Generation and collision-induced dissociation of ammonium tetrafluoroborate cluster ions

Singly and doubly charged cluster ions of ammonium tetrafluoroborate (NH4BF4) with general formula [(NH4BF4)nNH4]+ and [(NH4BF4)m(NH4)2]2+, respectively, were generated by electrospray ionization (ESI) and their fragmentation examined using collision-induced dissociation (CID) and ion-trap tandem mass spectrometry. CID of [(NH4BF4)nNH4]+ caused the loss of one or more neutral NH4BF4 units. The n = 2 cluster, [(NH4BF4)2NH4]+, was unique in that it also exhibited a dissociation pathway in which HBF4 was eliminated to create [(NH4BF4)(NH3)NH4]+. Dissociation of [(NH4BF4)m(NH4)2]2+ occurred through two general pathways: (a) 'fission' to produce singly charged cluster ions and (b) elimination of one or more neutral NH4BF4 units to leave doubly charged product ions. CID profiles, and measurements of changing precursor and product ion signal intensity as a function of applied collision voltage, were collected for [(NH4BF4)nNH4]+ and compared with those for analogous [(NaBF4)nNa]+ and [(KBF4)nK]+ ions to determine the influence of the cation on the relative stability of cluster ions. In general, the [(NH4BF4)nNH4]+ clusters were found to be easier to dissociate than both the sodium and potassium clusters of comparable size, with [(KBF4)nK]+ ions the most difficult to dissociate.     

Theoretical study on tetranuclear boron clusters: B4X4 (X = H, F, Cl, Br, I)

The molecular orbitals for B4H4, B4F4, B4Cl4, B4Br4 and B4I4 have been calculated by using all-electron or effective core potential ab initio method at the self-consistent field level using basis sets with diffuse and polarization functions. The boron-boron and boron-halide (-hydrogen) distances of these cage compounds are optimized with three kinds of basis sets constrained to a tetrahedral symmetry. According to the localization scheme of Boys, four three-centered two-electron (3c2e) B-B-B bonds localized on each of the faces of the B4 tetrahedron are derived for B4X4 clusters. The HOMO-LUMO energy gaps, atomization energies and Mulliken overlap populations of these compounds indicate that the stabilities of the clusters decrease in the sequence of B4F4 > B4Cl4, B4H4 > B4Br4 > B4I4.     

Eight-vertex tetrametallic structures derived from cubanes: a close relationship between bisdisphenoidal metallaborane and organometallic clusters

The metallaborane Cp4Co4B4H4 and the organometallic cluster Cp4Fe4C4H4 (Cp = eta5-cyclopentadienyl) not only are isoelectronic but also exhibit completely analogous eight-vertex bisdisphenoidal structures. Such structures, as well as the tetracapped tetrahedral structure of the Cp4Fe4(mu3-CO)4 precursor to Cp4Fe4C4H4, can be derived from a cube by insertion of diagonals in each of the six faces. Furthermore, the formation of Cp4Fe4C4H4 from Cp4Fe4(mu3-CO)4 can be described as a double diamond-square-diamond process preserving D2d symmetry throughout the process.     

Stepwise bromination of two acetylene molecules on a butterfly-type tetrairon core and reactivity of the resulting bromoacetylene fragment toward nucleophiles

Treatment of the acetylene-coordinated tetrairon cluster, [(eta5-C5H4Me)4Fe4(HCCH)2]+, with N-bromosuccinimide led to stepwise bromination of two acetylene ligands to form [(eta5-C5H4Me)4Fe4(HCCBr)(HCCH)]+, [(eta5-C5H4Me)4Fe4(HCCBr)2]+, [(eta5-C5H4Me)4Fe4(BrCCBr)(HCCBr)]+, and [(eta5-C5H4Me)4Fe4(BrCCBr)2]+. The reactivity of the bromoacetylene fragment in [(eta5-C5H4Me)4Fe4(HCCBr)(HCCH)]+ toward water, pyridine, and ZnMe2 was also investigated.     

