Investigation of the Selectivity of L-Type Voltage-Gated Calcium Channels 1.3 for Pyrimidine-2,4,6-Triones Derivatives Based on Molecular Dynamics Simulation

Human Ca_v1.3 (hCa_v1.3) is of great interest as a potential target for Parkinson’s disease. However, common medications like dihydropyridines (DHPs), a kind of classic calcium channel blocker, have poor selectivity to hCa_v1.3 in clinical treatment, mainly due to being implicated in cardiovascular side-effects mediated by human Ca_v1.2 (hCa_v1.2). Recently, pyrimidine-2,4,6-triones (PYTs) have received extensive attention as prominent selective inhibitors to hCa_v1.3. In this study, we describe the selectivity mechanism of PYTs for hCa_v1.2 and hCa_v1.3 based on molecular dynamic simulation methods. Our results reveal that the van der Waals (vdW) interaction was the most important force affecting selectivity. Moreover, the hydrophobic interaction was more conducive to the combination. The highly hydrophobic amino acid residues on hCa_v1.3, such as V162 (IR1), L303 (IR2), M481 (IR3), and F484 (IR3), provided the greatest contributions in the binding free energy. On the other hand, the substituents of a halogen-substituted aromatic ring, cycloalkyl and norbornyl on PYTs, which are pertinent to the steric hindrance of the compounds, played core roles in the selectivity and affinity for hCa_v1.3, whereas strong polar substituents needed to be avoided. The findings could provide valuable information for designing more effective and safe medicines for Parkinson’s disease.     

Synthesis and biological evaluation of anthranilamide-based non-peptide mimetics of ω-conotoxin GVIA

Non-peptide mimetics based on an anthranilamide ‘scaffold’ possessing fragments that mimic Lys2, Tyr13 and Arg17 in ω-conotoxin GVIA have been prepared. Compounds were assayed for binding to the voltage-gated calcium channels Ca_v2.2 (‘N-type’) and Ca_v2.1 (‘P/Q-type’) in rat brain. The primary synthetic target, 2-(6-amino-hexanoylamino)-5-(3-guanidino-propoxy)-N-[4-(4-hydroxyphenoxy)-phenyl]-benzamide (2a), exhibited low μM binding to Ca_v2.2 and was more than 30-fold selective for Ca_v2.2 over Ca_v2.1.     

Monoterpene Indole Alkaloids with Cav3.1 T-Type Calcium Channel Inhibitory Activity from Catharanthus roseus

Catharanthus roseus is a well-known traditional herbal medicine for the treatment of cancer, hypertension, scald, and sore in China. Phytochemical investigation on the twigs and leaves of this species led to the isolation of two new monoterpene indole alkaloids, catharanosines A (1) and B (2), and six known analogues (3–8). Structures of 1 and 2 were established by ¹H-, ¹³C- and 2D-NMR, and HREIMS data. The absolute configuration of 1 was confirmed by single-crystal X-ray diffraction analysis. Compound 2 represented an unprecedented aspidosperma-type alkaloid with a 2-piperidinyl moiety at C-10. Compounds 6–8 exhibited remarkable Ca_v3.1 low voltage-gated calcium channel (LVGCC) inhibitory activity with IC₅₀ values of 11.83 ± 1.02, 14.3 ± 1.20, and 14.54 ± 0.99 μM, respectively.     

PET Diagnostic Molecules Utilizing Multimeric Cyclic RGD Peptide Analogs for Imaging Integrin αvβ3 Receptors

Multimeric ligands consisting of multiple pharmacophores connected to a single backbone have been widely investigated for diagnostic and therapeutic applications. In this review, we summarize recent developments regarding multimeric radioligands targeting integrin α_vβ₃ receptors on cancer cells for molecular imaging and diagnostic applications using positron emission tomography (PET). Integrin α_vβ₃ receptors are glycoproteins expressed on the cell surface, which have a significant role in tumor angiogenesis. They act as receptors for several extracellular matrix proteins exposing the tripeptide sequence arginine-glycine-aspartic (RGD). Cyclic RDG peptidic ligands c(RGD) have been developed for integrin α_vβ₃ tumor-targeting positron emission tomography (PET) diagnosis. Several c(RGD) pharmacophores, connected with the linker and conjugated to a chelator or precursor for radiolabeling with different PET radionuclides (¹⁸F, ⁶⁴Cu, and ⁶⁸Ga), have resulted in multimeric ligands superior to c(RGD) monomers. The binding avidity, pharmacodynamic, and PET imaging properties of these multimeric c(RGD) radioligands, in relation to their structural characteristics are analyzed and discussed. Furthermore, specific examples from preclinical studies and clinical investigations are included.     

