https://github.com/cran/AntAngioCOOL
Tip revision: 45df2234862a7196e883c1ff1bbf90ab27d6066b authored by Javad Zahiri on 01 August 2016, 14:01:06 UTC
version 1.2
version 1.2
Tip revision: 45df223
AntAngioCOOL.Rd
% Generated by roxygen2: do not edit by hand
% Please edit documentation in R/AntAngiCOOL.R
\name{AntAngioCOOL}
\alias{AntAngioCOOL}
\title{AntAngioCOOL}
\usage{
AntAngioCOOL(Input_Sequence, Classifier = 1, SF = FALSE, AF = FALSE)
}
\arguments{
\item{Input_Sequence}{A peptide sequence}
\item{Classifier}{1 if you want to get the prediction from model with maximum Accuracy (according to the independent test reasults), 2 if maximum Sensivity is desired and 3 if maximum Specefity is desired.}
\item{SF}{if True then all 2343 selected features (out of 175062 features) that had been used for prediction will be returned.}
\item{AF}{if True then all 175062 extracted features will be returned.}
}
\value{
If Predicted class (Anti-angiogenic/ Not anti-angiogenic) of the input peptide and a subset of descriptors upon request.
}
\description{
Machine learning based package to predict anti-angiogenic peptides using heterogeneous sequence descriptors.
}
\details{
AntAngioCOOL is a machine learning based package to predict anti-angiogenic peptides using heterogeneous sequence descriptors.
This package consists of three different predictors according to the obtained performances on independent test set: sensitive model, specific model and accurate model. These models have been build using the gold standard dataset that published by Ramaprasad et al. (Ettayapuram Ramaprasad et al., 2015).
Four different features have been used to encode peptides:
1- Pseudo Amino Acid Composition (PseAAC) that has been used effectively in predicting cell penetrating peptides (Chen, Chu, Huang, Kong, & Cai, 2015). Despite the simple amino acid composition, PseAAC considers the sequence-order information of the peptide.
2- K-mer composition that shows the fraction of all possible subsequences with length k in the given peptide. To compute k-mer composition features, reduced amino acid alphabet that proposed by Zahiri et al (Zahiri et al., 2014) has been exploited: the 20 alphabet of amino acids have been reduced to a new alphabet with size 8 according to 544 physicochemical and biochemical indices that extracted from AAIndex database (Kawashima et al., 2008) (C1={A, E}, C2={I, L, F, M, V}, C3={N, D, T, S}, C4={G}, C5={P}, C6={R, K, Q, H}, C7={Y, W}, C8={C}). We have computed k-mer composition for k=2,3,4 for each peptide.
3- Physico-chemical profile : To compute these features, 544 different physico-chemical indices have been extracted from AAINDEX (Kawashima et al., 2008). To remove redundant indices, a subset of indices with correlation coefficient less than 0.8 and greater than -0.8 has been selected. This feature type for 5 amino acids of N- termini (5-NT) and C-termini (5-CT).
4- Atomic profile : A 50-dimentional feature vector has been used to encode each peptide according to its atomic properties (frequency of five types of atoms: C, H, N, O, S). For details of atomic composition for each 20 natural amino acid see Kumar et al., 2015.
References
1- Chen, L., Chu, C., Huang, T., Kong, X., & Cai, Y.-D. (2015). Prediction and analysis of cell-penetrating peptides using pseudo-amino acid composition and random forest models. Amino Acids, 47(7), 1485-93. http://doi.org/10.1007/s00726-015-1974-5
2- Ettayapuram Ramaprasad, A. S., Singh, S., Gajendra P. S, R., Venkatesan, S., Brem, S., Cotran, R., . Stephens, R. (2015). AntiAngioPred: A Server for Prediction of Anti-Angiogenic Peptides. PLOS ONE, 10(9), e0136990. http://doi.org/10.1371/journal.pone.0136990
3- Kawashima, S., Pokarowski, P., Pokarowska, M., Kolinski, A., Katayama, T., & Kanehisa, M. (2008). AAindex: amino acid index database, progress report 2008. Nucleic Acids Research, 36(Database issue), D202-5. http://doi.org/10.1093/nar/gkm998
3- Kumar, R., Chaudhary, K., Singh Chauhan, J., Nagpal, G., Kumar, R., Sharma, M., & Raghava, G. P. S. (2015). An in silico platform for predicting, screening and designing of antihypertensive peptides. Scientific Reports, 5, 12512. http://doi.org/10.1038/srep12512
4- Zahiri, J., Mohammad-Noori, M., Ebrahimpour, R., Saadat, S., Bozorgmehr, J. H., Goldberg, T., & Masoudi-Nejad, A. (2014). LocFuse: Human protein-protein interaction prediction via classifier fusion using protein localization information. Genomics, 104(6), 496-503.
}
\examples{
AntAngioCOOL("AAPFLECQGN",2,SF=TRUE)
}
\author{
Babak Khorsand
}