The conjugative metabolism of 4-methylumbelliferone and deconjugation to the parent drug examined by isolated perfused liver and in vitro liver homogenate of rats

We examined the disposition of 4-methylumbelliferone (4-MU) and its conjugative metabolites, glucuronide (4-MUG) and sulfate (4-MUS), using a single-pass rat liver perfusion system. When 4-MU was delivered, the steady-state hepatic extraction ratio for 4-MU was very high (approximately 1.0) and its conjugative metabolites, 4-MUG and 4-MUS, appeared to a large extent in the effluent perfusate. The biliary excretion rate of the 4-MUG conjugated from 4-MU was 44% of the infusion rate at the steady-state, whereas those of 4-MU and 4-MUS were less than 1% of the infusion rate. When 4-MUG was delivered, the steady-state hepatic extraction ratio for 4-MUG was very low (less than 0.05) and the removal rate of 4-MUG from the perfusate was almost identical to the excretion rate of 4-MUG into the bile, while 4-MU and 4-MUS were slightly excreted into the bile (1% of the total biliary excretion rate), suggesting that a little deconjugation of 4-MUG to 4-MU occurred in the liver. Similarly, 4-MU and 4-MUS were not detectable in the effluent perfusate. The apparent extraction ratio (Eapp) for the intracellularly conjugated 4-MUG was approximately twenty times higher than that for the pre-conjugated 4-MUG. This discrepancy between the values of Eapp for the intracellularly conjugated and pre-conjugated 4-MUG might be attributed mainly to the diffusional barrier for the metabolite between the blood and hepatocytes, as suggested in the previous simulation (J. Pharmacokin, Biopharm., 15, 399 (1987].(ABSTRACT TRUNCATED AT 250 WORDS)     

Zur Synthese sulfonierter Derivate von 4- und 5-Aminoindan

On the Synthesis of Sulfonated Derivatives of 4- and 5-Aminoindan Baking the hydrogensulfate salt of 4-aminoindan (1) and 5-aminoindan (2) led, respectively, to 4-aminoindan-7-sulfonic acid (3) and 5-aminoindan-6-sulfonic acid (4). Acid 4 was also obtained by direct sulfonation of 2. 4-Aminoindan-6-sulfonic acid (5) and 6-aminoindan-4-sulfonic acid (6) were prepared by sulfonation of 4-nitroindan (7) and 5-nitroindan (9) , respectively, to 4-nitroindan-6-sulfonic acid (8) and 6-nitroindan-4-sulfonic acid (10) , followed by a Béchamp-reduction. Treatment of 1 with amidosulfuric acid gave 3 , whereas the same reaction with 2 led to a mixture of 4 and 5-aminoindan-4-sulfonic acid (11). Independent synthesis of 11 was achieved by the following sequence of reactions: sulfur dioxide treatment of the diazonium chloride derived from 4-amino-5-nitrodan (13) gave 5-nitroindan-4-sulfonyl chloride (14) ; hydrolysis to 5-nitroindan-4-sulfonic acid (15) , and final reduction. The 4-aminoindan-5-sulfonic acid (16) was synthesized by treatment of 4-amino-7-bromoindan (18) with amidosulfuric acid to give 4-amino-7-bromoindan-5-sulfonic acid (19) followed by hydrogenolysis. Sulfonation of 4-acetyl-amino-7-bromoindan (17) with oleum followed by hydrolysis led to 7-amino-4-bromoindan-5-sulfonic acid (20) , the structure of which was confirmed by reductive dehalogenation to 5 .     

Nucleophilic substitution and ring closure reactions of 4-chloro-3-nitro-2-quinolones

4-Chloro-3-nitro-2-quinolones 3 obtained from the 4-hydroxy quinolones 1 by nitration and chlorination, reacted with sodium azide to the 4-azido derivatives 4 which cyclized on thermolysis to yield the furoxanes 5 . Nucleophilic substitution reactions of 3 led to the 4-amino-, 4-fluoro- and 4-alkoxy-3-nitroquinolones 7, 8 and 9 , respectively. With thiols either 4-thio-3-nitro- 10 or 3,4-dithioquinolones 11 were obtained depending on the basic catalyst.     

