Reaction of vinyl chloride with group 4 metal olefin polymerization catalysts

The reactions of three types of group 4 metal olefin polymerization catalysts, (C(5)R(5))(2)ZrX(2)/activator, (C(5)Me(5))TiX(3)/MAO (MAO = methylalumoxane), and (C(5)Me(4)SiMe(2)N(t)Bu)MX(2)/activator (M = Ti, Zr), with vinyl chloride (VC) and VC/propylene mixtures have been investigated. Two general pathways are observed: (i) radical polymerization of VC initiated by radicals derived from the catalyst and (ii) net 1,2 VC insertion into L(n)MR(+) species followed by beta-Cl elimination. rac-(EBI)ZrMe(mu-Me)B(C(6)F(5))(3) (EBI = 1,2-ethylenebis(indenyl)) reacts with 2 equiv of VC to yield oligopropylene, rac-(EBI)ZrCl(2), and B(C(6)F(5))(3). This reaction proceeds by net 1,2 VC insertion into rac-(EBI)ZrMe(+) followed by fast beta-Cl elimination to yield [rac-(EBI)ZrCl][MeB(C(6)F(5))(3)] and propylene. Methylation of rac-(EBI)ZrCl(+) by MeB(C(6)F(5))(3)(-) enables a second VC insertion/beta-Cl elimination to occur. The evolved propylene is oligomerized by rac-(EBI)ZrR(+) as it is formed. At high Al/Zr ratios, rac-(EBI)ZrMe(2)/MAO catalytically converts VC to oligopropylene by 1,2 VC insertion into rac-(EBI)ZrMe(+), beta-Cl elimination, and realkylation of rac-(EBI)ZrCl(+) by MAO; this process is stoichiometric in Al-Me groups. The evolved propylene is oligomerized by rac-(EBI)ZrR(+). Oligopropylene end group analysis shows that the predominant chain transfer mechanism is VC insertion/beta-Cl elimination/realkylation. In the presence of trace levels of O(2), rac-(EBI)ZrMe(2)/MAO polymerizes VC to poly(vinyl chloride) (PVC) by a radical mechanism initiated by radicals generated by autoxidation of Zr-R and/or Al-R species. CpTiX(3)/MAO (Cp = C(5)Me(5); X = OMe, Cl) initiates radical polymerization of VC in CH(2)Cl(2) solvent at low Al/Ti ratios under anaerobic conditions; in this case, the source of initiating radicals is unknown. Radical VC polymerization can be identified by the presence of terminal and internal allylic chloride units and other "radical defects" in the PVC which arise from the characteristic chemistry of PCH(2)CHCl(*) macroradicals. However, this test must be used with caution, since the defect units can be consumed by postpolymerization reactions with MAO. (C(5)Me(4)SiMe(2)N(t)Bu)MMe(2)/[Ph(3)C]][B(C(6)F(5))(4)] catalysts (M = Ti, Zr) react with VC by net 1,2 insertion/beta-Cl elimination, yielding [(C(5)Me(4)SiMe(2)N(t)Bu)MCl][B(C(6)F(5))(4)] species which can be trapped as (C(5)Me(4)SiMe(2)N(t)Bu)MCl(2) by addition of a chloride source. The reaction of rac-(EBI)ZrMe(2)/MAO or [(C(5)Me(4)SiMe(2)N(t)Bu)ZrMe][B(C(6)F(5))(4)] with propylene/VC mixtures yields polypropylene containing both allylic and vinylidene unsaturated chain ends rather than strictly vinylidene chain ends, as observed in propylene homopolymerization. These results show that the VC insertion of L(n)M(CH(2)CHMe)(n)R(+) species is also followed by beta-Cl elimination, which terminates chain growth and precludes propylene/VC copolymerization. Termination of chain growth by beta-Cl elimination is the most significant obstacle to metal-catalyzed insertion polymerization/copolymerization of VC.     

Lewis acid-activated oxidation of alcohols by permanganate

The oxidation of alcohols by KMnO(4) is greatly accelerated by various Lewis acids. Notably the rate is increased by 4 orders of magnitude in the presence of Ca(2+). The mechanisms of the oxidation of CH(3)OH and PhCH(OH)CH(3) by MnO(4)(-) and BF(3)·MnO(4)(-) have also been studied computationally by the DFT method.     

