Mechanosensitive Self-Replication Driven by Self-Organization

At Sixes and Sevens Molecular synthesis and macroscopic aggregation have often been regarded as entirely separate processes. From the researcher's standpoint, once reagents have been mixed, synthesis is largely passive, whereas processes such as crystallization can be more actively manipulated. Carnall et al. (p. 1502) characterized an unusual system in which the formation of aggregated cyclic macromolecules (macrocycles) from small peptide-based building blocks was governed by intimately interdependent factors ranging from the scale of covalent bond formation all the way to micron scale fiber growth. As the macrocycles stacked against one another to form the fibers, they remained loosely bonded enough internally to incorporate or expel individual building blocks. Varying the type of mechanical force applied to the growing fibers (either through shaking or stirring the solution), alternately favored formation of either 6-membered or 7-membered covalent macrocycles. The type of mechanical agitation applied to a solution influences which of two molecular products dominate. Self-replicating molecules are likely to have played an important role in the origin of life, and a small number of fully synthetic self-replicators have already been described. Yet it remains an open question which factors most effectively bias the replication toward the far-from-equilibrium distributions characterizing even simple organisms. We report here two self-replicating peptide-derived macrocycles that emerge from a small dynamic combinatorial library and compete for a common feedstock. Replication is driven by nanostructure formation, resulting from the assembly of the peptides into fibers held together by β sheets. Which of the two replicators becomes dominant is influenced by whether the sample is shaken or stirred. These results establish that mechanical forces can act as a selection pressure in the competition between replicators and can determine the outcome of a covalent synthesis.

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