单个离子标准迁移自由能的测定

本文采用活化分析法测定参考解质Ph4AsPh4B晶体在水和有机溶剂中的溶解度和计算了它从水迁移到有机溶剂中的标准迁移Gibbs自由能△^s^wG^0t.根据Ph4AsPh4B假定,求得参考正负离子Ph4As^+和Ph4B^-的标准迁移Gibbs自由能.又通过测定Ph4AsTcO4,CsPh4B,KPh4B和CsTCO4等晶体在水和有机溶剂站的溶解度,求得TcO4^-,K^+,Cs^+等离子的标准迁移自由能,并对结果进行了讨论.     

Ring transformation of 5-acylpyrimidines into 4-acylpyrazoles with hydrazine and phenylhydrazine in acidic medium

5-Benzoyl-4-methylpyrimidines 4a,b and 5-acetyl-4-phenylpyrimidines 5a,b reacted with hydrazines in alcoholic acidic medium to give respectively 4-acetyl-3-phenylpyrazoles 7, 9 and 10 and 4-benzoyl-3-methylpyrazoles 6, 8 and 11 . In the reaction with phenylhydrazine, 5-benzoyl-4-methyl-2-methylthiopyrimidine ( 4a ) led exclusively to 4-acetyl-1,3-diphenylpyrazole ( 10 ) as 5-acetyl4-phenyl-2-methylthiopyrimidine ( 5a ) led to 4-benzoyl-3-methyl-1-phenylpyrazole ( 11 ) via the initial formation of phenylhydrazones of pyrimidines 4a and 5a . However, 5-benzoyl-4-methyl-2-phenylpyrimidine ( 4b ) and 5-acetyl-2,4-diphenylpyrimidine ( 5b ) reacted with phenylhydrazine to afford, each of them, a mixture of two isomeric pyrazoles. The mechanism of these ring contraction reactions is discussed.     

Substitution at C-4 in 3,5-disubstituted 4H-1,2,6-thiadiazin-4-ones

3,5-Diaryl-4H-1,2,6-thiadiazin-4-ones react with NaBH₄ to give the 3,5-diaryl-4H-1,2,6-thiadiazin-4-ols and with MeLi to give 4-methyl-3,5-diaryl-4H-1,2,6-thiadiazin-4-ols. The latter dehydrate with p-toluenesulfonic acid to give (3,5-diarylthiadiazin-4-ylidene)methanes. (3,5-Diphenyl-4H-1,2,6-thiadiazin-4-ylidene)methane 15 suffers mono bromination with NBS to give bromo(3,5-diphenyl-4H-1,2,6-thiadiazin-4-ylidene)methane 17. Dichloro- and dibromo(3,5-diphenyl-4H-1,2,6-thiadiazin-4-ylidene)methanes 18 and 19 are formed directly from the 3,5-diphenylthiadiazin-4-one 9 via the Appel reaction using Ph₃P and CCl₄ or CBr₄, respectively. 3,5-Diarylthiadiazin-4-ones treated with P₂S₅ give 3,5-diarylthiadiazine-4-thiones that react with tetracyanoethylene oxide to give the (thiadiazin-4-ylidene)malononitriles. Finally, the 3,5-diphenylthiadiazine-4-thione 20 reacts with ethyl diazoacetate to give ethyl 2-(3,5-diphenyl-4H-1,2,6-thiadiazin-4-ylidene)acetate 26. The above reactions show that a variety of substitutions at C-4 of 3,5-diaryl substituted 1,2,6-thiadiazin-4-ones can be achieved, which extends the potential applications of this heterocycle. All compounds are fully characterized and a brief comparison of their spectroscopic properties is given.     

