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AMR/R/resistance.R

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# ==================================================================== #
# TITLE #
# Antimicrobial Resistance (AMR) Analysis #
# #
# AUTHORS #
# Berends MS (m.s.berends@umcg.nl), Luz CF (c.f.luz@umcg.nl) #
# #
# LICENCE #
# This program is free software; you can redistribute it and/or modify #
# it under the terms of the GNU General Public License version 2.0, #
# as published by the Free Software Foundation. #
# #
# This program is distributed in the hope that it will be useful, #
# but WITHOUT ANY WARRANTY; without even the implied warranty of #
# MERCHANTABILITY or FITNESS FOR A PARTICULAR PURPOSE. See the #
# GNU General Public License for more details. #
# ==================================================================== #
#' Calculate resistance of isolates
#'
#' These functions can be used to calculate the (co-)resistance of microbial isolates (i.e. percentage S, SI, I, IR or R). All functions can be used in \code{dplyr}s \code{\link[dplyr]{summarise}} and support grouped variables, see \emph{Examples}.
#' @param ab,ab1,ab2 vector of antibiotic interpretations, they will be transformed internally with \code{\link{as.rsi}}
#' @param include_I logical to indicate whether antimicrobial interpretations of "I" should be included
#' @param minimum minimal amount of available isolates. Any number lower than \code{minimum} will return \code{NA}.
#' @param as_percent logical to indicate whether the output must be returned as percent (text), will else be a double
#' @param interpretation antimicrobial interpretation
#' @details \strong{Remember that you should filter your table to let it contain only first isolates!} Use \code{\link{first_isolate}} to determine them in your data set.
#'
#' All return values are calculated using hybrid evaluation (i.e. using C++), which makes these functions 60-65 times faster than in \code{AMR} v0.2.0 and below. The \code{rsi} function is available for backwards compatibility and deprecated. It now uses the \code{resistance} and \code{susceptibility} functions internally, based on the \code{interpretation} parameter.
#' \if{html}{
#' \cr
#' To calculate the probability (\emph{p}) of susceptibility of one antibiotic, we use this formula:
#' \out{<div style="text-align: center">}\figure{mono_therapy.png}\out{</div>}
#' To calculate the probability (\emph{p}) of susceptibility of more antibiotics (i.e. combination therapy), we need to check whether one of them has a susceptible result (as numerator) and count all cases where all antibiotics were tested (as denominator). \cr
#' \cr
#' For two antibiotics:
#' \out{<div style="text-align: center">}\figure{combi_therapy_2.png}\out{</div>}
#' \cr
#' Theoretically for three antibiotics:
#' \out{<div style="text-align: center">}\figure{combi_therapy_3.png}\out{</div>}
#' }
#' @keywords resistance susceptibility rsi_df antibiotics isolate isolates
#' @return Double or, when \code{as_percent = TRUE}, a character.
