三硼八氢N-(二茂铁基次甲基)三甲基季铵的多核、二维NMR波谱和空间结构研究

本文获得了标题季铵盐的~1H、~(13)C、~(11)B、~(13)C-~1H多核和二维异核相关波谱,并作了归属,还弄清了~(13)C和~1H核间相干传递关系。探寻了[B_3H_8]~-的波谱特性及其原因。从X射线单晶衍射法获得的键长、键角、二面角、配位数等数据和晶胞中分子的空间排列图,确定出分子的空间结构。     

The Aggregation of Cyclodextrins as Studied by Photon Correlation Spectroscopy

Photon correlation spectroscopy has been used to study theaggregation processes of natural and some modified cyclodextrins (CDs) in diluted aqueoussolutions. -, -, and -CD form large, polydisperse aggregatesin water, although the aggregation capability is different depending on the macrocycle considered. -CD solutions filtered through 0.2~m give a single-modaldistribution of aggregates of 224 nm in size. The monomeric -CD can be isolated by filtering through 0.1 m. -CD displays a bimodaldistribution (monomer + aggregates) with both pore sizes. At the concentrations studied (0.012 M) the contribution in mass of the aggregates with both CDs isnegligible. -CD is much more persistent in its aggregation, even after sievingits solutions through 0.02 m filters, and time dependent. The aggregation displayed byCDs with partial substitution of the OH groups (Methyl--CD and Hydroxypropyl--CD) is much weaker, indicating the implication of the hydrophilic rims ofthe CDs in the process. High temperatures, addition of urea or electrolytes andionisation of the OH groups by raising the pH, prevent the aggregation.     

Interaction Between Liposomes and Neutral Polymers: Effect of Adsorption on Drug Release

The processes of adsorption of two neutral polymers (poly(vinyl pyrrolidone), PVP and poly(vinyl alcohol), PVA) were investigated on liposomes composed of soy lecithin/dicetyl phosphate/cholesterol = 25:2:3 (molar ratio). The liposomes were prepared in buffered solution at pH = 7.4 and mixed with the solution of the measured polymers in the desired polymer/lipid (w/w) ratios. Adsorption was measured by determination of the equilibrium bulk concentration of the polymer. In the case of PVA quantitative adsorption measurements with a specific reagent were possible. Adsorption isotherms were recorded at 25 ± 1°C. It was concluded that adsorbed and unadsorbed PVA molecules are in equilibrium even at low polymer/ lipid ratios. The results were confirmed by dynamic laser light scattering (DLS), and thermal activity monitoring (TAM) experiments. Another group of the liposomes was prepared in 60 mM ammonium sulphate (pH = 5.0) and we filled the vesicles with a test dye, acridine orange (AO) using the pH-gradient (remote loading) method. The AO release property of liposomes was tested with a special vertical diffusion cell after we had made PVA adsorb on their surface in different PVA/lipid (w/w) ratios.     

2-Phosphonobutane-1,2,4,-Tricarboxylic Acid (PBTC): pH-Dependent Behavior Studied by Means of Multinuclear NMR Spectroscopy

Although 2-phosphonobutane-1,2,4,-tricarboxylic acid, PBTC, has manifold industrial applications, relevant and reliable data on the protonation of PBTC are poor. However, these data are critical parameters for ascertaining PBTC speciation, especially with regard to a sound structural and thermodynamic characterization of its metal ion complexes. A rigorous evaluation of pH-dependent ¹H, ¹³C, and ³¹P chemical shifts along with accessible scalar spin–spin coupling constants (J) was performed in order to determine the pK_a values of PBTC in 0.5 molal NaCl aqueous solution by means of nuclear magnetic resonance (NMR) spectroscopy. The phosphonate group revealed pK_a values of 0.90 ± 0.02 and 9.79 ± 0.02, and the pK_a values associated with the carboxylic groups are 3.92 ± 0.02, 4.76 ± 0.03, and 6.13 ± 0.03. Supported by DFT-calculated structures revealing strong intramolecular hydrogen bonding, the sequence of deprotonation could be unambiguously determined.     