Li2SO4-K2SO4-MgSO4-H2O体系及次级体系298.15K时的热化学研究

用连续滴定量热法研究Li2SO4-K2SO4-MgSO4-H2O体系及次级体系Li2SO4-K2SO40H2O、Li2SO4-MgSO4-H2O和K2SO4-MgSO4-H2O 298.15K时在离子强度为15-0.1范围内的比热容和稀释热, 并结合Debye-Huckel焓极限公式研究离子强度在15-0.0001范围内的表观摩尔焓。     

C_4O_4~(m-)(m=0,1,2,3,4)的从头算研究——1.平衡几何和相对稳定性

在RHF(基离子在UHF和ROHF)/6-31G,6-31G~*和6-31 G水平优化得到C_4O_4~(m-)(m=0,1,2,3,4)的平衡几何构型,发现从中性分子(C_4O_4)到负4价离子(C_4O_4~(4-))经历了一个由非芳香性到芳香性再到反芳香性的结构变化过程,它们的相对稳定性为C_4O_4~->C_4O_4~(2-)>C_4O_4>C_4O_4~(3-)>C_4O_4~(4-).     

Tetraphosphinite resorcinarene complexes: silver(I) capsule complexes

Resorcinarene tetraphosphinite ligands, P4, react with silver(I) trifluoroacetate or silver(I) triflate, AgX, to give the corresponding [Ag4X4(P4)] complexes. The resorcinarene skeleton in these complexes adopts a boat conformation with the silver(I) phosphinite units on the horizontal, rather than the upright, arene units of the resorcinarene. The [Ag4X4(P4)] complexes react with free P4 ligand to yield the [Ag2X2(P4)] or [AgX(P4)] complexes, which are characterized in solution by NMR spectroscopy to have a conformation opposite to that of the [Ag4X4(P4)] complexes; the silver(I) phosphinite groups are on the upright arene rings of the resorcinarene "boat" instead of the horizontal arene units. There is an easy equilibrium between these complexes. When X = triflate, the [Ag4X4(P4)] complexes disproportionate and add aqua ligands during slow crystallization to give "capsule complexes", which are characterized crystallographically as [Ag10(O3SCF3)10(OH2)6(P4)2], [Ag10(O3SCF3)6(OH2)8(P4)2][O3SCF3]4, or [Ag13(O3SCF3)13(OH2)7(P4)2] depending on the resorcinarene tetraphosphinite ligand P4 used. These unusual capsule complexes are formed by the tail-to-tail self-assembly of pairs of [Ag4(P4)]4+ units linked by additional silver ions that bind to the phenyl substituents of one resorcinarene through {Ag(eta2-C6H5)}+ binding and to the bridging triflate ligands, aqua ligands, or both of the other resorcinarene unit.     

光引发剂(4-甲苯基)(4-异丁基苯基)碘鎓六氟磷酸盐的合成研究

以对甲苯胺为原料,经重氮化、KI分解得到对-碘甲苯.在NH4Cl存在下,对-碘甲苯在过硫酸铵的氧化下与异丁苯反应,得到(4-甲苯基)(4-异丁基苯基)碘鎓氯.在丙酮溶剂中,(4-甲苯基)(4-异丁基苯基)碘鎓氯与六氟磷酸钾进行离子交换,得到目的产物(4-甲苯基)(4-异丁基苯基)碘鎓六氟磷酸盐.总收率为46.7%.通过紫外光谱、红外光谱和核磁共振测定,对产物进行了结构确证.     

Structural characterization of G-quadruplexes in deoxyguanosine clusters using ion mobility mass spectrometry

The aggregation and conformation of deoxyguanosine (dG) in an ammonium acetate buffer solution were examined using mass spectrometry, ion mobility, and molecular mechanics/dynamics calculations. The nano-ESI mass spectrum indicated that 4 and 6 dGs cluster with 1 NH4+; 11 dGs with 2 NH4+; 14, 16, and 17 dGs with 3 NH4+; and 23 dGs with 4 NH4+. The collision cross sections with helium were measured and compared with calculated cross sections of theoretical structures generated by molecular mechanics/dynamics calculations. Three distinct arrival time distribution (ATD) peaks were observed for (4dG + NH4)+. One peak was assigned to the quadruplex structure of (4dG + NH4)+, while the other two peaks corresponded to the quadruplex structures of (8dG + 2NH4)2+ and (12dG + 3NH4)3+, all with the same m/z. Four ATD peaks were observed for (6dG + NH4)+ and assigned to the globular structure of (6dG + NH4)+, and the quadruplex structures of (12dG + 2NH4)2+, (18dG + 3NH4)3+, and (24dG + 4NH4)4+. Two ATD peaks were observed for (11dG + 2NH4)2+ and assigned to the quadruplex structures of (11dG + 2NH4)2+ and (22dG + 4NH4)4+. All of the other clusters in the mass spectrum (14, 16, and 17 dGs with 3 NH4+ and 23 dGs with 4 NH4+) only had one peak in their ATDs and in all cases the theoretical structures in a quadruplex arrangement agreed with the experimental cross sections. These results provide compelling evidence that quadruplexes are present in solution and retain their structure during the spray process, dehydration, and detection.     

