TRUE) && any(uti_current %in% c(FALSE, NA)) && message_not_thrown_before("as.sir", "uti", ab_coerced)) {
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# only UTI breakpoints available
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warning_("in `as.sir()`: interpretation of ", font_bold(ab_formatted), " is only available for (uncomplicated) urinary tract infections (UTI) for some microorganisms, thus assuming `uti = TRUE`. See `?as.sir`.")
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rise_warning <- TRUE
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} else if (nrow(breakpoints_current) > 1 && length(unique(breakpoints_current$site)) > 1 && any(is.na(uti_current)) && all(c(TRUE, FALSE) %in% breakpoints_current$uti, na.rm = TRUE) && message_not_thrown_before("as.sir", "siteUTI", mo_current, ab_coerced)) {
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# both UTI and Non-UTI breakpoints available
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msgs <- c(msgs, paste0("Breakpoints for UTI ", font_underline("and"), " non-UTI available for ", ab_formatted, " in ", mo_formatted, " - assuming ", site, ". Use argument `uti` to set which isolates are from urine. See `?as.sir`."))
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breakpoints_current <- breakpoints_current %pm>%
pm_filter(uti == FALSE)
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} else if (nrow(breakpoints_current) > 1 && length(unique(breakpoints_current$site)) > 1 && all(breakpoints_current$uti == FALSE, na.rm = TRUE) && message_not_thrown_before("as.sir", "siteOther", mo_current, ab_coerced)) {
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# breakpoints for multiple body sites available
msgs <- c(msgs, paste0("Multiple breakpoints available for ", ab_formatted, " in ", mo_formatted, " - assuming ", site, "."))
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} else if (nrow(breakpoints_current) == 0) {
# # do not note - it's already in the header before the interpretation starts
next
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}
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# first check if mo is intrinsic resistant
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if (isTRUE(add_intrinsic_resistance) && guideline_coerced %like% "EUCAST" && paste(mo_current, ab_coerced) %in% AMR_env$intrinsic_resistant) {
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msgs <- c(msgs, paste0("Intrinsic resistance applied for ", ab_formatted, " in ", mo_formatted, ""))
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new_sir <- rep(as.sir("R"), length(rows))
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} else if (nrow(breakpoints_current) == 0) {
# no rules available
new_sir <- rep(NA_sir_, length(rows))
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} else {
# then run the rules
breakpoints_current <- breakpoints_current[1L, , drop = FALSE]
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if (any(breakpoints_current$mo == "UNKNOWN", na.rm = TRUE) | any(breakpoints_current$ref_tbl %like% "PK.*PD", na.rm = TRUE)) {
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msgs <- c(msgs, "Some PK/PD breakpoints were applied - use `include_PKPD = FALSE` to prevent this")
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}
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if (any(breakpoints_current$site %like% "screen", na.rm = TRUE) | any(breakpoints_current$ref_tbl %like% "screen", na.rm = TRUE)) {
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msgs <- c(msgs, "Some screening breakpoints were applied - use `include_screening = FALSE` to prevent this")
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}
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if (method == "mic") {
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new_sir <- case_when_AMR(
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is.na(values) ~ NA_sir_,
values <= breakpoints_current$breakpoint_S ~ as.sir("S"),
guideline_coerced %like% "EUCAST" & values > breakpoints_current$breakpoint_R ~ as.sir("R"),
guideline_coerced %like% "CLSI" & values >= breakpoints_current$breakpoint_R ~ as.sir("R"),
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# return "I" when breakpoints are in the middle
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!is.na(breakpoints_current$breakpoint_S) & !is.na(breakpoints_current$breakpoint_R) ~ as.sir("I"),
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# and NA otherwise
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TRUE ~ NA_sir_
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)
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} else if (method == "disk") {
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new_sir <- case_when_AMR(
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is.na(values) ~ NA_sir_,
as.double(values) >= as.double(breakpoints_current$breakpoint_S) ~ as.sir("S"),
guideline_coerced %like% "EUCAST" & as.double(values) < as.double(breakpoints_current$breakpoint_R) ~ as.sir("R"),
guideline_coerced %like% "CLSI" & as.double(values) <= as.double(breakpoints_current$breakpoint_R) ~ as.sir("R"),
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# return "I" when breakpoints are in the middle
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!is.na(breakpoints_current$breakpoint_S) & !is.na(breakpoints_current$breakpoint_R) ~ as.sir("I"),
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# and NA otherwise
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TRUE ~ NA_sir_
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)
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}
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# write to verbose output
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AMR_env$sir_interpretation_history <- rbind_AMR(
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AMR_env$sir_interpretation_history,
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# recycling 1 to 2 rows does not seem to work, which is why rep() was added
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data.frame(
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datetime = rep(Sys.time(), length(rows)),
index = rows,
