AI Article Synopsis
- Understanding intermediates in organic reactions has led to advancements in synthesizing important compounds, yet peptide/protein self-assembly intermediates remain poorly understood.
- The study shows that linear heterochiral peptides assemble more slowly than homochiral peptides, allowing observation of unique assembly intermediates like mixed helical and overtwisted forms.
- This research also enabled the creation of a functional NMR alignment medium to measure residual dipolar couplings, enhancing the understanding of self-assembly pathways in linear heterochiral peptides and guiding the development of advanced materials.
Article Abstract
Understanding the intermediates or transition states in organic reactions has made it possible to develop theories and to synthesize important compounds. In contrast to organic reaction intermediates and even protein folding intermediates, the intermediates of peptide/protein self-assembly are not very well understood. Here we report that the self-assembly kinetics of linear heterochiral peptides are significantly slower than those of the corresponding homochiral peptides, which enables direct microscopic observation of assembly intermediates. By designing racemic or asymmetric heterochiral peptides, we were able to discover unusual mixed helical (-helix) and overtwisted intermediates. The convergence of equilibrium morphology between the homochiral and heterochiral peptides enables us to reasonably deduce the unobservable intermediates of rapidly assembling homochiral peptides. By utilizing the discovered information about the assembly intermediates, we were able to develop a functional NMR alignment medium that enables the measurement of residual dipolar couplings (RDCs) in a time-dependent manner. Although much less studied than their cyclic counterparts, the linear form of heterochiral peptides provides a means of obtaining a more in-depth understanding of the self-assembly pathway and of developing sophisticated bottom-up materials.
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| http://dx.doi.org/10.1021/acsnano.9b09070 | DOI Listing |
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