Calculation of the rotational constants A and C for isotopic species of slightly perturbed CH3CN symmetric top molecules

A technique which was employed earlier to calculate the rotational constants of CH₃CCH has been extended to the ground and two vibrational levels in thev ₈ vibration of CH₃CN for several isotopic species. The moments of inertia and a computer iteration technique over experimental data for each isotopic species were employed to evaluate the constantA _v in an excited vibrational state for a symmetric top molecule. This method gave good estimates forA _v for each isotope. The angle of bending and the orientation of each molecular system in reference frames, one fixed on the carbon atom at the -CN site and the other at the center of mass, were explored. These results are discussed in this paper. The method, which was applied by Tam and Roberts to the nv₁₀,n=1, 2, 3, 4, vibrations of CH₃CCH earlier and which was extended to thev ₁₀=1 vibration of CH₃CCH with¹³C isotopic species, has been applied to¹³C isotopic species of CH₃CN and seems to be a useful tool to extract the value ofA ₀. Each of these molecules shows reasonable dependency ofA _v over vibrational levels. Values ofA _v calculated from the geometrical model are in good agreement with those obtained by fitting the terms in the frequency equations, which containedA _v , to the experimental data through an iteration technique in which the value ofA was allowed to vary.     

New cyclic RGD peptides: synthesis,characterization, and theoretical activity towards αvβ3 integrin

Two new cyclic RGD peptides were prepared using a click chemistry approach. The linear RGDfV peptide was synthesized by solid-phase peptide synthesis using a 9-fluorenylmetoxicarbonyl (Fmoc) strategy and a 2-chlorotrityl chloride resin. After coupling 5-hexynoic acid the peptide was cleaved from the resin and linked to propargylamine. The bis-alkynyl RGDfV peptide was then reacted with two different bis-azides by treatment with copper iodide and triethylamine. These two cyclic RGD peptides were characterized by NMR and HRMS. In order to evaluate the interaction of these new compounds with integrin α_vβ₃ docking experiments were carried out and the results compared with those obtained with cyclo(RGDf[N–Me]V) (Cilengitide). The two new cyclic RGD peptides showed a higher affinity to the α_vβ₃ integrin when compared with Cilengitide thus representing two new potential integrin α_vβ₃ antagonists.     

Structure and magnetism of rare-earth-substituted Ca3Co2O6

Yttrium- and rare-earth-substituted derivatives of Ca_3−vR_vCo₂O₆ (RY, Pr, Nd, Sm, Eu, Gd, Tb, Dy, Ho, Yb, and Lu) have been synthesized and structurally characterized by powder X-ray and neutron diffraction. All phases adopt the K₄CdCl₆-type structure with space group R3¯c), in which the trivalent R³⁺ substituents randomly occupy the Ca²⁺ site. The homogeneity range of Ca_3−vR_vCo₂O₆ extends to v≈0.90 for the substituents concerned. A significant increase in the Co2-O distances within the trigonal-prismatic Co2O₆ co-ordination polyhedra upon introduction of R³⁺ confirms that extra electrons from the R³⁺-for-Ca²⁺ substitution exclusively enter the Co2 site of the quasi-one-dimensional Ca_3−vR_vCo₂O₆ structure, thereby formally reducing its oxidation state. This is furthermore supported by magnetic susceptibility and low-temperature neutron diffraction measurements. The long-range ferrimagnetic ordering temperature is reduced upon R substitution and appears to vanish for v>∼0.30.     

