Vikram J. Pansare

Flash nanoprecipitation of polystyrene nanoparticles

Aside from polymerization techniques, polymer nanoparticles can be generated through the displacement of a solvent with a nonsolvent, i.e., nanoprecipitation. In this study, we utilize a facile process termed Flash NanoPrecipitation (FNP) to generate polystyrene (PS) nanoparticles of several different molecular weights. As compared to PS nanoparticles synthesized by surfactant free emulsion polymerization, nanoparticles prepared by FNP show comparable size distributions when the diameter is less than 150 nm. Furthermore, we illustrate that the sizes of PS nanoparticles prepared by FNP can be fine-tuned by changing the polymer and/or electrolyte concentration. The stabilized nanoparticles contain only the radically polymerized polymer chains, which have sulfate anions at the chain termini and no additional external stabilizers. Calculations of the mechanism of particle formation and stabilization show that the size-dependent electrostatic repulsions between nanoparticles and single collapsed polymer chains control assembly and monodispersity. The ability to independently vary polymer molecular weight and nanoparticle size will enable fundamental studies of the effect of confinement on polymer dynamics in a way not easily achievable by other techniques.

Quenched hexacene optoacoustic nanoparticles

Optoacoustic (photoacoustic) imaging enables high-resolution optical imaging at depths well beyond optical microscopy, revolutionizing optical interrogation of tissues. Operation in the near-infrared (NIR) is nevertheless necessary to capitalize on the technology potential and reach depths of several centimeters. Using Flash NanoPrecipitation for highly-scalable single-step encapsulation of hydrophobic hexacene at self-quenching concentrations, we propose quenched fluorescence-dye nanoparticles as a potent alternative to NIR metal nanoparticles for strong optoacoustic signal generation. Comprehensive hexacene-based nanoparticle characterization was based on a 5-step approach that examined the physicochemical features (Step 1), optoacoustic signal generation (Step 2), stability (Step 3), biocompatibility (Step 4) and spectral sensitivity (Step 5). Using this characterization framework we showcase the discovery of two nanoparticle formulations, QH2-50 nm and QH2-100 nm that attain superior stability characteristics and optimal optoacoustic properties compared to gold standards commonly employed for near-infrared optoacoustics. We discuss encapsulation and self-quenching (ESQ) of organic dyes as a promising strategy to generate optimal optoacoustic particles.

Adsorption characteristics of charged and nonionic small molecules to colloidal alumina

Dense fluorescent pigments used for inkjet printing of UV and IR-readable non-photobleaching security features require stabilizers to prevent aggregation/sedimentation and inkjet head clogging at high resolution. A study of small molecule adsorption to α-alumina, a model system for security pigments, is presented. Alumina is dispersed by two methods yielding different zeta potentials but identical isoelectric points. Essentially complete dispersion is obtained in water at pH 3 but aggregation occurs at pH 6 where the surface charging is lower. Adsorption studies focus on the naphthyl-phosphate, -sulfate, and hydroxyl (triethylene glycol) groups. Phosphate adsorption was strongest with a 1.2 molecules/nm2 plateau, close to the titratable exchange capacity of 1.3 OH groups/nm2 on the alumina surface with ΔHadsorption=-7.58±1.63kJ/mol determined by calorimetry. Sulfate adsorption was weaker with a more linear adsorption isotherm. The adsorption/exchange process yields a rise in pH that is correlated with the binding strength. Hydroxyl binding is weakest, being driven by hydrogen bonding, and showed no rise in pH during adsorption. A polyphosphate-poly(ethylene glycol) block copolymer is expected to be advantageous for the dispersion of such inkjet colloids.

Millisecond Self-Assembly of Stable Nanodispersed Drug Formulations

We report the development of a new spray-drying and nanoparticle assembly process (SNAP) that enables the formation of stable, yet rapidly dissolving, sub-200 nm nanocrystalline particles within a high Tg glassy matrix. SNAP expands the class of drugs that spray-dried dispersion (SDD) processing can address to encompass highly crystalline, but modestly hydrophobic, drugs that are difficult to process by conventional SDD. The process integrates rapid precipitation and spray-drying within a custom designed nozzle to produce high supersaturations and precipitation of the drug and high Tg glassy polymer. Keeping the time between precipitation and drying to tens of milliseconds allows for kinetic trapping of drug nanocrystals in the polymer matrix. Powder X-ray diffraction, solid state 2D NMR, and SEM imaging shows that adding an amphiphilic block copolymer (BCP) to the solvent gives essentially complete crystallization of the active pharmaceutical ingredient (API) with sub-200 nm domains. In contrast, the absence of the block copolymer results in the API being partially dispersed in the matrix as an amorphous phase, which can be sensitive to changes in bioavailability over time. Quantification of the API-excipient interactions by 2D 13C-1H NMR correlation spectroscopy shows that the mechanism of enhanced nanocrystal formation is not due to interactions between the drug and the BCP, but rather the BCP masks interactions between the drug and hydrophobic regions of the matrix polymers. BCP-facilitated SNAP samples show improved stability during aging studies and rapid dissolution and release of API in vitro.

Formulation of long-wavelength indocyanine green nanocarriers

Abstract. Indocyanine green (ICG), a Food and Drug Administration (FDA)-approved fluorophore with excitation and emission wavelengths inside the “optical imaging window,” has been incorporated into nanocarriers (NCs) to achieve enhanced circulation time, targeting, and real-time tracking in vivo. While previous studies transferred ICG exogenously into NCs, here, a one-step rapid precipitation process [flash nanoprecipitation (FNP)] creates ICG-loaded NCs with tunable, narrow size distributions from 30 to 180 nm. A hydrophobic ion pair of ICG-tetraoctylammonium or tetradodecylammonium chloride is formed either in situ during FNP or preformed then introduced into the FNP feed stream. The NCs are formulated with cores comprising either vitamin E (VE) or polystyrene (PS). ICG core loadings of 30 wt. % for VE and 10 wt. % for PS are achieved. However, due to a combination of molecular aggregation and Förster quenching, maximum fluorescence (FL) occurs at 10 wt. % core loading. The FL-per-particle scales with core diameter to the third power, showing that FNP enables uniform volume encapsulation. By varying the ICG counter-ion ratio, encapsulation efficiencies above 80% are achieved even in the absence of ion pairing, which rises to 100% with 1∶1 ion pairing. Finally, while ICG ion pairs are shown to be stable in buffer, they partition out of NC cores in under 30 min in the presence of physiological albumin concentrations.