Comparative study of three teicoplanin-based chiral stationary phases using the linear free energy relationship model

Teicoplanin (T) is a macrocyclic glycopeptide that is highly effective as a chiral selector for enantiomeric separations. In this study, we used three teicoplanin-based chiral stationary phases (CSPs) - native teicoplanin, teicoplanin aglycon (TAG) and recently synthesized methylated teicoplanin aglycon (MTAG). In order to examine the importance of various interaction types in the chiral recognition mechanism the three related CSPs were evaluated and compared using a linear free energy relationship (LFER). The capacity factors of 19 widely different solutes, with known solvation parameters, were determined on each of the columns under the same mobile phase conditions used for the chiral separations. The regression coefficients obtained revealed the magnitude of the contribution of individual interaction types to the retention on the compared columns under those specific experimental conditions. Statistically derived standardized regression coefficients were used to evaluate the contribution of individual molecular interactions within one stationary phase. It has been concluded that intermolecular interactions of the hydrophobic type significantly contribute to retention on all the CSPs studied here. Other retention increasing factors are n- and pi-electron interactions and dipole-dipole or dipole-induced dipole ones, while hydrogen donating or accepting interactions are more predominant with the mobile phase than with the stationary phases. However, these types of interactions are not equally significant for all the CSPs studied.     

Preservation strategies for inorganic arsenic species in high iron,low-<Emphasis Type="Italic">Eh</Emphasis> groundwater from West Bengal,India

Despite the importance of accurately determining inorganic arsenic speciation in natural waters to predicting bioavailability and environmental and health impacts, there remains considerable debate about the most appropriate species preservation strategies to adopt. In particular, the high-iron, low-Eh (redox potential) shallow groundwaters in West Bengal, Bangladesh and SE Asia, the use of which for drinking and irrigation purposes has led to massive international concerns for human health, are particularly prone to changes in arsenic speciation after sampling. The effectiveness of HCl and EDTA preservation strategies has been compared and used on variably arsenic-rich West Bengali groundwater samples, analysed by ion chromatography–inductively coupled plasma–mass spectrometry (IC–ICP–MS). Immediate filtration and acidification with HCl followed by refrigerated storage was found to be the most effective strategy for minimizing the oxidation of inorganic As(III) during storage. The use of a PRP-X100 (Hamilton) column with a 20 mmol L^–1 NH₄H₂PO₄ as mobile phase enabled the separation of Cl^– from As(III), monomethylarsonic acid, dimethylarsinic acid and As(V), thereby eliminating any isobaric interference between ⁴⁰Ar³⁵Cl⁺ and ⁷⁵As⁺. The use of EDTA as a preservative, whose action is impaired by the high calcium concentrations typical of these types of groundwater, resulted in marked oxidation during storage. The use of HCl is therefore indicated for analytical methods in which chloride-rich matrices are not problematical. The groundwaters analysed by IC–ICP–MS were found to contain between 5 and 770 ng As mL^–1 exclusively as inorganic arsenic species. As(III)/total-As varied between 0 and 0.94.     

Development of a relaxation-inducing cluster expansion formalism for treating strong relaxation and correlation effects

We present in this paper a comprehensive account of an explicitly spin-free coupled cluster theory for treating energy differences of open-shell states relative to a closed-shell ground state, where the open-shell states of interest are dominated by a few simple configuration state functions. We develop a valence-universal coupled cluster formalism to achieve this via a novel cluster expansion ansatz for the valence part of the wave operator, where the orbital relaxation and the correlation relaxation accompanying ionization/excitation from the ground state are taken care of to all orders in compact, efficient, and explicitly spin-free manner. The essential difference of our proposed ansatz from the ordinary and the normal-ordered cluster ansatz in vogue is that (a) we allow the valence cluster operators to be connected among themselves with spectator valence lines only and (b) we use suitable combinatoric factors accompanying powers of cluster operators thus connected, which are equal to the number of ways the operators can be joined, leading to the same excitation (the automorphic factor). We emphasize that such an ansatz does not generate terms (diagrams) with chains of cluster operators joined among themselves via spectator lines only. Barring only a few, almost all the terms in the working equations determining the cluster amplitudes involve contraction of the Hamiltonian with the cluster operators via at least one nonspectator line, leading to what we call a "strongly connected" series. The structure of the working equation is remarkably similar to the single-reference closed-shell equation, with a few additional terms. The presence of contractions among cluster operators via spectator lines introduces the additional physical effects of orbital and correlation relaxation using low-body cluster operators. As an illustrative application of the new multireference coupled cluster (CC) theory, we consider in this paper computation of ionization potentials (IPs) of one-valence problem with only one active orbital. The numerical applications are made for both the core- and the inner- and outer-valence IPs for several molecular systems. The numerical values demonstrate the superiority of the relaxation-inducing CC theory, as compared to the normal-ordered ansatz.     