Enantio- and diastereoselective stepwise cyclization of polyprenoids induced by chiral and achiral LBAs. A new entry to (-)-ambrox, (+)-podocarpa-8,11,13-triene diterpenoids, and (-)-tetracyclic polyprenoid of sedimentary origin

An enantio- and diastereoselective stepwise cyclization of polyprenoids induced by Lewis acid-assisted chiral Br?nsted acids (chiral LBAs) and achiral LBAs is described. In particular, the absolute stereocontrol in the initial cyclization of polyprenoids to form an A-ring induced by chiral LBAs and the importance of the nucleophilicity of the internal terminator in polyprenoids for the relative stereocontrol in subsequent cyclization are demonstrated. (-)-Ambrox was synthesized via the enantioselective cyclization of (E,E)-homofarnesyl triethylsilyl ether with tin(IV) chloride-coordinated (R)-2-(o-fluorobenzyloxy)-2'-hydroxy-1,1'-binaphthyl ((R)-BINOL-o-FBn) and subsequent diastereoselective cyclization with CF(3)CO(2)H.SnCl(4) as key steps. Protection of (E,E)-homofarnesol by a triethylsilyl group increased the enantioselectivity of chiral LBA-induced cyclization and both the chemical yield and diastereoselectivity in the subsequent cyclization. The enantioselective cyclization of homo(polyprenyl)arenes possessing an aryl group was also induced by (R)-BINOL-o-FBn.SnCl(4). Several optically active podocarpa-8,11,13-triene diterpenoids and (-)-tetracyclic polyprenoid of sedimentary origin were synthesized (75-80% ee) by the enantioselective cyclization of homo(polyprenyl)benzene derivatives induced by (R)-BINOL-o-FBn.SnCl(4) and subsequent diastereoselective cyclization induced by BF(3).Et(2)O/EtNO(2) or CF(3)CO(2)H .SnCl(4).     

Dioxomolybdenum(VI) Complexes with New Enantiomerically Pure Amino Diol Ligands

(R)-Phenylglycinol is shown to be an efficient building block for the synthesis of chiral amino diols in pure diastereomeric form by epoxide ring-opening reactions. The reaction with rac-trans-stilbene oxide gives [HOCH(2)-(R)-PhCH]NH[(S)-PhCH-(R)-PhCHOH] [2(R)-3(R)-4(S)-HNO(2)H(2)] in 32% yield, which can be methylated at nitrogen to give enantiomerically pure [HOCH(2)-(R)-PhCH]NCH(3)[(S)-PhCH-(R)-PhCHOH] [2(R)-3(R)-4(S)-MeNO(2)H(2)]. These amino diol ligands have been used to prepare chiral dioxomolybdenyl complexes of the formula N(R)-2(R)-3(R)-4(S)-(HNO(2))MoO(2) (1) and N(R)-2(R)-3(R)-4(S)-(MeNO(2))MoO(2) (2). The absolute configuration at each stereocenter in the Mo(VI) complexes has been established by (1)H NOESY spectroscopy. The configuration determined for 1 has been confirmed by an X-ray analysis. Crystal data: orthorhombic P2(1)2(1)2(1), a =7.620(3), b = 13.589(2), c = 20.339(3) ?, Z = 4, R = 0.0336. The structure consists of a polymeric chain of N(R)-2(R)-3(R)-4(S)-(HNO(2))MoO(2) molecules connected through unsymmetrical Mo=O --> Mo bridges. Each metal center is coordinated in a distorted octahedral geometry by a cis dioxo unit and by two trans alkoxo atoms. The coordination polyhedron is completed by a nitrogen atom and by a bridging oxo oxygen atom from an adjacent molecule. Compound 2 catalyzes the oxidation of PPh(3) to OPPh(3) by DMSO through a mechanism that involves the intermediacy of a Mo(IV) species.     

