ZIF-8 degrades in cell media,serum, and some—but not all—common laboratory buffers

ABSTRACT

Drug delivery using metal-organic frameworks (MOF) has elicited interest in their biocompatibility; however, few studies have been conducted on their stability in common buffers, cell media, and blood proteins. In particular, the use of ZIF-8, a MOF interconnected by Zn and methylimidazole, has been frequently employed. In this study, we tested single crystals of ZIF-8 with common laboratory buffers, cell media, and serum, and noted several issues. Buffers containing phosphate and bicarbonate alter the appearance and composition of ZIF-8; however, these buffers do not appear to cause cargo to leak out even when the ZIF-8 itself is displaced by phosphates. On the other hand, serum dissolves ZIF-8, causing premature cargo release. Our results show that ZIF-8 undergoes surface chemistry changes that may affect the interpretation of cellular uptake and cargo release data. On the other hand, it provides a rational explanation as to how ZIF-8 neatly dissolves in vivo.     

Design,Synthesis, and Phenotypic Profiling of Pyrano‐Furo‐Pyridone Pseudo Natural Products

Natural products (NPs) inspire the design and synthesis of novel biologically relevant chemical matter, for instance through biology‐oriented synthesis (BIOS). However, BIOS is limited by the partial coverage of NP‐like chemical space by the guiding NPs. The design and synthesis of “pseudo NPs” overcomes these limitations by combining NP‐inspired strategies with fragment‐based compound design through de novo combination of NP‐derived fragments to unprecedented compound classes not accessible through biosynthesis. We describe the development and biological evaluation of pyrano‐furo‐pyridone (PFP) pseudo NPs, which combine pyridone‐ and dihydropyran NP fragments in three isomeric arrangements. Cheminformatic analysis indicates that the PFPs reside in an area of NP‐like chemical space not covered by existing NPs but rather by drugs and related compounds. Phenotypic profiling in a target‐agnostic “cell painting” assay revealed that PFPs induce formation of reactive oxygen species and are structurally novel inhibitors of mitochondrial complex I.     

Rate-equilibrium relationships in hydride transfer reactions: the role of intrinsic barriers

A literature survey on the kinetics of hydride abstractions from CH-groups by carbocations reveals a general phenomenon: Variation of the hydride acceptor affects the rates of hydride transfer to a considerably greater extent than an equal change of the thermodynamic driving force caused by variation of the hydride donor. The origin of this relationship was investigated by quantum chemical calculations on various levels of ab initio and DFT theory for the transfer of an allylic hydrogen from 1-mono- and 1,1-disubstituted propenes (XYC=CH-CH(3)) to the 3-position of 1-mono- and 1,1-disubstituted allyl cations (XYC=CH-CH(2)(+)). The discussion is based on the results of the MP2/6-31+G(d,p)//RHF/6-31+G(d,p) calculations. Electron-releasing substituents X and Y in the hydride donors increase the exothermicity of the reaction, while electron-releasing substituents in the hydride acceptors decrease exothermicity. In line with Hammond's postulate, increasing exothermicity shifts the transition states on the reaction coordinate toward reactants, as revealed by the geometry parameters and the charge distribution in the activated complexes. Independent of the location of the transition state on the reaction coordinate, a value of 0.72 is found for Hammond-Leffler's alpha = deltaDeltaG/deltaDelta(r)G degrees when the hydride acceptor is varied, while alpha = 0.28 when the hydride donor is varied. The value of alpha thus cannot be related with the position of the transition state. Investigation of the degenerate reactions XYC=CH-CH(3) + XYC=CH-CH(2)(+) indicates that the migrating hydrogen carries a partial positive charge in the transition state and that the intrinsic barriers increase with increasing electron-releasing abilities of X and Y. Substituent variation in the donor thus influences reaction enthalpy and intrinsic barriers in the opposite sense, while substituent variation in the acceptor affects both terms in the same sense, in accord with the experimental findings. Marcus theory is employed to treat these effects quantitatively.     

The dynamics of rotational isomerism in crystals as studied by vibrational spectroscopy

Vibrational spectroscopy is uniquely capable of determining the structure and dynamics arising from the rotational degrees of freedom in molecular solids. Vibrational spectroscopy is sensitive to phenomena occurring on a time scale between the slow scale of magnetic, resonance methods and fast scale of diffraction methods; a time scale appropriate for both internal and overall rotation. Rotational motion of molecules in crystals provide examples of very simple reactions. Our understanding of the spectra of reacting molecules can thus be tested on these systems, and we conclude that Redfield equations can describe such spectra.A rich variety of motional effects are described: (1) The libration of the water of hydration in sodium perchlorate which illustrates a simple reacting system. (2) The libration of the adamantane molecule in both its ordered and disordered crystal phases which illustrates intermolecular interactions in organic crystals and the consequences of disorder. (3) The libration of the ammonium ion in crystals of ammonium salts which illustrated both change of orientational position by tunneling and the subtle orientating effects of isotopic substitution. (4) The internal rotation in n-alkane crystals which illustrates the ability to determine conformers and the relationship between the occurrence of disordered conformers and the occurrence of phase transitions.     