Density functional theory analysis of the reaction pathway for methane oxidation to acetic acid catalyzed by Pd2+ in sulfuric acid

Density functional theory has been used to investigate the thermodynamics and activation barriers associated with the direct oxidation of methane to acetic acid catalyzed by Pd2+ cation in concentrated sulfuric acid. Pd2+ cations in such solutions are ligated by two bisulfate anions and by one or two molecules of sulfuric acid. Methane oxidation is initiated by the addition of CH4 across one of the Pd-O bonds of a bisulfate ligand to form Pd(HSO4)(CH3)(H2SO4)2. The latter species will react with CO to produce Pd(HSO4)(CH3CO)(H2SO4)2. The most likely path to the final products is found to be via oxidation of Pd(HSO4)(CH3)(H2SO4)2 and Pd(HSO4)(CH3CO)(H2SO4)2 to form Pd(eta2-HSO4)(HSO4)2(CH3)(H2SO4) and Pd(eta2-HSO4)(HSO4)2(CH3CO)(H2SO4), respectively. CH3HSO4 or CH3COHSO4 is then produced by reductive elimination from the latter two species, and CH(3)COOH is then formed by hydrolysis of CH3COHSO4. The loss of Pd2+ from solution to form Pd(0) or Pd-black is predicted to occur via reduction with CO. This process is offset, though, by reoxidation of palladium by either H2SO4 or O2.     

Probing Lewis acidity of Y(BH4)3 via its reactions with MBH4 (M = Li, Na, K, NMe4)

High-energy milling of Y(BH(4))(3) (containing LiCl as a by-product, which has not been removed) with MBH(4) (M = Li, Na, K, (CH(3))(4)N) leads to the first two examples of quasi-ternary yttrium borohydrides: KY(BH(4))(4) and (CH(3))(4)NY(BH(4))(4), while no chemical reaction is observed for LiBH(4) and NaBH(4). KY(BH(4))(4) is isostructural to NaSc(BH(4))(4) (Cmcm, a = 8.5157(4) ?, b = 12.4979(6) ?, c = 9.6368(5) ?, V = 1025.62(9) ?(3), Z = 4), while (CH(3))(4)NY(BH(4))(4) crystallises in primitive orthorhombic cell, similarly to KSc(BH(4))(4) (Pnma, a = 15.0290(10) ?, b = 8.5164(6) ?, c = 12.0811(7) ?, V = 1546.29(17) ?(3), Z = 4). The thermal decomposition of hydrogen-rich KY(BH(4))(4) (8.6 wt.% H) involves the formation of an unidentified intermediate at 200 °C and recovery of KBH(4) at higher temperatures; at 410 °C, KCl and YH(2) are observed. The thermal decomposition of (CH(3))(4)NY(BH(4))(4) occurs via two partly overlapping endothermic steps with concomitant emission of H(2) and organic compounds. Heating of a NaBH(4)/Y(BH(4))(3) mixture above 165 °C results in a mixed-cation mixed-anion borohydride, NaY(BH(4))(2)Cl(2), but not NaY(BH(4))(4). The reduced reactivity of Y(BH(4))(3) towards borohydride Lewis bases when compared to hypothetical scandium borohydride can be explained by the lower Lewis acidity of Y(BH(4))(3) than Sc(BH(4))(3).     