Crystal structure and magnetic properties of the solid-solution phase Ca3Co2-vMnvO6

The homogeneity range of the Ca₃Co_2-vMn_vO₆ solid-solution phase covers the entire composition interval from v=0 to 1. A systematic powder X-ray and neutron diffraction, magnetic susceptibility, and magnetization study has been carried out to investigate effects of the Mn-for-Co substitution on structural and magnetic properties. The Mn substitution concerns primarily only the octahedral Co1 site of the Ca₃Co1Co2O₆ crystal structure, whereas the trigonal-prismatic Co2 site structurally is left essentially unaffected. The Ca₃Co_2-vMn_vO₆ crystal structure belongs to space group with unit-cell dimensions (in hexagonal setting) 9.084?a?9.134 Å and 10.448?c?10.583 Å. A cut through the magnetic phase diagram at 10 K shows a ferrimagnetic domain for 0?v<∼0.3 and an antiferromagnetic domain for ∼0.50<v<∼1. The magnetic ordering temperatures are quite low (<∼25/18 K), and even so further magnetic transitions appear to take place at still lower temperature. The legitimity and reliability of the different indicators used to establish the magnetic transitions, their individual accuracy, and mutual consistency are briefly discussed. Variable parameters of the crystal and magnetic structures of Ca₃Co1_1-vMn_vCo2O₆ are determined and their variation with v is briefly discussed in relation to chemical bonding. The magnetic structure in the ferrimagnetic region is essentially the same as that of the pristine v=0 phase, but since the moments at the Co2 site decrease and those at the (Co1,Mn) site increase with increasing v; characteristic traits of ferrimagnetism in magnetic susceptibility and magnetization gradually disappear. The magnetic arrangement in the antiferromagnetic region is characterized by differently sized moments at the (Co1,Mn) and Co2 sites, moments at adjacent sites in each of these sublattices being oppositely oriented along [001].     

Biological Studies of Some 2,4-Dichloro-5-fluorophenyl Containing Triazolothiadiazoles

Summary. A series of dichlorofluorophenyl containing triazolothiadiazoles were obtained by cyclocondensation of triazole with substituted benzoic, aryloxyacetic, and anilinoacetic acids using POCl₃ as cyclizing agent. The structures of the newly synthesized compounds were characterized and confirmed by IR, ¹H NMR, mass spectra, and elemental analysis. Selected compounds were screened for their antitubercular activity against Mycobacterium tuberculosis. The compound bearing 2,4-dichloro-5-fluorophenyl moiety at position 3, and 6 of the triazolothiadiazole showed excellent activity in vitro primary screening. Compounds with 3-chloro-4-fluorophenyl and 4-fluorophenoxymethyl moieties at position 6 of the triazolothiadiazole showed very good analgesic activity. Triazolothiadiazole with 4-chlorophenyl, 4-fluoro-3-phenoxyphenyl, and 2,4-dichloro-5-fluorophenyl moieties showed excellent antimicrobial activity against the tested strains at 6.25 μg cm⁻³ concentrations.     

Crystal structure and magnetic properties of the solid-solution phase Ca3Co2−vScvO6

The two crystallographically non-equivalent Co atoms of the quasi-one-dimensional crystal structure of Ca₃Co₂O₆ form chains with alternating, face-sharing polyhedra of Co2O₆ trigonal prisms and Co1O₆ octahedra. This compound forms a substitutional solid-solution phase with Sc, in which the Sc atoms enter the Co2 sublattice exclusively. The homogeneity range of Ca₃Co_2−vSc_vO₆ (more specifically Ca₃Co1Co2_1−vSc_vO₆) extends up to v≈0.55. The crystal structure belongs to space group R3¯c with lattice parameters (in hexagonal setting): 9.0846(3)?a?9.1300(2) Å and 10.3885(4)?c?10.4677(4) Å. The magnetic moment decreases rapidly with increasing amount of the non-magnetic Sc solute in the lattice.     

Polarised IR and Raman spectra of non-centrosymmetric Na3Li(SeO4)2.6H2O crystal--a new Raman laser material

Polarised IR and Raman spectra of Na₃Li(SeO₄)₂·6H₂O single crystal have been recorded. Discussion of the results has been based on the factor group approach for the trigonal R3c (C_3v⁶) space group with Z = 2. The obtained results for the spontaneous Raman scattering have been used in the discussion of the stimulated Raman spectra of the material studied—a new Raman laser crystal.     

