Researchers have long sought to use surface ligands to enhance energy migration in nanocrystal solids by decreasing the physical separation between nanocrystals and strengthening their electronic coupling. Exciton-delocalizing ligands, which possess frontier molecular orbitals that strongly mix with nanocrystal band-edge states, are well-suited for this role because they can facilitate carrier-wave function extension beyond the nanocrystal core, reducing barriers for energy transfer. This report details the use of the exciton-delocalizing ligand phenyldithiocarbamate (PDTC) to tune the transport rate and diffusion length of excitons in CdSe nanocrystal solids. A film composed of oleate-terminated CdSe nanocrystals is subjected to a solid-state ligand exchange to replace oleate with PDTC. Exciton migration in the films is subsequently investigated by femtosecond transient absorption. Our experiments indicate that the treatment of nanocrystal films with PDTC leads to rapid (∼400 fs) downhill energy migration (∼80 meV), while no such migration occurs in oleate-capped films. Kinetic Monte Carlo simulations allow us to extract both rates and length scales for exciton diffusion in PDTC-treated films. These simulations reproduce dynamics observed in transient absorption measurements over a range of temperatures and confirm excitons hop via a Miller-Abrahams mechanism. Importantly, our experiments and simulations show PDTC treatment increases the exciton hopping rate to 200 fs, an improvement of 5 orders of magnitude relative to oleate-capped films. This exciton hopping rate stands as one of the fastest determined for CdSe solids. The facile, room-temperature processing and improved transport properties offered by the solid-state exchange of exciton-delocalizing ligands show they offer promise for the construction of strongly coupled nanocrystal arrays.
Small-angle X-ray scattering analyses reveal that the hydrated diblock oligomer n -C 16 H 23 (OCH 2 CH 2 ) 20 -OH (C 16 E 20 or Brij 58) forms lyotropic liquid crystals (LLCs) exhibiting face-centered cubic (FCC), body-centered cubic (BCC), Frank–Kasper (FK) A15, and cylindrical (H I ) morphologies over the concentration range 30–65 wt % amphiphile. Heating LLCs comprising 54–59 wt % C 16 E 20 drives the temperature-dependent phase transition sequence: A15 → BCC → H I . However, rapidly quenching the resulting H I phase from 70 to 25 °C initially forms a BCC phase that isothermally transforms into a complex, tetragonal FK σ phase comprising 30 quasispherical micelles. The metastability of this micellar σ phase is shown to depend on the sample cooling rate, thermal quench depth, and isothermal annealing temperature. We rationalize the preference for the A15 structure at 25 °C in terms of minimizing unfavorable water/hydrophobic contacts, while maximizing local particle sphericity. The symmetry breaking transition kinetics in these micellar LLCs apparently stem from the temperature-dependent activation barriers for phase nucleation and growth, which are intimately coupled to the time scales for micelle reconfiguration by amphiphile chain exchange and their spatial rearrangement. These findings highlight how thermal processing influences nucleation and growth of the self-assembled morphologies of intrinsically reconfigurable, soft spherical particles.
Under the right conditions, some biological systems can maintain high viability after being frozen and thawed, but many others (e.g., organs and many mammalian cells) cannot. To increase the rates of post-thaw viability and widen the library of living cells and tissues that can be stored frozen, an improved understanding of the mode of action of polymeric cryoprotectants is required. Here, we present a polymeric cryoprotectant, poly(methyl glycidyl sulfoxide) (PMGS), that achieved higher post-thaw viability for fibroblast cells than its small-molecule analogue dimethyl sulfoxide. By limiting the amount of water that freezes and facilitating cellular dehydration after ice nucleation, PMGS mitigates the mechanical and osmotic stresses that the freezing of water imparts on cells and facilitates higher-temperature vitrification of the remaining unfrozen volume. The development of PMGS advances a fundamental physical understanding of polymer-mediated cryopreservation, which enables new material design for long-term preservation of complex cellular networks and tissue.
Capillary-driven thinning of a liquid bridge is commonly used to measure the extensional rheology of macromolecular solutions for assessment of material sprayability, printability, and jettability. Methods like dripping-onto-substrate (DoS) rheometry...
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