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Organocatalyzed ring-opening polymerization (ROP) is a versatile technique for synthesizing biodegradable polymers, including polyesters and polycarbonates. We introduce o-phenylene bisurea (OPBU) (di)anions as a novel class of organocatalysts that are fast, easily tunable, mildly basic, and exceptionally selective. These catalysts surpass previous generations, such as thiourea, urea, and TBD, in selectivity (kp/ktr) by 8 to 120 times. OPBU catalysts facilitate the ROP of various monomers, achieving high conversions (>95%) in seconds to minutes, producing polymers with precise molecular weights and very low dispersities (Đ ≈ 1.01). This performance nearly matches the ideal distribution expected from living polymerization (Poisson distribution). Density functional theory (DFT) calculations reveal that the catalysts stabilize the oxyanion transition state via a hydrogen bond pocket similar to the "oxyanion hole" in enzymatic catalysis. Both experimental and theoretical analyses highlight the critical role of the semi-rigid o-phenylene linker in creating a hydrogen bond pocket that is tight yet flexible enough to accommodate the oxyanion transition state effectively. These new insights have provided a new class of organic catalysts whose accessibility, moderate basicity, excellent solubility, and unparalleled selectivity and tunability open up new opportunities for controlled polymer synthesis. 

A library of structurally related heterocycles containing N-H motifs are explored as ring-opening polymerization (ROP) pre-catalysts. Upon deprotonation of these heterocycles with appropriate bases, corresponding salts are formed, which catalyze the ROP of various lactones and cyclic carbonates, affording polymers with dispersity values ranging from 1.01 to 1.12. These catalysts exhibit a wide range of catalytic activities, spanning over seven orders of magnitude (>107), with their relative rates generally correlating to the pKa of the N-H group in the neutral heterocycle. Despite apparent structural and electronic similarities, these heterocycle catalysts display markedly different kinetic behaviors regarding the identity of different cations. Kinetic and NMR studies have revealed two distinct sets of mechanisms: small alkali metal cations such as Li+ and Na+ reduce the activity of imidazol(in)e derived catalysts due to their tendency to associate with the alkoxide chain-end, thus inhibiting its propagation; conversely, these cations form robust cation-π assemblies with indolocarbazole anions, simultaneously binding and activating monomer carbonyls towards the nucleophilic attack, resulting in a significant rate enhancement. This distinctive activation motif of the indolocarbazole sets it apart from other catalysts by utilizing cations as a potent handle for modulating polymerization reactivity. Coupled with its high availability, good solubility, high activity, moderate basicity, and high selectivity, the indolocarbazole heterocycle emerges as one of the most versatile organocatalysts for ring-opening polymerization. 

Dynamic effects are an important determinant of chemical reactivity and selectivity, but the deliberate manipulation of atomic motions during a chemical transformation is not straightforward. Here, we demonstrate that extrinsic force exerted upon cyclobutanes by stretching pendant polymer chains influences product selectivity through force-imparted nonstatistical dynamic effects on the stepwise ring-opening reaction. The high product stereoselectivity is quantified by carbon-13 labeling and shown to depend on external force, reactant stereochemistry, and intermediate stability. Computational modeling and simulations show that, besides altering energy barriers, the mechanical force activates reactive intramolecular motions nonstatistically, setting up “flyby trajectories” that advance directly to product without isomerization excursions. A mechanistic model incorporating nonstatistical dynamic effects accounts for isomer-dependent mechanochemical stereoselectivity.