#' @rdname resistance
#' @export
#' @examples
#' library(dplyr)
#'
#' septic_patients %>%
#' group_by(hospital_id) %>%
#' summarise(p = susceptibility(cipr),
#' n = n_rsi(cipr)) # n_rsi works like n_distinct in dplyr
#'
#' septic_patients %>%
#' group_by(hospital_id) %>%
#' summarise(cipro_p = susceptibility(cipr, as_percent = TRUE),
#' cipro_n = n_rsi(cipr),
#' genta_p = susceptibility(gent, as_percent = TRUE),
#' genta_n = n_rsi(gent),
#' combination_p = susceptibility(cipr, gent, as_percent = TRUE),
#' combination_n = n_rsi(cipr, gent))
#'
#'
#' # Calculate resistance
#' resistance(septic_patients$amox)
#' rsi(septic_patients$amox, interpretation = "IR") # deprecated
#'
#' # Or susceptibility
#' susceptibility(septic_patients$amox)
#' rsi(septic_patients$amox, interpretation = "S") # deprecated
#'
#'
#' # Calculate co-resistance between amoxicillin/clav acid and gentamicin,
#' # so we can see that combination therapy does a lot more than mono therapy:
#' susceptibility(septic_patients$amcl) # p = 67.8%
#' n_rsi(septic_patients$amcl) # n = 1641
#'
#' susceptibility(septic_patients$gent) # p = 69.1%
#' n_rsi(septic_patients$gent) # n = 1863
#'
#' with(septic_patients,
#' susceptibility(amcl, gent)) # p = 90.6%
#' with(septic_patients,
#' n_rsi(amcl, gent)) # n = 1580
#'
#' \dontrun{
#' # calculate current empiric combination therapy of Helicobacter gastritis:
#' my_table %>%
#' filter(first_isolate == TRUE,
#' genus == "Helicobacter") %>%
#' summarise(p = susceptibility(amox, metr), # amoxicillin with metronidazole
#' n = n_rsi(amox, metr))
#' }
resistance <- function(ab,
include_I = TRUE,
minimum = 30,
as_percent = FALSE) {
if (NCOL(ab) > 1) {
stop('`ab` must be a vector of antimicrobial interpretations', call. = FALSE)
}
if (!is.logical(include_I)) {
stop('`include_I` must be logical', call. = FALSE)
}
if (!is.numeric(minimum)) {
stop('`minimum` must be numeric', call. = FALSE)
}
if (!is.logical(as_percent)) {
stop('`as_percent` must be logical', call. = FALSE)
}
x <- as.integer(as.rsi(ab))
total <- .Call(`_AMR_rsi_calc_total`, x)
if (total < minimum) {
return(NA)
}
found <- .Call(`_AMR_rsi_calc_R`, x, include_I)
if (as_percent == TRUE) {
percent(found / total, force_zero = TRUE)
} else {
found / total
}
}
#' @rdname resistance
#' @export
susceptibility <- function(ab1,
ab2 = NULL,
include_I = FALSE,
minimum = 30,
as_percent = FALSE) {
if (NCOL(ab1) > 1) {
stop('`ab1` must be a vector of antimicrobial interpretations', call. = FALSE)
}
if (!is.logical(include_I)) {
stop('`include_I` must be logical', call. = FALSE)
}
if (!is.numeric(minimum)) {
stop('`minimum` must be numeric', call. = FALSE)
}
if (!is.logical(as_percent)) {
stop('`as_percent` must be logical', call. = FALSE)
}
if (!is.null(ab2)) {
if (NCOL(ab2) > 1) {
stop('`ab2` must be a vector of antimicrobial interpretations', call. = FALSE)
}
x <- apply(X = data.frame(ab1 = as.integer(as.rsi(ab1)),
ab2 = as.integer(as.rsi(ab2))),
MARGIN = 1,
FUN = min)
} else {
x <- as.integer(as.rsi(ab1))
}
total <- .Call(`_AMR_rsi_calc_total`, x)
if (total < minimum) {
return(NA)
}
found <- .Call(`_AMR_rsi_calc_S`, x, include_I)
if (as_percent == TRUE) {
percent(found / total, force_zero = TRUE)
} else {
found / total
}
}
#' @rdname resistance
#' @export
n_rsi <- function(ab1, ab2 = NULL) {
if (NCOL(ab1) > 1) {
stop('`ab1` must be a vector of antimicrobial interpretations', call. = FALSE)
}
if (!is.null(ab2)) {
if (NCOL(ab2) > 1) {
stop('`ab2` must be a vector of antimicrobial interpretations', call. = FALSE)
}
x <- apply(X = data.frame(ab1 = as.integer(as.rsi(ab1)),
ab2 = as.integer(as.rsi(ab2))),
MARGIN = 1,
FUN = min)
} else {
x <- as.integer(as.rsi(ab1))
}
.Call(`_AMR_rsi_calc_total`, x)
}
#' @rdname resistance
#' @export
rsi <- function(ab1,
ab2 = NULL,
interpretation = "IR",
minimum = 30,
as_percent = FALSE) {
warning("'rsi' is deprecated. Use 'resistance' or 'susceptibility' instead.", call. = FALSE)
if (interpretation %in% c('IR', 'RI')) {
resistance(ab = ab1, include_I = TRUE, minimum = minimum, as_percent = as_percent)
} else if (interpretation == 'R') {
resistance(ab = ab1, include_I = FALSE, minimum = minimum, as_percent = as_percent)
} else if (interpretation %in% c('IS', 'SI')) {
susceptibility(ab1 = ab1, ab2 = ab2, include_I = TRUE, minimum = minimum, as_percent = as_percent)
} else if (interpretation == 'S') {
susceptibility(ab1 = ab1, ab2 = ab2, include_I = FALSE, minimum = minimum, as_percent = as_percent)
} else {
stop('invalid `interpretation`')
}
}
#' Predict antimicrobial resistance
#'
#' Create a prediction model to predict antimicrobial resistance for the next years on statistical solid ground. Standard errors (SE) will be returned as columns \code{se_min} and \code{se_max}. See Examples for a real live example.