Insights into the Reactivity of Gold–Dithiocarbamato Anticancer Agents toward Model Biomolecules by Using Multinuclear NMR Spectroscopy

Some gold(III)–dithiocarbamato derivatives of either single amino acids or oligopeptides have shown promise as potential anticancer agents, but their capability to interact with biologically relevant macromolecules is still poorly understood. We investigated the affinity of the representative complex [Au^IIIBr₂(dtc‐Sar‐OCH₃)] (dtc: dithiocarbamate; Sar: sarcosine (N‐methylglycine)) with selected model molecules for histidine‐, methionine‐, and cysteine‐rich proteins (that is, 1‐methylimidazole, dimethylsulfide, and N‐acetyl‐L ‐cysteine, respectively). In particular, detailed mono‐ and multinuclear NMR studies, in combination with multiple ¹³C/¹⁵N enrichments, allowed interactions to be followed over time and indicated somewhat unexpected reaction pathways. Whereas dimethylsulfide proved to be unreactive, a sudden multistep redox reaction occurred in the presence of the other potential sulfur donor, N‐acetyl‐L ‐cysteine (confirmed if glutathione was used instead). On the other hand, 1‐methylimidazole underwent an unprecedented acid–base reaction with the gold(III) complex, rather than the expected coordination to the metal center by replacing, for instance, a bromide. Our results are discussed herein and compared with the data available in the literature on related complexes; our findings confirm that the peculiar reactivity of gold(III)–dithiocarbamato complexes can lead to novel reaction pathways and, therefore, to new cytotoxic mechanisms in cancer cells.     

Differences in Human Plasma Protein Interactions between Various Polymersomes and Stealth Liposomes as Observed by Fluorescence Correlation Spectroscopy

A significant factor hindering the clinical translation of polymersomes as vesicular nanocarriers is the limited availability of comparative studies detailing their interaction with blood plasma proteins compared to liposomes. Here, polymersomes are self-assembled via film rehydration, solvent exchange, and polymerization-induced self-assembly using five different block copolymers. The hydrophilic blocks are composed of anti-fouling polymers, poly(ethylene glycol) (PEG) or poly(2-methyl-2-oxazoline) (PMOXA), and all the data is benchmarked to PEGylated “stealth” liposomes. High colloidal stability in human plasma (HP) is confirmed for all but two tested nanovesicles. In situ fluorescence correlation spectroscopy measurements are then performed after incubating unlabeled nanovesicles with fluorescently labeled HP or the specific labeled plasma proteins, human serum albumin, and clusterin (apolipoprotein J). The binding of HP to PMOXA-polymersomes could explain their relatively short circulation times found previously. In contrast, PEGylated liposomes also interact with HP but accumulate high levels of clusterin, providing them with their known prolonged circulation time. The absence of significant protein binding for most PEG-polymersomes indicates mechanistic differences in protein interactions and associated downstream effects, such as cell uptake and circulation time, compared to PEGylated liposomes. These are key observations for bringing polymersomes closer to clinical translation and highlighting the importance of such comparative studies.     

丝光沸石水蒸气/酸浸渍脱铝的多核固体核磁共振研究

采用¹H,²⁹Si,²⁷Al魔角旋转固体核磁共振(MASNMR)及¹H-²⁹Si交叉极化(CP)技术研究丝光沸石水蒸气/酸浸渍脱铝过程中各种铝物质的结构与性质.结果表明,丝光沸石上骨架铝原子在水分子作用下,生成非骨架四配位铝物质[Al(OH)₃(H₂O)],分别在²⁷Al谱δ45和¹H谱δ3.0处出现共振信号,这种铝物质不同于扭曲四配位铝,在高温下进一步水合生成Al(OH)₃(H₂O)₂和Al(OH)₃(H₂O)₃,即非骨架五配位和六配位铝物质.¹H-²⁹SiCP和¹H谱证实,水蒸气脱铝使丝光沸石产生了大量的硅羟基和铝羟基.     

四臂星形聚苯乙烯在良溶剂和0溶剂中分子扩散的光子相关光谱的研究

用光子相关光谱研究了四臂星形聚苯乙烯在良溶剂(四氢呋喃THF)和θ溶剂(环己烷CH)中扩散系数与溶剂的浓度和温度的依赖关系。用累积量方法分析光子相关数据给出了多分散样品的Z均扩散系数。在θ溶剂中,高于或低于θ温度时,聚合物在溶液中的分子扩散分别表现出具有在良溶剂与不良溶剂中的行为。外推浓度至零,得到无限稀时不同温度的分子扩散系数,借助Stokes-Einstein方程,给出了聚合物的流体力学半径。通过InD对I/T作图,得到了星形聚苯乙烯在THF与CH中的扩散活化能。     

