Literature DB >> 16084386

Glycine residues appear to be evolutionarily conserved for their ability to inhibit aggregation.

Claudia Parrini1, Niccolò Taddei, Matteo Ramazzotti, Donatella Degl'Innocenti, Giampietro Ramponi, Christopher M Dobson, Fabrizio Chiti.   

Abstract

Six glycine residues of human muscle acylphosphatase (AcP) are evolutionarily conserved across the three domains of life. We have generated six variants of AcP, each having a glycine substituted by an alanine (G15A, G19A, G37A, G45A, G53A, and G69A). Three additional variants had Gly45 replaced by serine, glutamate, and arginine, respectively. The mutational variants do not, on average, have a lower conformational stability than other variants with substitutions of nonconserved residues. In addition, only the G15A variant is enzymatically inactive. However, all variants, with the exception of the G15A mutant, form amyloid aggregates more rapidly than the wild-type. Dynamic light-scattering experiments carried out under conditions close to physiological confirm that aggregate formation is generally more pronounced for the glycine-substituted variants. Apart from the glycine at position 15, all other conserved glycine residues in this protein could have been maintained during evolution because of their ability to inhibit aggregation.

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Year:  2005        PMID: 16084386     DOI: 10.1016/j.str.2005.04.022

Source DB:  PubMed          Journal:  Structure        ISSN: 0969-2126            Impact factor:   5.006


  18 in total

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