Structure of microcin J25, a peptide inhibitor of bacterial RNA polymerase, is a lassoed tail

Microcin J25 (MccJ25) is a 21-amino acid peptide inhibitor active against the DNA-dependent RNA polymerase of Gram negative bacteria. Previously, the structure of MccJ25 was reported to be a head-to-tail circle, cyclo(-G(1)GAGHVPEYF(10)VGIGTPISFY(20)G-). On the basis of biochemical studies, mass spectrometry, and NMR, we show that this structure is incorrect, and that the peptide has an extraordinary structural fold. MccJ25 contains an internal lactam linkage between the alpha-amino group of Gly1 and the gamma-carboxyl of Glu8. The tail (Tyr9-Gly21) passes through the ring (Gly1-Glu8), with Phe19 and Tyr20 straddling each side of the ring, sterically trapping the tail in a noncovalent interaction we call a lassoed tail.     

Ladders of a magnetically active element in the structure of the novel complex boride Ti9Fe2Ru18B8: synthesis, structure, bonding, and magnetism

Polycrystalline samples and single crystals of the complex boride Ti9Fe2Ru18B8 were synthesized by arc-melting the elements and characterized by single-crystal X-ray diffraction and energy-dispersive X-ray analysis. Ti9Fe2Ru18B8 is a new substitutional variant of the Zn11Rh18B8 structure type, space group P4/mbm (No. 127), whose remarkable feature is that it contains one-dimensional chains of dumbbells of magnetically active Fe atoms, which form "ladders" along the c axis. The Fe-Fe distance within a dumbbell is 2.489(2) A, and the Fe2-Fe2 distance between two dumbbells is 2.968(1) A; in contrast, the chains are well-separated from each other by distances of at least 11.217(2) A. According to the results of tight-binding electronic structure calculations, Ru-B and Ti-Ru contacts are responsible for the structural robustness, while Fe-Fe interactions influence the magnetic behavior. According to magnetization measurements, Ti9Fe2Ru18B8 orders ferromagnetically between 10 and approximately 200 K. A model for ferromagnetism in this ladder-based structure identifies ferromagnetic coupling among neighboring spin-triplet Fe2 dimers along the c axis as the origin of the magnetic behavior.     

Synthesis and structural properties of patellamide A derivatives and their copper(II) compounds

The synthesis, characterization and copper(II) coordination chemistry of three new cyclic peptide ligands, PatJ(1) (cyclo-(Ile-Thr-(Gly)Thz-Ile-Thr-(Gly)Thz)), PatJ(2) (cyclo-(Ile-Thr-(Gly)Thz-(D)-Ile-Thr-(Gly)Thz)), and PatL (cyclo-(Ile-Ser-(Gly)Thz-Ile-Ser-(Gly)Thz)) are reported. All of these cyclic peptides and PatN (cyclo-(Ile-Ser-(Gly)Thz-Ile-Thr-(Gly)Thz)) are derivatives of patellamide A and have a [24]azacrown-8 macrocyclic structure. All four synthetic cyclic peptides have two thiazole rings but, in contrast to patellamide A, no oxazoline rings. The molecular structure of PatJ(1), determined by X-ray crystallography, has a saddle conformation with two close-to-coparallel thiazole rings, very similar to the geometry of patellamide D. The two coordination sites of PatJ(1) with thiazole-N and amide-N donors are each well preorganized for transition metal ion binding. The coordination of copper(II) was monitored by UV/Vis spectroscopy, and this reveals various (meta)stable mono- and dinuclear copper(II) complexes whose stoichiometry was confirmed by mass spectra. Two types of dinuclear copper(II) complexes, [Cu(2)(H(4)L)(OH(2))(n)](2+) (n=6, 8) and [Cu(2)(H(2)L)(OH(2))(n)] (n=4, 6; L=PatN, PatL, PatJ(1), PatJ(2)) have been identified and analyzed structurally by EPR spectroscopy and a combination of spectra simulations and molecular mechanics calculations (MM-EPR). The four structures are similar to each other and have a saddle conformation, that is, derived from the crystal structure of PatJ(1) by a twist of the two thiozole rings. The small but significant structural differences are characterized by the EPR simulations.     