Thermochemical properties of the Fe-analogue of cryolite, Na3FeF6

Relative enthalpies for low-and high-temperature modifications of Na₃FeF₆ and for the Na₃FeF₆ melt have been measured by drop calorimetry in the temperature range 723–1318 K. Enthalpy of modification transition at 920 K, δ_trans H(Na₃FeF₆, 920 K) = (19 ± 3) kJ mol⁻¹ and enthalpy of fusion at the temperature of fusion 1255 K, δ_fusH(Na₃FeF₆, 1255 K) = (89 ± 3) kJ mol⁻¹ have been determined from the experimental data. Following heat capacities were obtained for the crystalline phases and for the melt, respectively: C _p(Na₃FeF₆, cr, α) = (294 ± 14) J (mol K)⁻¹, for 723 = T/K ≤ 920, C _p(Na₃FeF₆, cr, β) = (300 ± 11) J (mol K)⁻¹ for 920 ≤ T/K = 1233 and C _p(Na₃FeF₆, melt) = (275 ± 22) J (mol K)⁻¹ for 1258 ≤ T/K ≤ 1318. The obtained enthalpies indicate that melting of Na3FeF6 proceeds through a continuous series of temperature dependent equilibrium states, likely associated with the production of a solid solution.      

The PVT properties of concentrated aqueous electrolytes. IV. Changes in the compressibilities of mixing the major sea salts at 25°C

The speed of sound of mixtures of the six possible combinations of the major sea salt ions (Na⁺, Mg²⁺, Cl^–, and SO ₄ ^2– ) have been determined at I=3.0 and at 25°C. The results have been used to determine the changes in the adiabatic compressibility of mixing K_m the major sea salts. The values of K_m have been fit to the equation K_m=y₂y₃I²[k₀+k₁(1-2y₃)] where y_i is the ionic strength fraction of solute i, k₀ and k₁ are parameters related to the interactions of like-charged ions. The Young cross-square rule is obeyed to within ±0.04×10^–6 cm³-kg^–1-bar^–1. A linear correlation was found between the compressibility k₀ and volume v₀ interaction parameters (10⁴k₀=–0.24+3.999 v₀, s=0.15) in agreement with out earlier findings. Estimates of the sound speeds for the cross square mixtures (NaCl+MgSO₄ and MgCl₂+Na₂SO₄) were made using the equations of Reilly and Wood. The estimated sound speeds were found to agree on the average with the measured values to ±0.36 m-sec^–1.     

超声化学法制备不同形貌的CaF2微米晶

采用超声化学法,以CaCl2与不同氟源(NaBF4、K2SiF6)在溶液中反应,制得了不同形貌的CaF2微米晶(立方体、花状、多面体)。用XRD、SEM及TEM对产物晶相及形貌进行了表征。XRD结果显示所有产物均为结晶良好的立方相CaF2。SEM及TEM结果表明由NaBF4制得的产物形貌为均匀的立方体微米晶,而由K2SiF6制得的产物为多面体。在添加配体Na2EDTA的情况下,由NaBF4得到的产物为纳米片组成的花状结构。本文详细讨论了氟源种类、反应物比例、配体等反应参数对产物CaF2形貌的影响,并提出了可能的反应机理。     

Irreversible Antagonists for the Adenosine A2B Receptor

Blockade of the adenosine A_2B receptor (A_2BAR) represents a potential novel strategy for the immunotherapy of cancer. In the present study, we designed, synthesized, and characterized irreversible A_2BAR antagonists based on an 8-p-sulfophenylxanthine scaffold. Irreversible binding was confirmed in radioligand binding and bioluminescence resonance energy transfer(BRET)-based Gα₁₅ protein activation assays by performing ligand wash-out and kinetic experiments. p-(1-Propylxanthin-8-yl)benzene sulfonyl fluoride (6a, PSB-21500) was the most potent and selective irreversible A_2BAR antagonist of the present series with an apparent K_i value of 10.6 nM at the human A_2BAR and >38-fold selectivity versus the other AR subtypes. The corresponding 3-cyclopropyl-substituted xanthine derivative 6c (PSB-21502) was similarly potent, but was non-selective versus A₁- and A_2AARs. Attachment of a reactive sulfonyl fluoride group to an elongated xanthine 8-substituent (12, K_i 7.37 nM) resulted in a potent, selective, reversibly binding antagonist. Based on previous docking studies, the lysine residue K269^7.32 was proposed to react with the covalent antagonists. However, the mutant K269L behaved similarly to the wildtype A_2BAR, indicating that 6a and related irreversible A_2BAR antagonists do not interact with K269^7.32. The new irreversible A_2BAR antagonists will be useful tools and have the potential to be further developed as therapeutic drugs.     