SYNTHESIS AND CHARACTERIZATION OF SIDE CHAIN LIQUID CRYSTATALLINE POLYSILOXANES CONTAINING BENZYL ETHER LINKING UNITS

Side chain liquid crystalline polysiloxanes containing benzyl ether linkingunits were synthesized by the hydrosilylation of poly (methylhydrosiloxane) with a series of4-(4-alkoxybenzyloxy)-4'-allyloxybiphenyl monomers [4-(4-methoxybenzyloxy )-4'-allyloxy-biphenyl(M_1), 4-(4-ethoxybenzyloxy)-4'-allyloxybiphenyl (M_2), 4-(4-propoxybenzyloxy)-4'-allyloxybiphenyl (M_3), 4-(4-butoxybenzyloxy)-4'-allylox(M_4), 4-(4-pentoxy-benzyloxy)-4'-allyloxybiphenyl (M_5), 4-benzyloxy-4'-allyloxybiphenyl (M_6)]. The phasebehavior of monomeric and polymeric liquid crystals was characterized by differential scan-ning calorimetry and optical polarization microscopy where the groups are ranged frommethoxy to pentoxy Both the monomeric and polymeric liquid crystals exhibit 1iquidcrystal behaviors.     

Current Advances towards 4-Hydroxybutyrate Containing Polyhydroxyalkanoates Production for Biomedical Applications

Polyhydroxyalkanoates (PHA) are polyesters having high promise in biomedical applications. Among different types of PHA, poly-4-hydroxybutyrate (P4HB) is the only polymer that has received FDA approval for medical applications. However, most PHA producing microorganisms lack the ability to synthesize P4HB or PHA comprising 4-hydroxybutyrate (4HB) monomer due to their absence of a 4HB monomer supplying pathway. Thus, most microorganisms require supplementation of 4HB precursors to synthesize 4HB polymers. However, usage of 4HB precursors incurs additional production cost. Therefore, researchers have adopted strategies to reduce the cost, such as utilizing low-cost substrate as well as constructing 4HB monomer supplying pathways in microorganisms. We herein summarize the biomedical applications of P4HB, the natural producers of 4HB polymer, and the various strategies that have been applied in producing 4HB polymers in non-4HB producing microorganisms. It is expected that the readers would gain a vivid idea on the different strategic developments in the field of 4HB polymer production.     

Gas-phase stability of G-quadruplex DNA determined by electrospray ionization tandem mass spectrometry and molecular dynamics simulations

The relative gas-phase stabilities of seven quadruplex DNA structures, [d(TG(4)T)](4), [d(T(2)G(3)T)](4), [d(G(4)T(4)G(4))](2), [d(T(2)AG(3))(2)](2), d(T(2)AG(3))(4), d(T(2)G(4))(4), and d(G(2)T(4))(4), were investigated using molecular dynamics simulations and electrospray ionization mass spectrometry (ESI-MS). MD simulations revealed that the G-quadruplexes maintained their structures in the gas phase although the G-quartets were distorted to some degree and ammonium ions, retained by [d(TG(4)T)](4) and [d(T(2)G(3)T)](4), played a key role in stabilizing the tetrad structure. Energy-variable collisional activated dissociation was used to assess the relative stabilities of each quadruplex based on E(1/2) values, and the resulting order of relative stabilities was found to be [d(TG(4)T)](4) > d(T(2)AG(3))(4) approximately d(T(2)G(4))(4) > [d(T(2)G(3)T)](4) > [d(T(2)AG(3))(2)](2) approximately d(G(2)T(4))(4) approximately [d(G(4)T(4)G(4))](2.) The stabilities from the E(1/2) values generally paralleled the RMSD and relative free energies of the quadruplexes based on the MD energy analysis. One exception to the general agreement is [d(G(4)T(4)G(4))](2), which had the lowest E(1/2) value, but was determined to be the most stable quadruplex according to the free-energy analysis and ranked fourth based on the RMSD comparison. This discrepancy is attributed to differences in the fragmentation pathway of the quadruplex.