#' @param tbl table that contains columns \code{col_ab} and \code{col_date}
#' @param col_ab column name of \code{tbl} with antimicrobial interpretations (\code{R}, \code{I} and \code{S}), supports tidyverse-like quotation
#' @param col_date column name of the date, will be used to calculate years if this column doesn't consist of years already, supports tidyverse-like quotation
#' @param year_max highest year to use in the prediction model, deafults to 15 years after today
#' @param year_every unit of sequence between lowest year found in the data and \code{year_max}
#' @param model the statistical model of choice. Valid values are \code{"binomial"} (or \code{"binom"} or \code{"logit"}) or \code{"loglin"} or \code{"linear"} (or \code{"lin"}).
#' @param I_as_R treat \code{I} as \code{R}
#' @param preserve_measurements overwrite predictions of years that are actually available in the data, with the original data. The standard errors of those years will be \code{NA}.
#' @param info print textual analysis with the name and \code{\link{summary}} of the model.
#' @return \code{data.frame} with columns \code{year}, \code{probR}, \code{se_min} and \code{se_max}.
#' @seealso \code{\link{resistance}} \cr \code{\link{lm}} \code{\link{glm}}
#' @rdname resistance_predict
#' @export
#' @importFrom dplyr %>% pull mutate group_by_at summarise filter
#' @importFrom reshape2 dcast
#' @examples
#' \dontrun{
#' # use it directly:
#' rsi_predict(tbl = tbl[which(first_isolate == TRUE & genus == "Haemophilus"),],
#' col_ab = "amcl", col_date = "date")
#'
#' # or with dplyr so you can actually read it:
#' library(dplyr)
#' tbl %>%
#' filter(first_isolate == TRUE,
#' genus == "Haemophilus") %>%
#' rsi_predict(amcl, date)
#' }
#'
#'
#' # real live example:
#' library(dplyr)
#' septic_patients %>%
#' # get bacteria properties like genus and species
#' left_join_microorganisms("bactid") %>%
#' # calculate first isolates
#' mutate(first_isolate =
#' first_isolate(.,
#' "date",
#' "patient_id",
#' "bactid",
#' col_specimen = NA,
#' col_icu = NA)) %>%
#' # filter on first E. coli isolates
#' filter(genus == "Escherichia",
#' species == "coli",
#' first_isolate == TRUE) %>%
#' # predict resistance of cefotaxime for next years
#' rsi_predict(col_ab = "cfot",
#' col_date = "date",
#' year_max = 2025,
#' preserve_measurements = FALSE)
#'
resistance_predict <- function(tbl,
col_ab,
col_date,
year_max = as.integer(format(as.Date(Sys.Date()), '%Y')) + 15,
year_every = 1,
model = 'binomial',
I_as_R = TRUE,
preserve_measurements = TRUE,
info = TRUE) {
if (nrow(tbl) == 0) {
stop('This table does not contain any observations.')
}
if (!col_ab %in% colnames(tbl)) {
stop('Column ', col_ab, ' not found.')
}
if (!col_date %in% colnames(tbl)) {
stop('Column ', col_date, ' not found.')