薄膜梯度扩散-分光光度法富集测量水中痕量Mo (VI)

建立了薄膜梯度扩散(DGT)- 硫氰酸钾(PT)分光光度法(DGT-PT法)富集测量水中痕量Mo (VI) 的分析方法。本研究先以聚季铵盐(PQAS)溶液为结合相的DGT技术 (PQAS DGT) 原位分离富集水中Mo (VI),再以PT分光光度法测定DGT结合相中Mo (VI)的含量,最后依据DGT方程计算水中Mo (VI)的浓度。DGT-PT法测得配制水中Mo ( VI) 的回收率为96.3% ~ 101.3%,相对标准偏差(RSD)为1.3% ~4.0%;测得工业废水中Mo (VI) 的浓度为27.13 ~ 121.79mg/L,加标回收率为96.0% ~ 101.6%。当采样时间为48h,PQAS DGT对水中Mo (VI) 富集近18倍,可显著降低分析方法的检测限,实现水中痕量Mo (VI) 的定量检测。     

Isotope dilution analysis in the micro and submicro range by double-labelling and precipitation on paper

A new variation of isotope dilution analysis based on double labelling and carried out on filter paper is described. The determination of microgram and submicrogram amounts of silver (labelled with (110m)Ag) by precipitation with iodide (labelled with (131)I) and of calcium (labelled with (45)Ca) by precipitation with phosphate (labelled with (32)P) are given as examples. In the first example the two radio-elements ((110m)Ag and (131)I) are measured by gamma-spectrometry, in the second one ((45)Ca and(32)P) by a beta-absorption method. A number of results show the usefulness of the method.     

Theoretical investigation of the mechanisms and stereoselectivities of reductions of acyclic phosphine oxides and sulfides by chlorosilanes

Computational studies were performed to explain the highly varied stereoselectivities obtained in the reductions of acyclic phosphine oxides and sulfides by different chlorosilanes. The reductions of phosphine oxides by HSiCl(3), HSiCl(3)/Et(3)N, and Si(2)Cl(6) and the reductions of phosphine sulfides by Si(2)Cl(6) (all in benzene) were explored by means of B3LYP, B3LYP-D, and SCS-MP2 calculations. For the reductions of phosphine oxides by HSiCl(3), the calculations support the mechanism proposed by Horner in which a hydride is transferred from silicon to phosphorus through a four-centered, frontside transition state. This mechanism leads to retention of stereochemistry at phosphorus. For the other three reductions, two classes of mechanisms were explored. Phosphorane-based mechanisms that were previously proposed by Mislow and involve SiCl(3)(-) were compared with novel alternative mechanisms that involve nonionic rearrangement processes. In one of these, donor-stabilized SiCl(2) is formed as an intermediate. The calculations support a phosphorane-based mechanism for the reductions of phosphine oxides by HSiCl(3)/Et(3)N and Si(2)Cl(6) (which proceed with inversion) but favor the rearrangement pathways for the reductions of phosphine sulfides by Si(2)Cl(6) (which proceed with retention).     

小分子配体诱导合成N,N-二苄基二硫代氨基甲酸镉(II)配合物及晶体结构

4,4'-联吡啶与二苄基二硫代氨基甲酸镉配合物[Cd(DBTC)₂]₂ (1)反应得到加合物[Cd(DBTC)₂(4,4'-bipy)] (2) (DBTC＝N,N-二苄基二硫代氨基甲酸), 通过晶体结构分析及红外光谱等研究其结构与性质. 结果表明: 引入小分子配体会破坏[Cd(DBTC)₂]₂ (1)的二聚结构, 加入吡啶则得到单核的吡啶加合物[Cd(DBTC)₂py] (3), 而引入4,4'-联吡啶后其结构变为新型的一维链状结构的配位聚合物2, 这种结构在二硫代氨基甲酸金属配合物中少见报道. 也比较了不同配体如吡啶及4,4'-联吡啶对Cd(II)及Zn(II)配合物结构的影响.     

