Spontaneous and Directed Symmetry Breaking in the Formation of Chiral Nanocrystals

The homochirality of biomolecules remains one of the outstanding puzzles concerning the beginning of life. Chiral amplification of a randomly perturbed racemic mixture of chiral molecules is a well-accepted prerequisite for all routes to biological homochirality. Some models have suggested that such amplification occurred due to asymmetric discrimination of chiral biotic or prebiotic molecules when they adsorbed onto crystalline surfaces. While chiral amplification has been demonstrated on surfaces of both chiral and achiral crystals, the mechanism that would produce an enantiomeric imbalance in the chiral surfaces themselves has not been addressed. Here we report strong chiral amplification in the colloidal synthesis of intrinsically chiral lanthanide phosphate nanocrystals, quantitatively measured via the circularly polarized luminescence of the lanthanide ions within the nanocrystals. The amplification involves spontaneous symmetry breaking into either left- or right-handed nanocrystals below a critical temperature. Furthermore, chiral tartaric acid molecules in the solution act as an external chiral field, sensitively directing the amplified nanocrystal handedness through a discontinuous transition between left- and right-handed excess. These characteristics suggest a conceptual framework for chiral amplification, based on the statistical thermodynamics of critical phenomena, which we use to quantitatively account for the observations. Our results demonstrate how chiral minerals with high enantiomeric excess could have grown locally in a primordial racemic aqueous environment.Comment: 9 pages, 4 figure

Reversible Dimerization of Polymeric Amphiphiles Acts as a Molecular Switch of Enzymatic Degradability

Enzyme-responsive polymeric micelles have great potential as drug delivery systems due to the high selectivity and overexpression of disease-associated enzymes, which could be utilized to trigger the release of active drugs only at the target site. We previously demonstrated that enzymatic degradation rates of amphiphilic PEG-dendron hybrids could be precisely tuned by gradually increasing the hydrophobic to hydrophilic ratio. However, with the increase in hydrophobicity, the micelles rapidly became too stable and could not be degraded, as often encountered for many other amphiphilic assemblies. Here we address the challenge to balance between stability and reactivity of enzymatically degradable assemblies by utilizing reversible dimerization of diblock polymeric amphiphiles to yield jemini amphiphiles. This molecular transformation serves as a tool to control the critical micelle concentration of the amphiphiles in order to tune their micellar stability and enzymatic degradability. To demonstrate this approach, we show that simple dimerization of two polymeric amphiphiles through a single reversible disulfide bond significantly increased the stability of their micellar assemblies toward enzymatic degradation, although the hydrophilic to hydrophobic ratio was not changed. Reduction of the disulfide bond led to dedimerization of the polymeric hybrids and allowed their degradation by the activating enzyme. The generality of the approach is demonstrated by designing both esterase- and amidase-responsive micellar systems. This new molecular design can serve as a simple tool to increase the stability of polymeric micelles without impairing their enzymatic degradability