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ab_user = rep(ab.bak, length(rows)),
mo_user = rep(mo.bak[match(mo_current, df$mo)][1], length(rows)),
ab = rep(ab_coerced, length(rows)),
mo = rep(breakpoints_current[, "mo", drop = TRUE], length(rows)),
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input = as.double(values),
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outcome = as.sir(new_sir),
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method = rep(method_coerced, length(rows)),
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breakpoint_S_R = rep(paste0(breakpoints_current[, "breakpoint_S", drop = TRUE], "-", breakpoints_current[, "breakpoint_R", drop = TRUE]), length(rows)),
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guideline = rep(guideline_coerced, length(rows)),
ref_table = rep(breakpoints_current[, "ref_tbl", drop = TRUE], length(rows)),
uti = rep(breakpoints_current[, "uti", drop = TRUE], length(rows)),
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stringsAsFactors = FALSE
)
)
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}
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df[rows, "result"] <- new_sir
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}
close(p)
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# printing messages
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if (has_progress_bar == TRUE) {
# the progress bar has overwritten the intro text, so:
message_(intro_txt, appendLF = FALSE, as_note = FALSE)
}
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if (isTRUE(rise_warning)) {
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message(font_rose_bg(" WARNING "))
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} else if (length(msgs) == 0) {
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message(font_green_bg(" OK "))
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} else {
msg_note(sort(msgs))
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}
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load_mo_uncertainties(metadata_mo)
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df$result
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}
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#' @rdname as.sir
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#' @param clean a [logical] to indicate whether previously stored results should be forgotten after returning the 'logbook' with results
#' @export
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sir_interpretation_history <- function(clean = FALSE) {
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meet_criteria(clean, allow_class = "logical", has_length = 1)
out <- AMR_env$sir_interpretation_history
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if (NROW(out) == 0) {
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message_("No results to return. Run `as.sir()` on MIC values or disk diffusion zones first to see a 'logbook' data set here.")
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return(invisible(NULL))
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}
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out$outcome <- as.sir(out$outcome)
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# keep stored for next use
if (isTRUE(clean)) {
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AMR_env$sir_interpretation_history <- AMR_env$sir_interpretation_history[0, , drop = FALSE]
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}
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# sort descending on time
out <- out[order(out$datetime, decreasing = TRUE), , drop = FALSE]
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if (pkg_is_available("tibble")) {
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import_fn("as_tibble", "tibble")(out)
} else {
out
}
}
# will be exported using s3_register() in R/zzz.R
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pillar_shaft.sir <- function(x, ...) {
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out <- trimws(format(x))
if (has_colour()) {
# colours will anyway not work when has_colour() == FALSE,
# but then the indentation should also not be applied
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out[is.na(x)] <- font_grey(" NA")
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out[x == "S"] <- font_green_bg(" S ")
out[x == "I"] <- font_orange_bg(" I ")
if (is_dark()) {
out[x == "R"] <- font_red_bg(" R ")
} else {
out[x == "R"] <- font_rose_bg(" R ")
}
}
create_pillar_column(out, align = "left", width = 5)
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}
# will be exported using s3_register() in R/zzz.R
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type_sum.sir <- function(x, ...) {
"sir"
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}
# will be exported using s3_register() in R/zzz.R
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freq.sir <- function(x, ...) {
x_name <- deparse(substitute(x))
x_name <- gsub(".*[$]", "", x_name)
if (x_name %in% c("x", ".")) {
# try again going through system calls
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x_name <- stats::na.omit(vapply(
FUN.VALUE = character(1),
sys.calls(),
function(call) {
call_txt <- as.character(call)
ifelse(call_txt[1] %like% "freq$", call_txt[length(call_txt)], character(0))
}
))[1L]
}
ab <- suppressMessages(suppressWarnings(as.ab(x_name)))
digits <- list(...)$digits
if (is.null(digits)) {
digits <- 2
}
if (!is.na(ab)) {
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cleaner::freq.default(
x = x, ...,
.add_header = list(
Drug = paste0(ab_name(ab, language = NULL), " (", ab, ", ", paste(ab_atc(ab), collapse = "/"), ")"),
`Drug group` = ab_group(ab, language = NULL),
`%SI` = trimws(percentage(susceptibility(x, minimum = 0, as_percent = FALSE),
digits = digits
))
)
)
} else {
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cleaner::freq.default(
x = x, ...,
.add_header = list(
`%SI` = trimws(percentage(susceptibility(x, minimum = 0, as_percent = FALSE),
digits = digits
))
)
)
}
}
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# will be exported using s3_register() in R/zzz.R
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get_skimmers.sir <- function(column) {