A reverse turn structure induced by a D,L-alpha-aminoxy acid dimer

Our previous work revealed that two adjacent D-alpha-aminoxy acids could form two homochiral N-O turns, with the backbone folding into an extended helical structure (1.8(8)-helix). Here, we report the conformational studies of linear peptides 3-6, which contain a D,L-alpha-aminoxy acid dimer segment. The NMR and X-ray analysis of 3 showed that it folded into a loop conformation with two heterochiral N-O turns. This loop segment can be used to constrain tetrapeptides 4 and 6 to form a reverse turn structure. (1)H NMR dilution studies, DMSO-d6 addition studies, and 2D-NOESY data indicated that tetrapeptides 4 and 6 folded into reverse turn conformations featured by a head-to-tail 16-membered-ring intramolecular hydrogen bond. In contrast, tetrapeptide 5 with L-Ala instead of Gly or D-Ala as the N-terminal amino acid could not form the desired reverse turn structure for steric reasons. Quantum mechanics calculations showed that model pentamide 7, with the same substitution pattern of 4, adopted a novel reverse turn conformation featuring two heterochiral N-O turns (each of an 8-membered ring hydrogen bond), a cross-strand 16-membered ring hydrogen bond, and a 7-membered ring gamma-turn.     

Triterpene glycosides from the sea cucumber Eupentacta fraudatrix. Structure and cytotoxic action of cucumariosides A2, A7, A9, A10, an, A13 and A14, seven new minor non-sulfated tetraosides and an aglycone with an uncommon 18-hydroxy group

Seven new minor triterpene glycosides, cucumariosides A2 (1), A7 (2), A9 (3), A10 (4), A11 (5), A13 (6) and A14 (7) have been isolated from the Far Eastern sea cucumber Eupentacta fraudatrix. Structures of the glycosides were elucidated by 2D NMR spectroscopy and MS. Glycosides 1-7 belong to the group of cucumariosides A, having linear tetrasaccharide carbohydrate moieties without any sulfate group and possessing 3-O-methyl-D-xylose as a terminal monosaccharide unit. Glycosides 1, 2, 5-7 differ from each other in side chain structures in aglycone moieties, while cucumarioside A10 (4) has a 23,24,25,26,27-pentanorlanostane aglycone with 18(16)-lactone. Cucumarioside A9 (3), having an uncommon 18-hydroxy group, is the second representative of the unique metabolically active glycosides that are regarded as intermediates of glycoside biosynthesis in sea cucumbers. Cytotoxic activities of glycosides 1-7 and cucumarioside A8 (8) against mouse spleen lymphocytes and the cells of the ascite form of mouse Ehrlich carcinoma, along with hemolytic activity against mouse erythrocytes and antifungal activity were studied. Cucumariosides A2 (1), A8 (8) and A13 (6) demonstrated high hemolytic activities. Glycosides 1, 4 and 6 showed moderate cytotoxic activity. Only cucumarioside A8 (8), having an 18-oxymethylene group and a 24(25)-double bond, was very active in all the tests.     

Synthesis and characterization of a series of novel heptanuclear trigonal-prismatic polyhedra with different edge-ligands