Two new mononuclear cobalt(II) complexes of pyrazole-based ligands: synthesis,structures and magnetic studies

We have synthesized two mononuclear cobalt(II) complexes (1 and 2) of pyrazole-based bidentate (NN) and tridentate (NNN) tripodal ligands. X-ray crystal structure determination reveals that complex 1 has a tetrahedral geometry, while complex 2 has a trigonal–bipyramidal geometry. Both the complexes have been characterized by variable-temperature magnetic measurements between 2 and 300 K. A weak ferromagnetic exchange interaction (J = +1.5 cm^?1) is observed for complex 2. Due to the presence of supramolecular CH···Cl and π···π interactions, a good magnetostructural correlation was found between the D parameter and angular distortion (δ) for complex 1 and related complexes reported in the literature.     

A phenoxo–azido assorted Schiff base copper(II) bridged dimer in trace level fluorescence sensing of a pesticide: a DFT supported phenomenon

A binuclear phenoxo- and azido-bridged copper(II) Schiff base complex has been synthesized along with its mononuclear copper-Schiff base analog. The compounds have been characterized by IR spectroscopy and CHN elemental analysis. The single-crystal structure and variable temperature magnetic properties of the binuclear compound have been studied from the X-ray crystallographic data and superconducting quantum interference device magnetometry, respectively. The synthesized crystalline binuclear complex has interesting spectral features that allow it to act as a spectral sensor toward an organophosphorus pesticide which is a potential environmental toxicant coming to the environment as agricultural waste. Although both the mononuclear and binuclear complexes are suitable as sensors for the organophosphorus, the binuclear complex being crystalline is suitable for attaining structural and mechanistic details of the interaction. Density functional theory calculations and ESI MS analysis of the interactions with the binuclear complex suggest that the binding of organophosphorus substrate with 2 occurs through one copper center.     

Three‐Arm,Biotin‐Tagged Carbazole–Dicyanovinyl–Chlorambucil Conjugate: Simultaneous Tumor Targeting,Sensing, and Photoresponsive Anticancer Drug Delivery

The design, synthesis, and in vitro biological studies of a biotin–carbazole–dicyanovinyl–chlorambucil conjugate (Bio‐CBZ‐DCV‐CBL; 6 ) are reported. This conjugate ( 6 ) is a multifunctional single‐molecule appliance composed of a thiol‐sensor DCV functionality, a CBZ‐derived phototrigger as well as fluorescent reporter, and CBL as the anticancer drug, and Bio as the cancer‐targeting ligand. In conjugate 6 , the DCV bond undergoes a thiol–ene click reaction at pH<7 with intracellular thiols, thereby shutting down internal charge transfer between the donor CBZ and acceptor DCV units, resulting in a change of the fluorescence color from green to blue, and thereby, sensing the tumor microenvironment. Subsequent photoirradiation results in release of the anticancer drug CBL in a controlled manner.     

A Three‐Site Mechanism for Agonist/Antagonist Selective Binding to Vasopressin Receptors

Molecular‐dynamics simulations with metadynamics enhanced sampling reveal three distinct binding sites for arginine vasopressin (AVP) within its V₂‐receptor (V₂R). Two of these, the vestibule and intermediate sites, block (antagonize) the receptor, and the third is the orthosteric activation (agonist) site. The contacts found for the orthosteric site satisfy all the requirements deduced from mutagenesis experiments. Metadynamics simulations for V₂R and its V_1aR‐analog give an excellent correlation with experimental binding free energies by assuming that the most stable binding site in the simulations corresponds to the experimental binding free energy in each case. The resulting three‐site mechanism separates agonists from antagonists and explains subtype selectivity.     

Selective Killing of Breast Cancer Cells by Doxorubicin‐Loaded Fluorescent Gold Nanoclusters: Confocal Microscopy and FRET

Fluorescent gold nanoclusters (AuNCs) capped with lysozymes are used to deliver the anticancer drug doxorubicin to cancer and noncancer cells. Doxorubicin‐loaded AuNCs cause the highly selective and efficient killing (90 %) of breast cancer cells (MCF7) (IC₅₀=155 nm ). In contrast, the killing of the noncancer breast cells (MCF10A) by doxorubicin‐loaded AuNCs is only 40 % (IC₅₀=4500 nm ). By using a confocal microscope, the fluorescence spectrum and decay of the AuNCs were recorded inside the cell. The fluorescence maxima (at ≈490–515 nm) and lifetime (≈2 ns), of the AuNCs inside the cells correspond to Au_10–13. The intracellular release of doxorubicin from AuNCs is monitored by Förster resonance energy transfer (FRET) imaging.     

Internalization of Ineffective Platinum Complex in Nanocapsules Renders It Cytotoxic

Anticancer therapy by platinum complexes, based on nanocarrier‐based delivery, may offer a new approach to improve the efficacy and tolerability of the platinum family of anticancer drugs. The original rules for the design of new anticancer platinum drugs were affected by the fact that, although cisplatin (cis‐[PtCl₂(NH₃)₂) was an anticancer drug, its isomer transplatin was not cytotoxic. For the first time, it is demonstrated that simple encapsulation of an inactive platinum compound in phospholipid bilayers transforms it into an efficient cytotoxic agent. Notably, the encapsulation of transplatin makes it possible to overcome the resistance mechanisms operating in cancer cells treated with cisplatin and prevents inactivation of transplatin in the extracellular environment. It is also shown that transplatin delivered to the cells in nanocapsules, in contrast to free (nonencapsulated) complex, forms cytotoxic cross‐links on DNA.