Zur Synthese sulfonierter Derivate von 2-Fluoranilin

Syntheses of Sulfonated Derivatives of 2-Fluoroaniline Synthesis of 4-amino-3-fluorobenzenesulfonic acid ( 3 ) was achieved in two ways: reaction of 2-fluoroaniline ( 1 ) with amidosulfonic acid and by first conventionally converting 4-nitro-3-fluoroaniline ( 8 ) to 4-nitro-3-fluorobenzenesulfonyl chloride ( 9 ) followed subsequently by hydrolysis to 3-fluoro-4-nitrobenzenesulfonic acid ( 10 ) and reduction. Hydrogenolysis of 3 gave sulfanilic acid ( 7 ). Both, sulfonation of fluorobenzene ( 6 ) to 4-fluorobenzenesulfonic acid ( 11 ) followed by nitration and sulfonation of 1-fluoro-2-nitrobenzene ( 12 ) led to 4-fluoro-3-nitrobenzenesulfonic acid ( 13 ). Reduction of 13 gave the isomeric 3-amino-4-fluorobenzenesulfonic acid ( 4 ), which was also obtained both by sulfonation of 1 and by sulfonation of o-fluoroacetanilide ( 14 ) followed by hydrolysis. Selective hydrogenolyses of 2-amino-5-bromo-3-fluorobenzenesulfonic acid ( 15 ), prepared by reaction of 4-bromo-2-fluoroaniline ( 16 ) with amidosulfonic acid, and of 4-amino-2-bromo-5-fluorobenzenesulfonic acid ( 20 ), obtained by sulfonation of 5-bromo-2-fluoroaniline ( 19 ) yielded the isomers 2-amino-3-fluorobenzenesulfonic acid ( 5 ) and 3 , respectively. The fourth isomer, 3-amino-2-fluorobenzenesulfonic acid ( 2 ), was synthesized by sulfur dioxide treatment of the diazonium chloride derived from 2-fluoro-3-nitroaniline ( 21 ) to 2-fluoro-3-nitrobenzenesulfonyl chloride ( 22 ), followed by hydrolysis to 2-fluoro-3-nitrobenzenesulfonic acid ( 23 ) and final Béchamp-reduction.     

Insertion and substitution chemistry at the boron fourth position in charge-neutral zwitterionic tripodal tris(methimazolyl)borate ligands

A number of new charge-neutral zwitterionic tris(methimazolyl)borate ligands have been synthesized, either by substitution of the dimethylamine group in the adduct (dimethylamine)tris(methimazolyl)borane (1) or by insertion into its B-N(dimethylamine) bond by an unsaturated Lewis base. Two new anionic ligands, (thiocyanato)tris(methimazolyl)borate and (cyano)tris(methimazolyl)borate, have also been accessed by this method.     

Strategy for the study of paramagnetic proteins with slow electronic relaxation rates by nmr spectroscopy: application to oxidized human [2Fe-2S] ferredoxin

NMR studies of paramagnetic proteins are hampered by the rapid relaxation of nuclei near the paramagnetic center, which prevents the application of conventional methods to investigations of the most interesting regions of such molecules. This problem is particularly acute in systems with slow electronic relaxation rates. We present a strategy that can be used with a protein with slow electronic relaxation to identify and assign resonances from nuclei near the paramagnetic center. Oxidized human [2Fe-2S] ferredoxin (adrenodoxin) was used to test the approach. The strategy involves six steps: (1) NMR signals from (1)H, (13)C, and (15)N nuclei unaffected or minimally affected by paramagnetic effects are assigned by standard multinuclear two- and three-dimensional (2D and 3D) spectroscopic methods with protein samples labeled uniformly with (13)C and (15)N. (2) The very broad, hyperfine-shifted signals from carbons in the residues that ligate the metal center are classified by amino acid and atom type by selective (13)C labeling and one-dimensional (1D) (13)C NMR spectroscopy. (3) Spin systems involving carbons near the paramagnetic center that are broadened but not hyperfine-shifted are elucidated by (13)C[(13)C] constant time correlation spectroscopy (CT-COSY). (4) Signals from amide nitrogens affected by the paramagnetic center are assigned to amino acid type by selective (15)N labeling and 1D (15)N NMR spectroscopy. (5) Sequence-specific assignments of these carbon and nitrogen signals are determined by 1D (13)C[(15)N] difference decoupling experiments. (6) Signals from (1)H nuclei in these spin systems are assigned by paramagnetic-optimized 2D and 3D (1)H[(13)C] experiments. For oxidized human ferredoxin, this strategy led to assignments (to amino acid and atom type) for 88% of the carbons in the [2Fe-2S] cluster-binding loops (residues 43-58 and 89-94). These included complete carbon spin-system assignments for eight of the 22 residues and partial assignments for each of the others. Sequence-specific assignments were determined for the backbone (15)N signals from nine of the 22 residues and ambiguous assignments for five of the others.     