Five novel heptanuclear trigonal-prismatic polyhedra, Na4[PrNi6(Gly)9(mu 3-OH)3(H2O)6].(ClO4)7 (1), Na2[PrNi6(Gly)8(mu 3-OH)3(mu 2-OH2)-(H2O)6].(ClO4)6.(H2O)2 (2), Na[DyNi6(Gly)7(mu 3-OH)3(mu 2-OH2)2(H2O)6].(ClO4)6.H2O (3), [SmNi6(Gly)6-(mu 3-OH)3Cl3(H2O)6].Cl3.(H2O)9 (4), and [ErNi6(Gly)6(mu 3-OH)3Cl3(H2O)6].Cl3.(H2O)9 (5), were synthesized through self-assembly and characterized by X-ray structure analysis. Complex 1 crystallizes in the trigonal P3 space group (a = b = 18.1121(2), c = 11.987(0) A, and Z = 2). Complex 2 belongs to the triclinic P1 space group (a = 16.0145(3), b = 20.58650(10), c = 20.8452(3) A, alpha = 78.0590(10), beta = 67.9200(10), gamma = 68.1540(10) degrees, and Z = 4). Complex 3 belongs to the monoclinic P2(1)/m space group (a = 14.9863(3), b = 13.533, c = 15.6171(3) A, beta = 116.8970(10) degrees, and Z = 2). Complexes 4 and 5 are isomorphous (4: trigonal, P3; a = b = 11.8661(4), c = 18.2034(10) A, Z = 2; 5: a = b = 11.9001(5), c = 18.1229(11) A, Z = 2). A Ln3+ ion is in the center of the prism formed by six nickel atoms. It coordinates to nine oxygen atoms. Its coordination polyhedron may be best described as a tricapped trigonal prism. The five complexes all have a core of [LnNi6(Gly)6-(mu 3-OH)3(H2O)6]6+ and were obtained through the edge-ligand exchange of the three mu 2-OH2 ligands of [LnNi6(Gly)6-(mu 3-OH)3(H2O)6(mu 2-OH2)3]6+ partly or wholly by glycine or Cl-. Magnetic measurements reveal that 1 and 4 exhibit antiferromagnetic interaction, while 5 exhibits a ferromagnetic interaction.     

Structure characterization of lipocyclopeptide antibiotics,aspartocins A,B & C,by ESI‐MSMS and ESI‐nozzle‐skimmer‐MSMS

Three lipocyclopeptide antibiotics, aspartocins A (1), B (2), and C (3), were obtained from the aspartocin complex by HPLC separation methodology. Their structures were elucidated using previously published chemical degradation results coupled with spectroscopic studies including ESI‐MS, ESI‐Nozzle Skimmer‐MSMS and NMR. All three aspartocin compounds share the same cyclic decapeptide core of cyclo [Dab2 (Asp1‐FA)‐Pip3‐MeAsp4‐Asp5‐Gly6‐Asp7‐Gly8‐Dab9‐Val10‐Pro11]. They differ only in the fatty acid side chain moiety (FA) corresponding to (Z)‐13‐methyltetradec‐3‐ene‐carbonyl, (+,Z)‐12‐methyltetradec‐3‐ene‐carbonyl and (Z)‐12‐methyltridec‐3‐ene‐carbonyl for aspartocins A (1), B (2), and C (3), respectively. All of the sequence ions were observed by ESI‐MSMS of the doubly charged parent ions. However, a number of the sequence ions observed were of low abundance. To fully sequence the lipocyclopeptide antibiotic structures, these low abundance sequence ions together with complementary sequence ions were confirmed by ESI‐Nozzle‐Skimmer‐MSMS of the singly charged linear peptide parent fragment ions H‐Asp5‐Gly6‐Asp7‐Gly8‐Dab9‐Val10‐Pro11‐Dab2¹⁺‐Asp1‐FA. Cyclization of the aspartocins was demonstrated to occur via the β‐amino group of Dab2 from ions of moderate intensity in the ESI‐MSMS spectra. As the fatty acid moieties do not undergo internal fragmentations under the experimental ESI mass spectral conditions used, the 14 Da mass difference between the fatty acid moieties of aspartocins A (1) and B (2) versus aspartocin C (3) was used as an internal mass tag to differentiate fragment ions containing fatty acid moieties and those not containing the fatty acid moieties. The most numerous and abundant fragment ions observed in the tandem mass spectra are due to the cleavage of the tertiary nitrogen amide of the pipecolic acid residue‐3 (16 fragment ions) and the proline residue‐11 (7 fragment ions). In addition, the neutral loss of ethanimine from α,β‐diaminobutyric acid residue 9 was observed for the parent molecular ion and for 7 fragment ions. Copyright © 2009 John Wiley & Sons, Ltd.     