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# get the variable name 'skim_variable'
name_call <- function(.data) {
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calls <- sys.calls()
frms <- sys.frames()
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calls_txt <- vapply(calls, function(x) paste(deparse(x), collapse = ""), FUN.VALUE = character(1))
if (any(calls_txt %like% "skim_variable", na.rm = TRUE)) {
ind <- which(calls_txt %like% "skim_variable")[1L]
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vars <- tryCatch(eval(parse(text = ".data$skim_variable$sir"), envir = frms[[ind]]),
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error = function(e) NULL
)
tryCatch(ab_name(as.character(calls[[length(calls)]][[2]]), language = NULL),
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error = function(e) NA_character_
)
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} else {
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NA_character_
}
}
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skimr::sfl(
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skim_type = "sir",
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ab_name = name_call,
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count_R = count_R,
count_S = count_susceptible,
count_I = count_I,
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prop_R = ~ proportion_R(., minimum = 0),
prop_S = ~ susceptibility(., minimum = 0),
prop_I = ~ proportion_I(., minimum = 0)
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)
}
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#' @method print sir
#' @export
#' @noRd
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print.sir <- function(x, ...) {
cat("Class 'sir'\n")
print(as.character(x), quote = FALSE)
}
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#' @method droplevels sir
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#' @export
#' @noRd
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droplevels.sir <- function(x, exclude = if (any(is.na(levels(x)))) NULL else NA, ...) {
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x <- droplevels.factor(x, exclude = exclude, ...)
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class(x) <- c("sir", "ordered", "factor")
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x
}
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#' @method summary sir
#' @export
#' @noRd
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summary.sir <- function(object, ...) {
x <- object
n <- sum(!is.na(x))
S <- sum(x == "S", na.rm = TRUE)
I <- sum(x == "I", na.rm = TRUE)
R <- sum(x == "R", na.rm = TRUE)
pad <- function(x) {
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if (is.na(x)) {
return("??")
}
if (x == "0%") {
x <- " 0.0%"
}
if (nchar(x) < 5) {
x <- paste0(rep(" ", 5 - nchar(x)), x)
}
x
}
value <- c(
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"Class" = "sir",
"%R" = paste0(pad(percentage(R / n, digits = 1)), " (n=", R, ")"),
"%SI" = paste0(pad(percentage((S + I) / n, digits = 1)), " (n=", S + I, ")"),
"- %S" = paste0(pad(percentage(S / n, digits = 1)), " (n=", S, ")"),
"- %I" = paste0(pad(percentage(I / n, digits = 1)), " (n=", I, ")")
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)
class(value) <- c("summaryDefault", "table")
value
}
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#' @method [<- sir
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#' @export
#' @noRd
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"[<-.sir" <- function(i, j, ..., value) {
value <- as.sir(value)
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y <- NextMethod()
attributes(y) <- attributes(i)
y
}
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#' @method [[<- sir
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#' @export
#' @noRd
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"[[<-.sir" <- function(i, j, ..., value) {
value <- as.sir(value)
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y <- NextMethod()
attributes(y) <- attributes(i)
y
}
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#' @method c sir
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#' @export
#' @noRd
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c.sir <- function(...) {
as.sir(unlist(lapply(list(...), as.character)))
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}
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#' @method unique sir
#' @export
#' @noRd
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unique.sir <- function(x, incomparables = FALSE, ...) {
y <- NextMethod()
attributes(y) <- attributes(x)
y
}
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#' @method rep sir
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#' @export
#' @noRd
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rep.sir <- function(x, ...) {
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y <- NextMethod()
attributes(y) <- attributes(x)
y
}
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check_reference_data <- function(reference_data, .call_depth) {
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if (!identical(reference_data, AMR::clinical_breakpoints)) {
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class_sir <- vapply(FUN.VALUE = character(1), AMR::clinical_breakpoints, function(x) paste0("<", class(x), ">", collapse = " and "))
class_ref <- vapply(FUN.VALUE = character(1), reference_data, function(x) paste0("<", class(x), ">", collapse = " and "))
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if (!all(names(class_sir) == names(class_ref))) {
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stop_("`reference_data` must have the same column names as the 'clinical_breakpoints' data set.", call = .call_depth)
}
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if (!all(class_sir == class_ref)) {
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stop_("`reference_data` must be the same structure as the 'clinical_breakpoints' data set. Column '", names(class_ref[class_sir != class_ref][1]), "' is of class ", class_ref[class_sir != class_ref][1], ", but should be of class ", class_sir[class_sir != class_ref][1], ".", call = .call_depth)
}
}
}