Jiahui Qi scite author profile

In nature, living organisms use peptides and proteins to precisely control the nucleation and growth of inorganic minerals and sequester CO(2)via mineralization of CaCO(3). Here we report the exploitation of a novel class of sequence-specific non-natural polymers called peptoids as tunable agents that dramatically control CaCO(3) mineralization. We show that amphiphilic peptoids composed of hydrophobic and anionic monomers exhibit both a high degree of control over calcite growth morphology and an unprecedented 23-fold acceleration of growth at a peptoid concentration of only 50 nM, while acidic peptides of similar molecular weight exhibited enhancement factors of only ∼2 or less. We further show that both the morphology and rate controls depend on peptoid sequence, side-chain chemistry, chain length, and concentration. These findings provide guidelines for developing sequence-specific non-natural polymers that mimic the functions of natural peptides or proteins in their ability to direct mineralization of CaCO(3), with an eye toward their application to sequestration of CO(2) through mineral trapping.

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Tuning calcite morphology and growth acceleration by a rational design of highly stable protein-mimetics

Chen

Tao

et al. 2014

Sci Rep

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In nature, proteins play a significant role in biomineral formation. One of the ultimate goals of bioinspired materials science is to develop highly stable synthetic molecules that mimic the function of these natural proteins by controlling crystal formation. Here, we demonstrate that both the morphology and the degree of acceleration or inhibition observed during growth of calcite in the presence of peptoids can be rationally tuned by balancing the electrostatic and hydrophobic interactions, with hydrophobic interactions playing the dominant role. While either strong electrostatic or hydrophobic interactions inhibit growth and reduces expression of the {104} faces, correlations between peptoid-crystal binding energies and observed changes in calcite growth indicate moderate electrostatic interactions allow peptoids to weakly adsorb while moderate hydrophobic interactions cause disruption of surface-adsorbed water layers, leading to growth acceleration with retained expression of the {104} faces. This study provides fundamental principles for designing peptoids as crystallization promoters, and offers a straightforward screening method based on macroscopic crystal morphology. Because peptoids are sequence-specific, highly stable, and easily synthesized, peptoid-enhanced crystallization offers a broad range of potential applications.

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HMGB1–RAGE signaling pathway in severe preeclampsia

Zhu

Zhang

et al. 2015

Placenta

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Jiahui Qi

Engineered Biomimetic Polymers as Tunable Agents for Controlling CaCO₃ Mineralization

Tuning calcite morphology and growth acceleration by a rational design of highly stable protein-mimetics

HMGB1–RAGE signaling pathway in severe preeclampsia

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Jiahui Qi

Engineered Biomimetic Polymers as Tunable Agents for Controlling CaCO3 Mineralization

Tuning calcite morphology and growth acceleration by a rational design of highly stable protein-mimetics

HMGB1–RAGE signaling pathway in severe preeclampsia

Contact Info

Product

Resources

About

Engineered Biomimetic Polymers as Tunable Agents for Controlling CaCO₃ Mineralization