Synthesis and Crystal Structure of a New Mononuclear Cobalt(Ⅲ) Complex with 2,2''-Dipyridylamine and Glycine as Ligands

A new mononuclear cobalt(Ⅲ) complex [Co(dpa)2(Gly)](ClO4)2·4H2O was synthesized by the reaction of Co2 , glycine (gly) and 2,2'-dipyridylamine (dpa) in a methanol-water solution, and its structure was characterized by IR, EA, ES-MS and X-ray structure analysis. The compound crystallizes in the monoclinic system, space group P21/n with a = 12.8795(2), b =13.2904(2), c = 19.1104(2) (A),β= 109.378(1)°, V= 3085.89(8) (A)3, Z = 4, Mr = 746.36, Dc = 1.606g/cm3,μ= 0.808 mm-1, F(000) = 1536, the final R = 0.0543 and wR = 0.1306 for 5393 independent reflections. The magnetic measurement of the compound at room temperature shows that it is diamagnetic and the cobalt ion is in low spin 3 oxidation state. ES-MS experiments show that the [Co(dpa)2(Gly)]2 cation is very stable in the methanol solution.     

Preparation of S-acetylthioglycoloyl insulins based on separation by anion-exchange high-performance liquid chromatography.

A method for the preparation of insulin derivatives having protected sulfhydryl group(s) on definite site(s) on the molecule which uses anion-exchange high performance liquid chromatography on a TSKgel DEAE-2SW column for separation is described. Porcine insulin reacts with N-succinimidyl S-acetylthioacetate to afford four species of insulin derivatives that have S-acetylthioglycoloyl group(s) at: i) Gly(A1), ii) Gly(A1) and Phe(B1), iii) Gly(A1) and Lys(B29), and iv) Gly(A1), Phe(B1) and Lys(B29) positions. An insulin derivative which has a group at the Lys(B29)-position is prepared by the S-acetylthioglycoloylation of Gly(A1), Phe(B1)-dicitraconyl insulin followed by decitraconylation. The five derivatives are readily deacetylated with hydroxylamine to yield the corresponding sulfhydryl insulin derivatives.     

Hypervalent radical formation probed by electron transfer dissociation of zwitterionic tryptophan and tryptophan‐containing dipeptides complexed with Ca2+ and 18‐crown‐6 in the gas phase

The relationship between peptide structure and electron transfer dissociation (ETD) is important for structural analysis by mass spectrometry. In the present study, the formation, structure and reactivity of the reaction intermediate in the ETD process were examined using a quadrupole ion trap mass spectrometer equipped with an electrospray ionization source. ETD product ions of zwitterionic tryptophan (Trp) and Trp‐containing dipeptides (Trp‐Gly and Gly‐Trp) were detected without reionization using non‐covalent analyte complexes with Ca²⁺ and 18‐crown‐6 (18C6). In the collision‐induced dissociation, NH₃ loss was the main dissociation pathway, and loss related to the dissociation of the carboxyl group was not observed. This indicated that Trp and its dipeptides on Ca²⁺(18C6) adopted a zwitterionic structure with an NH₃⁺ group and bonded to Ca²⁺(18C6) through the COO^? group. Hydrogen atom loss observed in the ETD spectra indicated that intermolecular electron transfer from a molecular anion to the NH₃⁺ group formed a hypervalent ammonium radical, R‐NH₃, as a reaction intermediate, which was unstable and dissociated rapidly through N–H bond cleavage. In addition, N–C_α bond cleavage forming the z₁ ion was observed in the ETD spectra of Trp‐GlyCa²⁺(18C6) and Gly‐TrpCa²⁺(18C6). This dissociation was induced by transfer of a hydrogen atom in the cluster formed via an N–H bond cleavage of the hypervalent ammonium radical and was in competition with the hydrogen atom loss. The results showed that a hypervalent radical intermediate, forming a delocalized hydrogen atom, contributes to the backbone cleavages of peptides in ETD. Copyright © 2015 John Wiley & Sons, Ltd.     

