Literature DB >> 20962881

Low-complexity sequences and single amino acid repeats: not just "junk" peptide sequences.

Wilfried Haerty1, G Brian Golding.   

Abstract

For decades proteins were thought to interact in a "lock and key" system, which led to the definition of a paradigm linking stable three-dimensional structure to biological function. As a consequence, any non-structured peptide was considered to be nonfunctional and to evolve neutrally. Surprisingly, the most commonly shared peptides between eukaryotic proteomes are low-complexity sequences that in most conditions do not present a stable three-dimensional structure. However, because these sequences evolve rapidly and because the size variation of a few of them can have deleterious effects, low-complexity sequences have been suggested to be the target of selection. Here we review evidence that supports the idea that these simple sequences should not be considered just "junk" peptides and that selection drives the evolution of many of them.

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Year:  2010        PMID: 20962881     DOI: 10.1139/g10-063

Source DB:  PubMed          Journal:  Genome        ISSN: 0831-2796            Impact factor:   2.166


  28 in total

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7.  ProRepeat: an integrated repository for studying amino acid tandem repeats in proteins.

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8.  Three glycoside hydrolase family 12 enzymes display diversity in substrate specificities and synergistic action between each other.

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9.  Androgen receptor polyglutamine repeat number: models of selection and disease susceptibility.

Authors:  Calen P Ryan; Bernard J Crespi
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10.  A test of somatic mosaicism in the androgen receptor gene of Canada lynx (Lynx canadensis).

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