Preparation of fluoroalkyl end-capped cooligomers/silica nanoparticles: A new approach to fluorinated nanoparticle inhibitors of Human Immunodeficiency Virus Type 1 and Simian Immunodeficiency Virus (SIVmac)

Fluoroalkyl end-capped acrylic acid and sulfonic acid cooligomers reacted with tetraethoxysilane (TEOS) and silica/nanoparticles under alkaline conditions to afford the corresponding cooligomers/silica nanoparticles (mean diameters: 32-173 nm) with a good dispersibility and stability in aqueous and organic media. Interestingly, fluorinated nanoparticles containing carboxy groups were found to exhibit a potent and selective anti-HIV-1 activity in vitro. In contrast, fluorinated cooligomers containing sulfo groups were shown to have a potent and selective anti-SIV_mac activity in vitro.     

The Activity Coefficients of HCl in HCl–Na2SO4 Solutions from 0 to 50°C and Ionic Strengths Up to 6 Molal

The electromotive force of HCl−Na₂SO₄ solutions has been determined from 5 to 50°C and ionic strengths from 0.5 to 6m with a Harned type cell The results have been used to determine the activity coefficient of HCl in the mixtures. The activity coefficiencts have been analyzed with the Pitzer equations to account for the ionic interactions. The measurements were used to determine interaction coefficients (β⁰, β¹) for NaHSO₄ solutions from 5 to 50°C. The model represents the mean activity coefficients HCl in the mixtures to ±0.005 over the entire temperature and concentration range of the measurements. The results have been combined with literature data to provide parameters that are valid from 0 to 250°C for NaHSO₄ solutions.     

Vibrational frequencies and force constants of N2O4 in complexes with molecules of different solvents determined by Raman spectra andAb initio calculation

The Raman spectra of N₂O₄ solutions in organic solvents have been recorded. The frequencies ofv ₁,v ₂, andv ₃ bands of N₂O₄ increase with increasing solvent electron-donor properties. Especially large changes ofv ₃ N-N stretching band have been observed (254.5 cm^–1 in n-hexane, 276.5 cm^–1 in 1,4-dioxane). The ab initio calculations have shown that the interaction between N₂O₄ and electron-donor molecules causes an increase of N-N and N-O stretching and O-N-O bending force constants of N₂O₄ in agreement with the results of Raman study.     

Low temperature preparation and uses of potent oxidizers

Because electronegativity of an oxidation state is low in an anion, salts of the high oxidation-state species [AgF₄]⁻ and [NiF₆]²⁻ can be easily made, at 0 °C, in liquid anhydrous HF (aHF) made basic with alkali fluorides. The containers are transparent fluorocarbon, and the F₂ is photo-dissociated. The [NiF₆]²⁻ salts, and the metastable binary fluorides NiF₄ and NiF₃, derived from them, are efficient fluorinating agents for the conversion of hydrido compounds to their fully fluorinated relatives. With F₂ in aHF made acidic with fluoride-ion acceptors (e.g. MF₅, M = As, Sb, Bi) attained oxidation-states are often lower (e.g. Ag^II, Au^II) because of the higher electronegativity in cations. Cationic Ag^III and Ni^IV species (derived from the anions) are sufficiently long-lived, and potent, to generate the most powerfully oxidizing hexafluorides of the second and third transition series (i.e. [MF₆], M = Pt, Ru, Rh). This synthesis is especially valuable for RhF₆, and has provided for the reinvestigation of the interaction of it with O₂. It is proposed that the unexpectedly large unit cell of O₂RhF₆ is a result of the presence of neutral O₂ and neutral RhF₆ as well as O₂⁺ and RhF₆⁻ in the lattice.     

Sorption of copper salts by a polymer based on dibenzo-18-crown-6

The Sorption of Cu(NO₃)₂ and CuCl₂ by a polymer containing immobilized dibenzo-18-crown-6 from binary and multicomponent ethanol solutions was studied. In the sorbent phase copper exists as the Cu²⁺ cations, which form a 11 complex with the macrocyclic ligand. The constant of the transfer of Cu(NO₃)₂ from the solution to the polymer was calculated.ESR spectra were obtained by V. P. Barveno.Translated fromIzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 1, pp. 67–69, January, 1995.