Relative Configuration and Conformation of 5-(Dimethoxyphosphoryl)-2-methoxy-1,2λ5-oxaphospholan-2-ones by Multinuclear NMR Spectroscopy

Information on the hitherto unknown relative configuration and on the conformation of the title compounds in solution can be derived from nuclear Overhauser effects and coupling constants. Whereas the bridged 5-(dimethoxyphosphoryl)-2-methoxy-1,2λ⁵-oxaphospholan-2-ones 6 and 7 are sterically strained and, therefore, conformationally rigid, the C(3)-unsubstituted compound 1 does not show a preferred solution conformation. Phenyl substituents at C(3) (compounds 2 – 5 ) tend to adopt a pseudoequatorial position, this way leading to a definite conformation of the respective compounds. The influence of the conformation on the NMR spectra is discussed. ³¹P-NMR Spectroscopy is ideally suited for the characterization and quantification of the isomers 2 – 5 present in the reaction mixture.     

Detection of Hindered Rotation and Inversion by NMR Spectroscopy

Rotations and inversions in organic molecules are readily recognizable from the temperature dependence of the NMR spectra. The study of the effects of substituents on the activation barriers of such processes permits the elucidation of reaction mechanisms, and the stability limits of isomers can also be determined. The knowledge of the stability limits is necessary for the specific synthesis of stable rotamers and invertomers.     

Interaction of Nonionic Block Copolymeric (Poloxamer) Surfactants with Poly (Acrylic Acid), Studied by Photon Correlation Spectroscopy

The interaction between certain hydrophilic pluronic (poloxamer) surfactants and a poly (acrylic acid) has been investigated. Both the PPO and the PEO groups of the surfactants, and the -COOH groups and aliphatic side chains of the PAA molecule, were found to be crucial in this interaction to form complexes. At pH 2 and with a low poloxamer:PAA molar ratio, maximum interaction was observed, giving rise to large-sized complexes that were unstable but possessing bioadhesive properties. At the same pH but with higher poloxamer:PAA molar ratio, the complexes became smaller in size and more stable and were used to prepare stable w/o/w emulsions. A further increase in the poloxamer:PAA molar ratio or increase in the pH causes a further decrease in particle size with eventual nonformation of complexes. Interaction and stability studies of the complexes were done using photon correlation spectroscopy. The overall interaction appears to be a combination of hydrophobic interaction and hydrogen bonding. This has given rise to a unique ratio which we have called the [oxyphobic]/[oxyphilic] ratio or OOR. The interaction was found to depend on the molar ratio between poloxamer surfactants and PPA; the [O]_total/[-COOH] ratio; the size of the PPO hydrophobe, and the pH of the reaction mixture. pH measurement studies of these mixtures also gave similar results.     

Multinuclear Diffusion NMR Spectroscopy and DFT Modeling: A Powerful Combination for Unraveling the Mechanism of Phosphoester Bond Hydrolysis Catalyzed by Metal‐Substituted Polyoxometalates

A detailed reaction mechanism is proposed for the hydrolysis of the phosphoester bonds in the DNA model substrate bis(4‐nitrophenyl) phosphate (BNPP) in the presence of the Zr^IV‐substituted Keggin type polyoxometalate (Et₂NH₂)₈[{α‐PW₁₁O₃₉Zr(μ‐OH) (H₂O)}₂] ? 7 H₂O (ZrK 2:2) at pD 6.4. Low‐temperature ³¹P DOSY spectra at pD 6.4 gave the first experimental evidence for the presence of ZrK 1:1 in fast equilibrium with ZrK 2:2 in purely aqueous solution. Moreover, theoretical calculations identified the ZrK 1:1 form as the potentially active species in solution. The reaction intermediates involved in the hydrolysis were identified by means of ¹H/³¹P NMR studies, including EXSY and DOSY NMR spectroscopy, which were supported by DFT calculations. This experimental/theoretical approach enabled the determination of the structures of four intermediate species in which the starting compound BNPP, nitrophenyl phosphate (NPP), or the end product phosphate (P) is coordinated to ZrK 1:1. In the proposed reaction mechanism, BNPP initially coordinates to ZrK 1:1 in a monodentate fashion, which results in hydrolysis of the first phosphoester bond in BNPP and formation of NPP. EXSY NMR studies showed that the bidentate complex between NPP and ZrK 1:1 is in equilibrium with monobound and free NPP. Subsequently, hydrolysis of NPP results in P, which is in equilibrium with its monobound form.     