Molecular carpentry: piecing together helices and hairpins in designed peptides

The design of a peptide that contains two distinct elements of secondary structure, helix and beta-hairpin, is described. Two designed 17-residue peptides: Boc-Val-Ala-Leu-Aib-Val-Ala-Leu-Gly-Gly-Leu-Phe-Val-D-Pro-Gly-Leu-Phe-Val-OMe (I) and Boc-Leu-Aib-Val-Ala-Leu-Aib-Val-Gly-Gly-Leu-Val-Val-D-Pro-Gly-Leu-Val-Val-OMe (II) have been conformationally characterized by NMR spectroscopy. Peptides I and II contain a seven-residue helical module at the N terminus and a eight-residue beta-hairpin module at the C terminus, which are connected by a conformationally flexible Gly-Gly segment. The choice of the secondary-structure modules is based upon prior crystallographic and spectroscopic analysis of the individual modules. Analysis of 500 MHz 1H NMR data, recorded as solutions in methanol, suggests that the observed pattern of chemical shifts, 3JHN CalphaH values, temperature coefficients of the NH chemical shifts, and backbone inter-residue nuclear Overhauser effects favor helical structures for residues 1-7 and beta-hairpin structures for residues 10-17. The spectroscopic data are compatible with termination of the helical segment by formation of a Schellman motif; this restricts Gly(8) to a left-handed alpha-helical conformation. Gly(9) is the only residue with multiple conformational possibilities in phi,psi space. Possible orientations of the two secondary-structure modules are considered. This study validates the use of stereochemically rigid peptide modules as prefabricated elements in the construction of synthetic protein mimics.     

Synthesis,Crystal and Band Structures,and Optical Properties of Mercury Pnictide Halide Hg19As10Br18

A mercury pnictide halide semiconductor Hg19As10Br18(1) has been prepared by the solid-state reaction and structurally characterized by single-crystal X-ray diffraction analysis.Compound 1 crystallizes in triclinic,space group P with a = 11.262(4),b = 11.352(4),c = 12.309(5) ,α = 105.724(2),β = 105.788(4),γ = 109.0780(10)° and V = 1314.3(8) 3.The structure of 1 is composed of parallel perovskite-like layers bridged by the linearly coordinated Br atoms to form a three-dimensional framework.The optical properties were investigated in terms of the diffuse reflectance spectrum.The electronic band structure along with density of states(DOS) calculated by DFT method indicates that compound 1 is a semiconductor with an indirect band gap,and that the optical absorption is mainly originated from the charge transitions from Br-4p and As-4p to the Hg-6s states.     

Direct Synthesis of Z,Boc, Fmoc,Alloc[ddot] Derivatives of 5-Aminooxazoles Starting from Acylamino Acids and Chlorosulfonylcarbamates

A one-step synthesis of 5-oxazolecarbamates 1–11 can be easily carried out starting from N-acetylated and benzoylated aminoacids such as Gly, Ala, Leu, Phe, and chlorosulfonyl carbamates, prepared in situ by addition of alcohols on chlorosulfonyl isocyanate (CSI). The structure of the compounds was confirmed by X-Ray crystallography. A subsequent exocyclic N-alkylation gave substituted 12–18 derivatives. Carbamate cleavage gave by spontaneous reopening substituted N-acylaminoamides, in excellent yields.     

金(Ⅲ)与杯[4]乙酯合钠髣超分子化合物:[Na(C_(60)H_(80)O_(12))]~ [Au(SCN)_4]~-的合成、结构及性能

0引言杯芳烃是由酚环和亚甲基组成的环多聚体,杯芳烃奇异的环状结构和可调节的空穴特征,引起广大化学工作者的浓厚研究兴趣,不同类型的新型杯芳烃及其衍生物已相继被合成出来[1]。其中有些杯芳烃化合物在浓缩分离、催化仿生、环境保护等方面已显示出良好的应用性能[2,3];一些杯     

Carboxylate anion diminishes chloride transport through a synthetic, self-assembled transmembrane pore