Characterization of some physical and chromatographic properties of monolithic poly(styrene-co-divinylbenzene) columns

Monolithic capillary columns were prepared by copolymerization of styrene and divinylbenzene inside a 200 microm i.d. fused silica capillary using a mixture of tetrahydrofuran and decanol as porogen. Important chromatographic features of the synthesized columns were characterized and critically compared to the properties of columns packed with micropellicular, octadecylated poly(styrene-co-divinylbenzene) (PS-DVB-C18) particles. The permeability of a 60 mm long monolithic column was slightly higher than that of an equally dimensioned column packed with PS-DVB-C18 beads and was invariant up to at least 250 bar column inlet pressure, indicating the high-pressure stability of the monolithic columns. Interestingly, monolithic columns showed a 3.6 times better separation efficiency for oligonucleotides than granular columns. To study differences of the molecular diffusion processes between granular and monolithic columns, Van Deemter plots were measured. Due to the favorable pore structure of monolithic columns all kind of diffusional band broadening was reduced two to five times. Using inverse size-exclusion chromatography a total porosity of 70% was determined, which consisted of internodule porosity (20%) and internal porosity (50%). The observed fast mass transfer and the resulting high separation efficiency suggested that the surface of the monolithic stationary phase is rather rough and does not feature real pores accessible to macromolecular analytes such as polypeptides or oligonucleotides. The maximum analytical loading capacity of monolithic columns for oligonucleotides was found to be in the region of 500 fmol, which compared well to the loading capacity of the granular columns. Batch-to-batch reproducibility proved to be better with granular stationary phases compared to monolithic stationary phase, in which each column bed is the result of a unique column preparation process.     

Characterization of colloidal hematite particle shape and dispersion behavior

An elliptically polarized light scattering (EPLS) technique for the size and shape characterization of ellipsoidal hematite particles is presented. The hematite particles are synthesized by aging aqueous FeCl(3) or Fe(NO(3))(3) solutions at 100 degrees C. Different reaction conditions create particles of aspect ratios between 1 (spherical) and 8 (elongated). Cross-sectional diameter and aspect ratio are observed as a function of reaction (aging) time. Growth of the elongated particles, as well as their fractal aggregation behavior, is characterized using EPLS and comparisons are made with photon correlation spectroscopy and TEM measurements.     

Quantification of the electrophilic reactivities of aldehydes, imines, and enones

The rates of the epoxidation reactions of aldehydes, of the aziridination reactions of aldimines, and of the cyclopropanation reactions of α,β-unsaturated ketones with aryl-stabilized dimethylsulfonium ylides have been determined photometrically in dimethyl sulfoxide (DMSO). All of these sulfur ylide-mediated cyclization reactions as well as the addition reactions of stabilized carbanions to N-tosyl-activated aldimines have been shown to follow a second-order rate law, where the rate constants reflect the (initial) CC bond formation between nucleophile and electrophile. The derived second-order rate constants (log k(2)) have been combined with the known nucleophilicity parameters (N, s(N)) of the aryl-stabilized sulfur ylides 4a,b and of the acceptor-substituted carbanions 4c-h to calculate the electrophilicity parameters E of aromatic and aliphatic aldehydes (1a-i), N-acceptor-substituted aromatic aldimines (2a-e), and α,β-unsaturated ketones (3a-f) according to the linear free-energy relationship log k(2) = s(N)(N + E) as defined in J. Am. Chem. Soc.2001, 123, 9500-9512. The data reported in this work provide the first quantitative comparison of the electrophilic reactivities of aldehydes, imines, and simple Michael acceptors in DMSO with carbocations and cationic metal-π complexes within our comprehensive electrophilicity scale.     

Enantiotopic discrimination in the deuterium NMR spectrum of solutes with S4 symmetry in chiral liquid crystals

Enantiotopic discrimination in the NMR spectra of prochiral rigid solutes in chiral liquid crystals (CLC), by the ordering mechanism, is limited to molecules possessing one of the four, so called, "allowed" symmetries, D(2d), C(2v), C(s), and S(4). So far, such spectral discrimination was demonstrated only for solutes possessing one of the first three symmetries. In this work, we present deuterium NMR measurements on a rigid S(4) compound dissolved in a chiral nematic solvent and demonstrate, for the first time, enantiotopic discrimination in such symmetry. The measurements were performed on the isotopically normal icosane derivative (1) and on its isotopomer (1-d(8)), specifically deuterated in its four core methylene groups. As a CLC solvent, a lyotropic mesophase, consisting of a solution of poly-γ-benzyl-L-glutamate (PBLG) in pyridine, was employed. For comparison with a corresponding achiral liquid crystal (ALC) solvent, a solution of a racemic mixture of poly-γ-benzylglutamate (PBG) of similar composition in the same co-solvent was used. The spectra were recorded at 92.1 MHz using the 2D Q-COSY Fz sequence with proton decoupling. In the CLC solvents they exhibited clear discrimination due to different enantiotopic sites, with components displaced symmetrically, at frequencies below and above those in the corresponding ALC, as expected for discrimination by ordering. Two procedures were employed for correlating the enantiotopic sites in the CLC spectra. For 1-d(8) the dipolar cross-peaks in a 2D (2)H-(2)H COSY-90 experiment provided identification of signals belonging to the same methylene (and hence the same enantiotopic) groups. For 1 the correlation was achieved using a least-square-deviation fitting of the experimental quadrupole splittings with respect to those expected from the molecular geometry. These results, with appropriate symmetry considerations were used to determine the symmetric (S(zz)) and antisymmetric (S(xy) and S(xx)-S(yy)) components of the Saupe ordering matrix. Interpretation of the NMR spectra of prochiral solutes in CLC suffers from the ambiguity in identifying the signals with specific enantiotopic groups. For this reason only the relative (but not the absolute) signs of the antisymmetric elements of the ordering matrix can be determined. For the S(4) group this leads to sign ambiguity in the rhombic term in the diagonalized ordering matrix. Similar (but not identical) ambiguities occur for solutes belonging to the other allowed groups. In a concluding section of the paper, the ambiguities in the antisymmetric order parameters for the various allowed groups are compared and their physical meaning are discussed.