}
if ('grouped_df' %in% class(tbl)) {
# no grouped tibbles please, mutate will throw errors
tbl <- base::as.data.frame(tbl, stringsAsFactors = FALSE)
}
if (I_as_R == TRUE) {
tbl[, col_ab] <- gsub('I', 'R', tbl %>% pull(col_ab))
}
if (!all(tbl %>% pull(col_ab) %>% as.rsi() %in% c(NA, 'S', 'I', 'R'))) {
stop('Column ', col_ab, ' must contain antimicrobial interpretations (S, I, R).')
}
year <- function(x) {
if (all(grepl('^[0-9]{4}$', x))) {
x
} else {
as.integer(format(as.Date(x), '%Y'))
}
}
years_predict <- seq(from = min(year(tbl %>% pull(col_date))), to = year_max, by = year_every)
df <- tbl %>%
mutate(year = year(tbl %>% pull(col_date))) %>%
group_by_at(c('year', col_ab)) %>%
summarise(n())
colnames(df) <- c('year', 'antibiotic', 'count')
df <- df %>%
reshape2::dcast(year ~ antibiotic, value.var = 'count')
if (model %in% c('binomial', 'binom', 'logit')) {
logitmodel <- with(df, glm(cbind(R, S) ~ year, family = binomial))
if (info == TRUE) {
cat('\nLogistic regression model (logit) with binomial distribution')
cat('\n------------------------------------------------------------\n')
print(summary(logitmodel))
}
predictmodel <- stats::predict(logitmodel, newdata = with(df, list(year = years_predict)), type = "response", se.fit = TRUE)
prediction <- predictmodel$fit
se <- predictmodel$se.fit
} else if (model == 'loglin') {
loglinmodel <- with(df, glm(R ~ year, family = poisson))
if (info == TRUE) {
cat('\nLog-linear regression model (loglin) with poisson distribution')
cat('\n--------------------------------------------------------------\n')
print(summary(loglinmodel))
}
predictmodel <- stats::predict(loglinmodel, newdata = with(df, list(year = years_predict)), type = "response", se.fit = TRUE)
prediction <- predictmodel$fit
se <- predictmodel$se.fit
} else if (model %in% c('lin', 'linear')) {
linmodel <- with(df, lm((R / (R + S)) ~ year))
if (info == TRUE) {
cat('\nLinear regression model')
cat('\n-----------------------\n')
print(summary(linmodel))
}
predictmodel <- stats::predict(linmodel, newdata = with(df, list(year = years_predict)), se.fit = TRUE)
prediction <- predictmodel$fit
se <- predictmodel$se.fit
} else {
stop('No valid model selected.')
}
# prepare the output dataframe
prediction <- data.frame(year = years_predict, probR = prediction, stringsAsFactors = FALSE)
prediction$se_min <- prediction$probR - se
prediction$se_max <- prediction$probR + se
if (model == 'loglin') {
prediction$probR <- prediction$probR %>%
format(scientific = FALSE) %>%
as.integer()
prediction$se_min <- prediction$se_min %>% as.integer()
prediction$se_max <- prediction$se_max %>% as.integer()
colnames(prediction) <- c('year', 'amountR', 'se_max', 'se_min')
} else {
prediction$se_max[which(prediction$se_max > 1)] <- 1
}
prediction$se_min[which(prediction$se_min < 0)] <- 0
total <- prediction
if (preserve_measurements == TRUE) {
# geschatte data vervangen door gemeten data
if (I_as_R == TRUE) {
if (!'I' %in% colnames(df)) {
df$I <- 0
}
df$probR <- df$R / rowSums(df[, c('R', 'S', 'I')])
} else {
df$probR <- df$R / rowSums(df[, c('R', 'S')])
}
measurements <- data.frame(year = df$year,
probR = df$probR,
se_min = NA,
se_max = NA,
stringsAsFactors = FALSE)
colnames(measurements) <- colnames(prediction)
prediction <- prediction %>% filter(!year %in% df$year)
total <- rbind(measurements, prediction)
}
total
}
#' @rdname resistance_predict
#' @export
rsi_predict <- resistance_predict
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