Take the 2-minute tour ×
Stack Overflow is a question and answer site for professional and enthusiast programmers. It's 100% free, no registration required.

I have a large number of protein sequences in fasta format.

I want to get the pair-wise sequence similarity score for each pairs of the proteins.

Any package in R could be used to get the blast similarity score for protein sequences?

share|improve this question
2  
Are you familiar with bioconductor? I know nothing about proteins, fasta formats, or pair-wise sequence similarity scores - but that'd be where I'd go to look. –  Chase Jun 30 '11 at 3:57
    
Thank you Chase for introduction to Bioconductor. It am new to it. Thanks Gavin Simpson for editing my poor English. –  user2718 Jun 30 '11 at 14:59

1 Answer 1

up vote 8 down vote accepted

As per Chase's suggestion, bioconductor is indeed the way to go and in particular the Biostrings package. To install the latter I would suggest installing the core bioconductor library as such:

source("http://bioconductor.org/biocLite.R")
biocLite()

This way you will cover all dependencies. Now, to align 2 protein sequences or any two sequences for that matter you will need to use pairwiseAlignment from Biostrings. Given a fasta protseq.fasta file of 2 sequences that looks like this:

>protein1
MYRALRLLARSRPLVRAPAAALASAPGLGGAAVPSFWPPNAAR
MASQNSFRIEYDTFGELKVPNDKYYGAQTVRSTMNFKIGGVTE
RMPTPVIKAFGILKRAAAEVNQDYGLDPKIANAIMKAADEVAE
GKLNDHFPLVVWQTGSGTQTNMNVNEVISNRAIEMLGGELGSK
IPVHPNDHVNKSQ
>protein2
MRSRPAGPALLLLLLFLGAAESVRRAQPPRRYTPDWPSLDSRP
LPAWFDEAKFGVFIHWGVFSVPAWGSEWFWWHWQGEGRPYQRF
MRDNYPPGFSYADFGPQFTARFFHPEEWADLFQAAGAKYVVLT
TKHHEGFTNW*

If you want to globally align these 2 sequences using lets say BLOSUM100 as your substitution matrix, 0 penalty for opening a gap and -5 for extending one then:

require("Biostrings")
data(BLOSUM100)
seqs <- readFASTA("~/Desktop/protseq.fasta", strip.descs=TRUE)
alm <- pairwiseAlignment(seqs[[1]]$seq, seqs[[2]]$seq, substitutionMatrix=BLOSUM100, gapOpening=0, gapExtension=-5)

The result of this is (removed some of the alignment to save space):

> alm
Global PairwiseAlignedFixedSubject (1 of 1)
pattern: [1] MYRALRLLARSRPLVRA-PAAALAS....
subject: [1] M-R-------SRP---AGPALLLLL.... 
score: -91

To only extract the score for each alignment:

> score(alm)
[1] -91

Given this you can easily now do all pairwise alignments with some very simple looping logic. To get a better hang of pairwise alignment using bioconductor I suggest you read this.

An alternative approach would be to do a multiple sequence alignment instead of pairwise. You could use bio3d and from there the seqaln function to align all sequences in your fasta file.

share|improve this answer

Your Answer

 
discard

By posting your answer, you agree to the privacy policy and terms of service.

Not the answer you're looking for? Browse other questions tagged or ask your own question.