Encapsulation of cationic ruthenium complexes into a chiral self-assembled cage

A chiral supramolecular assembly encapsulates the two cationic ruthenium sandwich complexes [CpRu(eta(6)-C(6)H(6))](+) and [CpRu(p-cymene)](+). The host-guest complexes K(11)[CpRu(eta(6)-C(6)H(6)) subset Ga(4)L(6)] (2) and K(11)[CpRu(p-cymene) subset Ga(4)L(6)] (3) were characterized by one- and two-dimensional NMR techniques as well as by electrospray mass spectrometry. Encapsulation of the prochiral complex [CpRu(p-cymene)](+) by the chiral host renders enantiotopic protons diastereotopic as evidenced by (1)H NMR spectroscopy.     

Cu(II) complexes with heterocyclic substituted thiosemicarbazones: the case of 5-formyluracil. Synthesis,characterization, x-ray structures,DNA interaction studies,and biological activity

Two new 5-formyluracil thiosemicarbazone (H(3)ut) derivatives, Me-H(3)ut (1) and Me(2)-H(3)ut (2), were synthesized by reacting thiosemicarbazides, mono- and dimethylated on the aminic nitrogen, with 5-formyluracil and were subsequently characterized. These ligands, treated with copper chloride and nitrate, afforded three complexes: [Cu(Me-H(3)ut)Cl(2)].H(2)O (3), [Cu(Me(2)-H(3)ut)Cl(2)].H(2)O (4), and [Cu(Me-H(3)ut)(NO(3))(OH(2))(2)]NO(3) (5). The crystal structures of these complexes have been determined by single-crystal X-ray diffraction. In 3 and 4, a similar pentacoordination is present; the copper atom is surrounded by the ligand SNO donor atoms and by two chloride ions. The structure of 5 consists of [Cu(Me-H(3)ut)(NO(3))(OH(2))(2)](+) cations and nitrate anions. The copper coordination (4 + 2) involves the SNO ligand atoms and a water oxygen in the basal plane; the apical positions are occupied by a second water oxygen and by an oxygen of a monodentate nitrate group. Two biochemical techniques, namely DNA titration in the UV-vis region and thermal denaturation, have been employed to probe the details of DNA binding of these compounds. Analysis of the results suggests that our compounds are able to interact with DNA by electrostatic and groove binding but not by intercalation. The compounds have been also tested in vitro on human leukemic cell line U937, but they are not able to inhibit significantly cell proliferation.     

Photocatalytic Oxidation of Aromatic Hydrocarbons

In acidic aqueous solutions UO(2)(2+) serves as a photocatalyst (lambda(irr) >/= 425 nm) for the oxidation of benzene by H(2)O(2). Under conditions where 50% of the excited state UO(2)(2+) is quenched by H(2)O(2) (k = 5.4 x 10(6) M(-)(1) s(-)(1)) and 50% by benzene (k = 2.9 x 10(8) M(-)(1) s(-)(1)), the quantum yield for the formation of phenol is 0.70. The yield does not change when benzene is replaced by benzene-d(6), but decreases by a factor of approximately 4 upon the change of solvent from H(2)O to D(2)O. Photocatalytic oxidation of toluene by UO(2)(2+)/H(2)O(2) produces PhCHO, PhCH(2)OH, and a mixture of cresols with a total quantum yield of 0.28 under conditions where 50% of UO(2)(2+) is quenched by H(2)O(2). The quenching of UO(2)(2+) by benzene and substituted benzenes takes place with k > 10(8) M(-)(1) s(-)(1). The system UO(2)(2+)/t-BuOOH/C(6)H(6)/hnu does not result in the oxidation of benzene, but instead yields methane and ethane.     