Study of Lysozyme Glycation Reaction by Mass Spectrometry and NMR Spectroscopy

The Advanced Glycation End Products (AGEs) are the causative substances of lifestyle‐habit illness. To elucidate the glycation mechanism of the protein, the reaction of lysozyme with D ‐glucose was analyzed by the fluorescence, TOF‐MS, and ¹³C‐NMR spectroscopy under the physiological condition. The fluorescence intensity of lysozyme in the glycation solution increased proportionally with a reaction time of ten weeks. The MALDI‐TOF‐MS spectra of the reaction solution after two weeks showed a peak at m/z 15066, which indicated the presence of a larger molecule than the native lysozyme (m/z 14331), and new peaks at m/z 30105 (dimer) and 45000 (trimer) were also observed. The spectral analysis supported the assumption of a continuous glycation reaction of D ‐glucose with lysozyme and a 30% transformation of lysozyme to the dimeric form during ten weeks. The ¹³C‐NMR spectra of lysozyme showed six [¹³C]‐labeled signals by the glycation reaction with [¹³C]‐glucose after two weeks of reaction. The combined analysis of TOF‐MS and ¹³C‐NMR spectra uncovered that first products of the glycation reaction of lysozyme with D ‐glucose can be observed already three hours after starting the reaction and that nine D ‐glucose units are attached during ten weeks at 37°.     

分子筛材料的酸性和择形选择性的固体核磁共振研究

分子筛材料具有酸性可调节和择形选择性的优势, 因而在多相催化反应中表现出优异的性能. 本文综述了利用固体核磁共振(ssNMR)光谱对分子筛的酸性和择形选择性进行研究的最新进展. 通过采用或不采用探针分子的ssNMR技术, 探测了分子筛中酸性位的数量、 酸强、 酸类型及酸位之间的协同作用. 此外, 通过直接观察多相催化反应中关键中间体的存在, ssNMR光谱提供了分子筛择形选择性的证据. 酸性和择形选择性的协同作用有助于更好地设计分子筛材料, 以实现更好的多相催化.     

Mechanisms and Beyond: Elucidation of Fluxional Dynamics by Exchange NMR Spectroscopy

Detailed mechanistic information is crucial to our understanding of reaction pathways and selectivity. Dynamic exchange NMR techniques, in particular 2D exchange spectroscopy (EXSY) and its modifications, provide indispensable intricate information on the mechanisms of organic and inorganic reactions and other phenomena, for example, the dynamics of interfacial processes. In this Review, key results from exchange NMR studies of small molecules over the last few decades are systemised and discussed. After a brief introduction to the theory, the key types of dynamic processes are identified and fundamental examples given of intra- and intermolecular reactions, which, in turn, could involve, or not, bond-making and bond-breaking events. Following that logic, internal molecular rotation, intramolecular stereomutation and molecular recognition will first be considered because they do not typically involve bond breaking. Then, rearrangements, substitution-type reactions, cyclisations, additions and other processes affecting chemical bonds will be discussed. Finally, interfacial molecular dynamics and unexpected combinations of different types of fluxional processes will also be highlighted. How exchange NMR spectroscopy helps to identify conformational changes, coordination and molecular recognition processes as well as quantify reaction energy barriers and extract detailed mechanistic information by using reaction rate theory in conjunction with computational techniques will be shown.     

NMR Crystallography of an Oxovanadium(V) Complex by an Approach Combining Multinuclear Magic Angle Spinning NMR,DFT, and Spin Dynamics Simulations

Bioinorganic vanadium(V) solids are often challenging for structural analysis. Here, we explore an NMR crystallography approach involving multinuclear ¹³C/⁵¹V solid‐state NMR spectroscopy, density functional theory (DFT), and spin dynamics numerical simulations, for the spectral assignment and the 3D structural analysis of an isotopically unmodified oxovanadium(V) complex, containing 17 crystallographically inequivalent ¹³C sites. In particular, we report the first NMR determination of C–V distances. So far, the NMR observation of ¹³C–⁵¹V proximities has been precluded by the specification of commercial NMR probes, which cannot be tuned simultaneously to the close Larmor frequencies of these isotopes (100.6 and 105.2 MHz for ¹³C and ⁵¹V, respectively, at 9.4 T). By combining DFT calculations and ¹³C–⁵¹V NMR experiments, we propose a complete assignment of the ¹³C spectrum of this oxovanadium(V) complex. Furthermore, we show how ¹³C–⁵¹V distances can be quantitatively estimated.     

