Clustalw Alignment - Conserved Regions
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11.2 years ago
ugartecj • 0

I am studying 3 proteins from the same family and I have performed an CLUSTALw alignment of each protein. It comes from their origin (fishes or amphibians depends) to primates. Afterthat with the human protein and PROSITE database I have scanned for patterns and profiles to check if these patterns are conserved in the CLUSTALw alignment. Now, without considering the regions that showed a pattern, I still have regions very conserved.

So then, I would like to know if there is a way to know the role of these regions. I have been looking for in literature or in a database of regular expression.... but does anyone an idea?

The regions comes from 2-3 aa to a maximun of 15-16 aa. They are transmembrane proteins. The conserved regions are out of the TM domain.

Thanks

clustalw • 4.6k views
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11.2 years ago
aswad87 • 0

to begin with, 3 proteins is not a big enough sample to say that something is conserved for functional reasons. it depends on how distant they are i suppose.

you could make some educated guesses based on the properties of the amino acid as well as where they are in the protein. furthermore, if you model the 3d structure of the protein you might find that they are important for a loop or something else structural.

I also suggest you have a look at the underlying nucleotides, to see how divergent they are.

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11.2 years ago
ugartecj • 0

Thank you aswad87

the 3 proteins belongs to the same family. I have done the CULSTALw alginment for each protein in a evolutionary way. So I have 3 CLUSTALw with 20 sequences approximately from amphibians or birds & reptiles (depend the protein) to primates. I have been checking the patterns and profiles got it for the 3 human proteins in each CLUSTALw to see how conserved are in the evolution.

After that I still have some regions very conserved.

I will check the predicted structure of each protein to see where these regions are located.

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11.2 years ago

This is similar/related to the questions asked and answers given in these posts: A: locating motif within a protein sequence, Predicting protein-protein binding, Identifying functional regions of proteins

To give a direct answer to this question - coming from a group that works on understanding/predicting the function of short functional regions of proteins, I'd point you in the direction of the resources developed in our group, ELM, phosophELM, and the alignment-focused Conservation Scorer, and check out also the links there

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