Reactions of octacyanomolybdate(V) and octacyanotungstate(V) with s(2) metal-ion reducing centers

The s(2) centers, Sn(II), Ge(II), and In(i) reduce Mo(V)(CN)(8)(3-) and W(V)(CN)(8)(3-) quantitatively to the corresponding octacyanomolybdate(IV) and -tungstate(iv) anions. Reductions by In(i) proceed 10(3)-10(5) times as rapidly as those by Sn(II) and Ge(II). All reactions are triggered by a single electron oxidation, yielding a much more reactive s(1) intermediate. Reductions by Sn(II) in chloride medium proceed predominantly through the SnCl(3)(-) anion. The Ge(II)-W(CN)(8)(3-) reaction is initiated by a slow unimolecular heterolysis of the Ge(II) center, yielding very nearly linear profiles when the reductant is in excess.     

Fluoride-ion acceptor properties of WSF4: synthesis, characterization, and computational study of the WSF5(-) and W2S2F9(-) anions and 19F NMR spectroscopic characterization of the W2OSF9(-) anion

The new [N(CH(3))(4)][WSF(5)] salt was synthesized by two preparative methods: (a) by reaction of WSF(4) with [N(CH(3))(4)][F] in CH(3)CN and (b) directly from WF(6) using the new sulfide-transfer reagent [N(CH(3))(4)][SSi(CH(3))(3)]. The [N(CH(3))(4)][WSF(5)] salt was characterized by Raman, IR, and (19)F NMR spectroscopy and [N(CH(3))(4)][WSF(5)]·CH(3)CN by X-ray crystallography. The reaction of WSF(4) with half an aliquot of [N(CH(3))(4)][F] yielded [N(CH(3))(4)][W(2)S(2)F(9)], which was characterized by Raman and (19)F NMR spectroscopy and by X-ray crystallography. The WSF(5)(-) and W(2)S(2)F(9)(-) anions were studied by density functional theory calculations. The novel [W(2)OSF(9)](-) anion was observed by (19)F NMR spectroscopy in a CH(3)CN solution of WOF(4) and WSF(5)(-), as well as CH(3)CN solutions of WSF(4) and WOF(5)(-).     

Synthesis,Structure, and Electrochemical Properties of Sterically Protected Molybdenum Trihydride Redox Pairs: A Paramagnetic “Stretched” Dihydrogen Complex?

Complexes [MoCp(#)(PMe(3))(2)H(3)] (Cp(#)=1,2,4-C(5)H(2)tBu(3), 2 a; C(5)HiPr(4), 2 b) have been synthesized from the corresponding compounds [MoCp(#)Cl(4)] (1 a, 1 b) and fully characterized, including by X-ray crystallography and by a neutron diffraction study for 2 a. Protonation of 2 a led to complex [Mo(1,2,4-C(5)H(2)tBu(3))(PMe(3))(2)H(4)](+) (3 a) in THF and to [Mo(1,2,4-C(5)H(2)tBu(3))(PMe(3))(2)(MeCN)H(2)](+) (4 a) in MeCN. Complex 4 b analogously derives from protonation of 2 b in MeCN, whereas the tetrahydride complex 3 b is unstable. One-electron oxidation of 2 a and 2 b by [FeCp(2)]PF(6) produces the EPR-active 17-electron complexes 2 a(+) and 2 b(+). The former is thermally more stable than the latter and could be crystallographically characterized as the PF(6) (-) salt by X-ray diffraction, providing evidence for the presence of a stretched dihydrogen ligand (H...H=1.36(6) angstroms). Controlled thermal decomposition of 2 a(+) yielded the product of H(2) elimination, the 15-electron monohydride complex [Mo(1,2,4-C(5)H(2)tBu(3))(PMe(3))(2)H]PF(6) (5 a), which was characterized by X-ray crystallography and by EPR spectroscopy at liquid He temperature. The compound establishes an equilibrium with the solvent adduct in THF. An electrochemical study by cyclic voltammetry provides further evidence for a rapid H(2) elimination process from the 17-electron complexes. In contrast to the previously investigated [MoCp*(dppe)H(3)](+) system (dppe=1,2-bis(diphenylphosphino)ethane; Cp*=pentamethylcyclopentadienyl), the decomposition of 2 a(+) by H(2) substitution with a solvent molecule appears to follow a dissociative pathway in MeCN.     