Observation and Kinetic Characterization of Transient Schiff Base Intermediates by CEST NMR Spectroscopy

In aqueous solution, many biochemical reaction pathways involve reaction of an aldehyde with an amine, which progresses through generally unstable, hydrated and dehydrated, Schiff base intermediates that often are unobservable by conventional NMR. There are 4 states in the relevant equilibrium: 1) gem‐diol, 2) aldehyde, 3) hemiaminal, and 4) Schiff base. For the reaction between protein amino groups and DOPAL, a highly toxic metabolite of dopamine, the ¹H resonances of both the hemiaminal and the dehydrated Schiff base can be observed by CEST NMR, even when their populations fall below 0.1 %. CEST NMR reveals the quantitative exchange kinetics between reactants and Schiff base intermediates, explaining why the Schiff base NMR signals are rarely observed. The reactivity of DOPAL with N^α‐amino groups is greater than with lysine N^?‐amines and, in the presence of O₂, both types of Schiff base DOPAL–peptide intermediates rapidly react with free DOPAL to irreversibly form dicatechol pyrrole adducts.     

Conformational Analysis of Guaianolide-Type Sesquiterpene Lactones by Low-Temperature NMR Spectroscopy and Semiempirical Calculations

Conformational analysis of 9-acetoxycumambrine A 1 and 8-O-isobutiryl-9-acetoxycumambrine B 2 was carried out by low-temperature NMR studies. Results suggested that lactones 1 and 2 are mixtures of two distinctive conformers, I and II. Based on low-temperature ¹H NMR spectra, in four solvents, the thermodynamic parameters of I II exchange process were assessed. Energy of activation of I II reaction was obtained by dynamic NMR simulations for both compounds. Results revealed that conformational exchange of lactones 1 and 2 occurs due to chair twisted chair interconversion of a heptane ring. The same PM3 semiempirical method was applied for geometry optimization of lactones 1 and 2, as well as of 9-hydroxycumambrine A 3, 9-acetoxycumambrine B 4, and cumambrine B 5.     

Polymer-Solvent Interactions in Solutions of Thermoresponsive Polymers Studied by NMR and IR Spectroscopy

Summary: NMR relaxation and diffusion coefficient measurements revealed that a portion of water molecules is bound in mesoglobules formed in poly(N-isopropylmethacrylamide) (PIPMAm) and poly(vinyl methyl ether) (PVME) aqueous solutions above the LCST, with fast exchange between bound and free states (residence time ∼1 ms). Two types of bound water molecules were assigned to water bound inside mesoglobules and on their surface. For highly concentrated PVME/D₂O solutions (c ≥ 20 wt%) a slow exchange was detected by NMR for bound water (residence time = 2.1 s). For PIPMAm aqueous solution IR spectra indicate a two-steps character of the phase transition. For PIPMAm in D₂O/ethanol (EtOH) mixtures the globular structures were observed by NMR at 298 K for certain compositions of the mixed solvent (cononsolvency effect). Virtually no EtOH is bound in these globular structures, in contrast to the temperature-induced globular structures.     

Exploring the Anion–Cation Interaction in m‐Terphenyltetrafluorosilicates by Using Multinuclear NMR Spectroscopy,X‐ray Diffraction,and ICR‐FT‐MS

The synthesis of a series of m‐terphenyl‐substituted tetrafluorosilicates with different cations (Na⁺, K⁺, Rb⁺, Cs⁺, Ag⁺, Tl⁺) is described and the interactions between the anion and cation are investigated in the solid, solution, and gas states by using multinuclear NMR spectroscopy, X‐ray diffraction, and ion cyclotron resonance Fourier‐transform mass spectrometry (ICR‐FT‐MS). In solution, heteronuclear NMR spectroscopy parameters show only limited sensitivity to the nature of the cation, which furthermore can be affected by solvent effects. More pronounced effects are observed in the structural data obtained from X‐ray diffraction studies, which are in good agreement with experimental gas‐phase data from ESIMS. ESIMS also reveals the existence of dimeric species of the type [M(DmpSiF₄)₂]^? (Dmp=2,6‐dimesitylphenyl), the stability of which was determined by normalized collision energy experiments.