Six amphiphilic heptapeptides with the structure (C18H37)2NCOCH2OCH2CO-(Gly)3-Pro-(Gly)n-(Glx)-(Gly)m-O(CH2)6CH3, in which Glx represents glutamic acid or its benzyl ester and n+m=2, have been studied. In addition, the glutamate residue in the GGGPGGE sequence was esterified by fluorescent 1-pyrenemethanol. These compounds insert into phospholipid bilayers and form anion-conducting pores. Hill plots based on carboxyfluorescein release indicate that the pores are at least dimeric. Studies that involved ion-selective electrode techniques showed that transport of chloride varied with the position of glutamate within the peptide chain and whether glutamic acid was present as the free acid or its benzyl ester. Chloride transport activity was significantly higher for the glutamate esters than for free carboxylates irrespective of the glutamate position. Activity was highest when the glutamate residue in approximately (Gly)3-Pro-(Xxx)3 approximately was closest to the C terminus of the peptide. A fluorescent pyrene residue was introduced to probe the aggregation state of the amphiphile. The selectivity of the pore for Cl(-) over K+ was maintained even when the carboxylate anion was present within it. Complexation of Cl(-) by the ionophoric peptides was confirmed by negative ion mass spectrometry. Planar bilayer voltage clamp experiments confirmed that pores with more than one conductance state may form in these dynamic, self-assembled pores.     

Preparation of acetylmercapto-3-carboxypropanoyl insulins using preparative high-performance liquid chromatography on an anion-exchange column.

A method for the preparation of insulin derivatives which have protected sulfhydryl group(s) at definite site(s) on the molecule is described. Porcine insulin reacts with S-acetylmercaptosuccinic anhydride to afford four species of insulin derivatives that have 2 (or 3)-acetylmercapto-3-carboxypropanoyl group(s) at i) Gly(A1), ii) Gly(A1) and Phe(B1), iii) Gly(A1) and Lys(B29), and iv) Gly(A1), Phe(B1) and Lys(B29) positions. The derivatives are efficiently separated in a preparative scale by anion-exchange high-performance liquid chromatography on a TSKgel DEAE-2SW column. The four derivatives are all readily deacetylated with hydroxylamine to give the corresponding sulfhydryl insulin derivatives.     

Systematic study of the transfer of amino acids across the water/l,2-dichloroethane interface facilitated by dibenzo-18-crown-6

Failitated ion transfer reactions of 20 amino acids with dibenzo-18-crown-6 (DB18C6) at the water/1,2-dichloroethane (W/DCE) interfaces supported at the tips of micro- and nano-pipets were investigated systematically using cyclic voltammetry. It was found that there were only 10 amino acids, that is, Leu, Val, lle, Phe, Trp, Met, Ala, Gly, Cys, Gln (in brief), whose protonated forms as cations can give well-defined facilitated ion transfer voltammograms within the potential window, and the reaction pathway was proven to be consistent with the transfer by interfacial complexation/dissociation (TIC/TID) mechanisms. The association constants of DB 18C6 with different amino acids in the DCE (β°), and the kinetic parameters of reaction were evaluated based on the steady-state voltammetry of micro- or nano-pipets, respectively. The experimental results demonstrated that the selectivity of complexation of protonated amino acid by DB18C6 compared with that of alkali metal cations was low, which can be attributed to the vicinal effect arising from steric hindrance introduced by their side group and the steric bulk effect by lipophilic stabilization. Moreover, the association constants and the standard rate constants for different amino acids showed good correlations with their hydrophobicity (π), except Gly and Met, which inferred that the selectivity of such heterogeneous complex reaction for different amino acids with DB18C6, was not only affected by discrimination in binding these ions to the crown ether macro-cycle, but also significantly modified by the ion transfer Gibbs energy which was closely related to the structure of the transferred ions, protonated amino acids.     