PHOTOREGULATION OF α-CHYMOTRYPSIN ACTIVITY IN ORGANIC MEDIA: EFFECTS OF BIOIMPRINTING

Abstract α-Chymotrypsin exhibits photoswitchable activities in an organic solvent after covalent modification of the protein backbone with thiophenefulgide active ester (2). The thiophenefulgide-modified α-chymotrypsin exhibits reversible photoisomerizable properties between states (3)-E and (3)-C. The modified α-chymotrypsin, where nine lysine residues are substituted by thiophenefulgide units, retains 60% of the activity of the native enzyme. The activities of thiophenefulgide-modified α-chymotrypsin toward esterification of N -acetyl-L-phenylalanine (4) by ethanol in cyclohexane are controlled by the configuration of the attached photoisomerizable component and by prior bioimprinting of the protein backbone with the reaction substrate (4). The esterification of (4) in cyclohexane using bioimprinted (3)-C is two-fold faster than in the presence of (3)-E. In the presence of a nonbioimprinted enzyme, esterification of (4) by (3)-C is five-fold faster than with (3)-E. The activity of bioimprinted (3)-E toward esterification of (4) is 4.5-fold higher than that of nonbioimprinted (3)-E. Switchable cyclic esterification of (4) is accomplished by sequential photoisomerization of the thiophenefulgide-modified α-chymotrypsin between states (3)-C and (3)-E.     

Structure and properties of ionic fullerene complex Co(+)(dppe)2·(C60˙-)·(C6H4Cl2)2: distortion of the ordered fullerene cage of C60˙- radical anions

New ionic complex {Co(+)(dppe)(2)}·(C(60)˙(-))·(C(6)H(4)Cl(2))(2) (1) was obtained by the reduction of a Co(dppe)Br(2) and C(60) mixture by TDAE in o-dichlorobenzene followed by precipitation of crystals by hexane. Optical and EPR spectra of 1 indicated the formation of C(60)˙(-) radical anions and diamagnetic Co(+)(dppe)(2) cations. The structure of 1 solved at 100(2) K involves chains of C(60)˙(-) arranged along the lattice a-axis with a center-to-center distance of 10.271 ?. The chains are separated by bulky Co(+)(dppe)(2) cations and solvent molecules. All components of 1 are well ordered allowing the distortion of the C(60)˙(-) radical anion to be analyzed. An elongation of the C(60)˙(-) sphere by 0.0254(2) was found. It is essentially smaller than those in the salts (Cp*(2)Ni(+))·(C(60)˙(-))·CS(2) and (PPN(+))(2)·(C(60)(2-)) with greater distortion of the fullerene cage. The calculation of the electronic structure of fullerene by the extended Hückel method showed slight splitting of the C(60) LUMO, due to the distortion, by three levels. Two levels are located 180 and 710 cm(-1) higher than the ground level. The averaged 6-6 and 5-6 bonds in C(60)˙(-) with lengths of 1.397(2) and 1.449(2) ? are close to those determined for the C(60)(2-) dianions in (PPN(+))(2)·(C(60)(2-)), but are slightly longer and shorter, respectively, than the length of these bonds in neutral C(60).     

Determination of chromium(III) in water by solid-phase microextraction with a polyimide-coated fiber and gas chromatography-flame photometric detection

A method for the determination of trace Cr(III) in aqueous solution by solid-phase microextraction (SPME) coupled with gas chromatography (GC)-flame photometric detection (FPD) was developed. Aqueous Cr(III) was first converted to the volatile chromium trifluoroacetylacetonate (Cr(tfa)3) by derivatization with 1,1,1-trifluoroacetylacetone (Htfa), followed by SPME extraction using a polyimide-coated silica fiber. The distribution constants (K) of derivatized cis- and trans-Cr(tfa)3 between the polyimide phase and aqueous phase were 2012 and 2214, respectively. The two Cr(tfa)3 isomers extracted can be efficiently separated by a DB-210 GC column within 9 min. Selective detection of Cr was performed by a FPD equipped with a 385-nm long-pass filter. Linearity (r> 0.99) over the concentration range 5-300 ng ml(-1) Cr was obtained and the limit of detection was 2 ng ml(-1) Cr. The relative standard deviation was 7% at 10 ng ml(-1) Cr (n = 5). Applicability of this method to water analysis was tested by analyzing the chromium content in a reference standard water sample and an industrial effluent.