Literature DB >> 19663418

Tuning the pH responsiveness of beta-hairpin peptide folding, self-assembly, and hydrogel material formation.

Karthikan Rajagopal1, Matthew S Lamm, Lisa A Haines-Butterick, Darrin J Pochan, Joel P Schneider.   

Abstract

A design strategy to control the thermally triggered folding, self-assembly, and subsequent hydrogelation of amphiphilic beta-hairpin peptides in a pH-dependent manner is presented. Point substitutions of the lysine residues of the self-assembling peptide MAX1 were made to alter the net charge of the peptide. In turn, the electrostatic nature of the peptide directly influences the solution pH at which thermally triggered hydrogelation is permitted. CD spectroscopy and oscillatory rheology show that peptides of lower net positive charge are capable of folding and assembling into hydrogel material at lower values of pH at a given temperature. The pH sensitive folding and assembling behavior is not only dependent on the net peptide charge, but also on the exact position of substitution within the peptide sequence. TEM shows that these peptides self-assemble into hydrogels that are composed of well-defined fibrils with nonlaminated morphologies. TEM also indicates that fibril morphology is not influenced by making these sequence changes on the hydrophilic face of the hairpins. Rheology shows that the ultimate mechanical rigidity of these peptide hydrogels is dependent on the rate of folding and self-assembly. Peptides that fold and assemble faster afford more rigid gels. Ultimately, this design strategy yielded a peptide MAX1(K15E) that is capable of undergoing thermally triggered hydrogelation at physiological buffer conditions (pH 7.4, 150 NaCl, 37 degrees C).

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Year:  2009        PMID: 19663418     DOI: 10.1021/bm900544e

Source DB:  PubMed          Journal:  Biomacromolecules        ISSN: 1525-7797            Impact factor:   6.988


  42 in total

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Authors:  J Nie; X Zhang; W Wang; J Ren; A-P Zeng
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9.  Iterative design of peptide-based hydrogels and the effect of network electrostatics on primary chondrocyte behavior.

Authors:  Chomdao Sinthuvanich; Lisa A Haines-Butterick; Katelyn J Nagy; Joel P Schneider
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10.  Length-dependent proteolytic cleavage of short oligopeptides catalyzed by matrix metalloprotease-9.

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