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Introduction to ampir
In ampir: Predict Antimicrobial Peptides
knitr::opts_chunk$set(
collapse = TRUE,
comment = "#>"
)
Background
The ampir (short for antimicrobial peptide prediction in r ) package was designed to be a fast and user-friendly method to predict antimicrobial peptides (AMPs) from any given size protein dataset. ampir uses a supervised statistical machine learning approach to predict AMPs. It incorporates two support vector machine classification models, "precursor" and "mature" that have been trained on publicly available antimicrobial peptide data. The default model, "precursor" is best suited for full length proteins and the "mature" model is best suited for small mature proteins (<60 amino acids). ampir also accepts custom (user trained) models based on the caret package. Please see the ampir "How to train your model" vignette for details.
Usage
Standard input to ampir is a data.frame with sequence names in the first column and protein sequences in the second column.
library(ampir)
Read in a FASTA formatted file as a data.frame with read_faa()
my_protein_df <- read_faa(system.file("extdata/little_test.fasta", package = "ampir"))
display_df <- my_protein_df
display_df$seq_aa <- paste(substring(display_df$seq_aa,1,45),"...",sep="")
knitr::kable(display_df)
Calculate the probability that each protein is an antimicrobial peptide with predict_amps() using the default "precursor" model.
Note that amino acid sequences that are shorter than 10 amino acids long and/or contain anything other than the standard 20 amino acids are not evaluated and will contain an NA as their prob_AMP value.
my_prediction <- predict_amps(my_protein_df, model = "precursor")
my_prediction$seq_aa <- paste(substring(my_prediction$seq_aa,1,45),"...",sep="")
knitr::kable(my_prediction, digits = 3)
Predicted proteins with a specified predicted probability value could then be extracted and written to a FASTA file:
my_predicted_amps <- my_protein_df[my_prediction$prob_AMP > 0.8,]
my_predicted_amps$seq_aa <- paste(substring(my_predicted_amps$seq_aa,1,45),"...",sep="")
knitr::kable(my_predicted_amps)
Write the data.frame with sequence names in the first column and protein sequences in the second column to a FASTA formatted file with df_to_faa()
df_to_faa(my_predicted_amps, tempfile("my_predicted_amps.fasta", tempdir()))
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ampir documentation built on June 29, 2021, 9:09 a.m.
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knitr::opts_chunk$set( collapse = TRUE, comment = "#>" )
Background
The ampir (short for antimicrobial peptide prediction in r ) package was designed to be a fast and user-friendly method to predict antimicrobial peptides (AMPs) from any given size protein dataset. ampir uses a supervised statistical machine learning approach to predict AMPs. It incorporates two support vector machine classification models, "precursor" and "mature" that have been trained on publicly available antimicrobial peptide data. The default model, "precursor" is best suited for full length proteins and the "mature" model is best suited for small mature proteins (<60 amino acids). ampir also accepts custom (user trained) models based on the caret package. Please see the ampir "How to train your model" vignette for details.
Usage
Standard input to ampir is a data.frame with sequence names in the first column and protein sequences in the second column.
library(ampir)
Read in a FASTA formatted file as a data.frame with read_faa()
my_protein_df <- read_faa(system.file("extdata/little_test.fasta", package = "ampir"))
display_df <- my_protein_df display_df$seq_aa <- paste(substring(display_df$seq_aa,1,45),"...",sep="") knitr::kable(display_df)
Calculate the probability that each protein is an antimicrobial peptide with predict_amps() using the default "precursor" model.
Note that amino acid sequences that are shorter than 10 amino acids long and/or contain anything other than the standard 20 amino acids are not evaluated and will contain an NA as their prob_AMP value.
my_prediction <- predict_amps(my_protein_df, model = "precursor")
my_prediction$seq_aa <- paste(substring(my_prediction$seq_aa,1,45),"...",sep="") knitr::kable(my_prediction, digits = 3)
Predicted proteins with a specified predicted probability value could then be extracted and written to a FASTA file:
my_predicted_amps <- my_protein_df[my_prediction$prob_AMP > 0.8,]
my_predicted_amps$seq_aa <- paste(substring(my_predicted_amps$seq_aa,1,45),"...",sep="") knitr::kable(my_predicted_amps)
Write the data.frame with sequence names in the first column and protein sequences in the second column to a FASTA formatted file with df_to_faa()
df_to_faa(my_predicted_amps, tempfile("my_predicted_amps.fasta", tempdir()))
Try the ampir package in your browser
Any scripts or data that you put into this service are public.
R Package Documentation
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We want your feedback!
Note that we can't provide technical support on individual packages. You should contact the package authors for that.
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