Binuclear homoleptic manganese carbonyls: Mn2(CO)x (x = 10, 9, 8, 7)

The unsaturated homoleptic manganese carbonyls Mn(2)(CO)(n)() (n = 7, 8, 9) are characterized by their equilibrium geometries, thermochemistry, and vibrational frequencies using methods from density functional theory (DFT). The computed metal-metal distances for global minima range from 3.01 A for the unbridged Mn(2)(CO)(10) with a Mn-Mn single bond to 2.14 A for a monobridged Mn(2)(CO)(7) formulated with a metal-metal quadruple bond. The global minimum for Mn(2)(CO)(9) has a four-electron bridging mu-eta(2)-CO group and a 2.96 A Mn-Mn distance suggestive of the single bond required for 18-electron configurations for both metal atoms. This structure is closely related to an experimentally realized structure for the isolated and structurally characterized stable phosphine complex [R(2)PCH(2)PR(2)](2)Mn(2)(CO)(4)(mu-eta(2)-CO). An unbridged (OC)(4)Mn-Mn(CO)(5) structure for Mn(2)(CO)(9) has only slightly (<6 kcal/mol) higher energy with a somewhat shorter metal-metal distance of 2.77 A. For Mn(2)(CO)(8) the lowest energy structure is a D(2)(d)() unbridged structure with a 2.36 A metal-metal distance suggesting the triple bond required for the favored 18-electron configuration for both metal atoms. However, the unbridged unsymmetrical (CO)(3)Mn-Mn(CO)(5) structure with a metal-metal bond distance of 2.40 A lies only 1 to 3 kcal/mol above this global minimum. The lowest energy structure of Mn(2)(CO)(7) is an unbridged C(s)() structure with a short metal-metal distance of 2.26 A. This is followed energetically by another C(s)() unbridged Mn(2)(CO)(7) structure with a somewhat longer metal-metal distance of 2.38 A.     

一维链状氢键型甘氨酸超分子化合物[(Gly)2+ (18-crown-6)2(MnCl4)2‒]的合成、 结构及介电性质

以甘氨酸(Gly)、 18-冠醚-6、 二氯化锰(MnCl₂)和盐酸为原料, 通过蒸发法获得一种新型相变一维链状氢键型甘氨酸超分子化合物[(Gly)₂⁺ (18-crown-6)₂(MnCl₄)^2?](1). 通过元素分析、 变温X射线单晶衍射和介电测试等手段对其进行了表征和解析. 实验结果表明, 该晶体属于单斜晶系, 空间群从P2₁/c(100 K)转化为C2/c(293 K). 随着温度升高, [MnCl₄]^2?呈现无序状态的共棱双四面体结构. 质子化甘氨酸分子和分子内羟基(—OH)发生动态摆动, 引起O—H…Cl型一维氢键链产生明显伸缩运动, 导致化合物1在一定温度范围内出现结构相变及介电异常.     

Syntheses, structures, and properties of high-nuclear 3d-4f clusters with amino acid as ligand: {Gd6Cu24}, {Tb6Cu26}, and {(Ln6Cu24)2Cu} (Ln = Sm, Gd)

Four novel high-nuclear 3d-4f heterometallic clusters were obtained through the self-assembly of Ln(III), Cu(II), and amino acid ligands (2-methylalanine (mAla), glycine (Gly), and L-proline (Pro), respectively). The metal skeleton of cluster 1, [Gd6Cu24(mu3-OH)30(mAla)16(ClO4)(H2O)22].(ClO4)17.(OH)2.(H2O)2(0), may be described as a huge {Gd6Cu12} octahedron connected with 12 additional Cu(II) ions. The structure of cluster 2, Na4[Tb6Cu26(mu3-OH)30(Gly)18(ClO4)(H2O)22].(ClO4)25.(H2O)42, may be described as a {Tb6Cu24} main structure connected with two [Cu(Gly)(H2O)2]+ groups. Compounds {[Ln6Cu24(mu3-OH)30(Pro)12(Ac)6(ClO4)(H2O)13]2Cu(Pro)2}.(ClO4)18.(OH)16.(H2O)55 (Ln= Sm (3), Gd (4)) are 61-nuclear clusters, which represent the largest known 3d-4f clusters so far, the structure can be described as two {Ln6Cu24} octahedral units connected by a trans-Cu(proline)2 bridge. The electrical conductivity measurements reveal that they are temperature-sensitive semiconductors. The magnetic susceptibility measurements display that compound 4 is ferromagnetic.