Cyclen based bis-macrocyclic ligands as phosphates receptors. A potentiometric and NMR study

The host-guest interaction between orthophosphate, pyrophosphate and triphosphate anions and four cyclen based bis-macrocycles ligands possessing ortho-(BOC), meta-(BMC), para-xylenyl (BPC) or 2,6-pyridinyl (BPyC) linker was investigated by potentiometric measurements and NMR spectroscopy. Each ligand gave protonated species in aqueous solution that further formed ternary complexes after binding with anions; these complexes were analyzed as a result of hydrogen bond formation and Coulombic attraction between the organic host and the inorganic guest. The equilibrium constants for all the detected species are reported and the selectivity, illustrated with species distribution diagrams, is discussed. The results unambiguously showed the importance of the distance between the two cyclen cores and underlined, especially for the triphosphate species, the contribution of the nitrogen atom of the pyridinyl spacer as a supplementary anchoring point in acidic medium.     

Synthesis of various sulfoforms of the trisaccharide beta-d-GlcpA-(1-->3)- beta-d-Galp-(1-->3)-beta-d-Galp-(1-->OMP) as probes for the study of the biosynthesis and sorting of proteoglycans

A straightforward preparation of various sulfoforms of the trisaccharide 4-methoxyphenyl O-(sodium beta-d-glucopyranosyluronate)-(1-->3)-( beta-d-galactopyranosyl)-(1-->3)-beta-d-galactopyranoside (1), namely its 6a- and 4a-monosulfate, 6b- and 4b-monosulfate and 6a,6b-disulfate derivatives, is reported for the first time. These compounds, which are partial structures of the linkage region of proteoglycans, will serve as probes for the study of the biosynthesis and sorting of these macromolecules. A key trisaccharide derivative, in which the two similar d-Gal units were differentiated at C-4,6 with 4,6-benzylidene and 4,6-di-tert-butylsilylene acetals, respectively, was used as a common intermediate. Both acetal groups showed excellent orthogonality, and allowed the preparation of all target compounds in high yield. Noteworthy is the possibility to prepare the 6a- and 6b-monosulfated and the 6a,6b-disulfated species through a one-pot regioselective procedure starting from a tetrol precursor.     

黄原胶以三价铬交联的水凝胶的脱水行为

对黄原胶／三价铬水凝胶在７０，８０和９０℃下的脱水行为进行了研究．脱水与凝胶的交联密度即参与交联反应的三价铬的含量有密切联系．突发脱水之后的过程可以用一级反应动力学描述，反应速度常数随三价铬的浓度和温度的增高而增大，活化能为３４．５ｋｃａｌ／ｍｏｌ．一价盐（ＮａＣｌ）的含量对脱水过程没有影响．     

Study of peptides containing modified lysine residues by tandem mass spectrometry: precursor ion scanning of hexanal-modified peptides

Upon hexanal-modification in the presence of NaCNBH(3), the oxidized B chain of insulin becomes mono- and further dialkylated on both the N-terminal and Lys(29) residues. A pseudo-MS(3) study was performed with a triple-quadrupole mass spectrometer on the different modified lysine-containing species to gain further insights into the characteristic fragmentation pattern. These fragmentations, in good agreement with true MS(3) measurements obtained using an ion trap mass spectrometer, highlighted characteristic monoalkylated lysine (immonium-NH(3)) and protonated modified caprolactam ions at m/z 168 and 213, respectively. In contrast, no fragment ion derived from a modified lysine residue (immonium or caprolactam) was observed when dialkylation occurs on Lys(29). However, a fragment ion corresponding to a protonated dihexylamine was observed at m/z 186. This loss, characteristic of dialkylated lysine fragmentation, was also observed upon dialkylation of N(alpha)-acetyllysine with either hexanal or pentanal. On the other hand, acetylation and malondialdehyde-modification of the N(alpha)-acetyllysine side chain led mainly to the corresponding modified (immonium-NH(3)) fragment ions at m/z 126 and 138, respectively. Finally, it was demonstrated that precursor ion scanning for both m/z 168 and 213 ions led to specific and sensitive identification of peptides containing hexanal-modified lysine residues within an unfractionated tryptic digest of hexanal-modified apomyoglobin. Thus, Lys(42), Lys(45), Lys(62), Lys(63), Lys(77), Lys(87), Lys(96), Lys(98), Lys(145) and Lys(147) were found to be modified upon reaction with hexanal.     

Pyridazines: (thiényl-2)-3 pyridazine,quelques (thiényl-2)-3 pyridazines substituées en 6 et systèmes à noyaux condensés dérivés

We describe the synthesis of 3-(2-thienyl)pyridazine and of some of its derivatives substituted on the 6 position eg., ethoxy, hydrazino and azido. Some of these compounds have lead to condensed rings systems, namely, triazolo- and tetrazolopyridazines.     

Effect of salinity on petroleum biodegradation

Summary The biodegradation of Ashtart crude oil by a mixed bacterial community (EH1) isolated from a marine sediment was investigated in varying concentration of sodium chloride (0 to 2 mol/l). Each fraction of Ashtart crude oil was biodegraded after a 30 day incubation period for a NaCl concentration equivalent to the one of seawater (0.4 mol/l). Saturates were more readily degraded than aromatics. The amount of oil degraded increased initially with increasing salt concentrations to a maximum level for 0.4 mol/l NaCl concentration. Thereafter the amount of oil degraded decreased with increasing salt concentrations. The polar fraction increased for the 0.4 to 1.4 mol/l NaCl concentration range. Asphaltenes were only slightly degraded (10%) for a NaCl concentration equivalent to the one of seawater (0.4 mol/l). NaCl concentrations seemed to affect the relative biodegradation of pristane and phytane. GC, UV fluorescence and FTIR techniques were used to study the evolution of each fraction of Ashtart crude oil.     

Theoretical and experimental reevaluation of the basicity of lambda3-phosphinine

We have investigated the basicity of phosphinine (C5H5P, phosphabenzene) in reevaluating its proton affinity (PA) and gas-phase basicity (GB) and the pK(a) value of its protonated form. As a necessary step, we have first determined its gas-phase proton affinity. Using both mass spectrometric and quantum chemical methods, we have obtained the values PA(C5H5P) = 195.8 +/- 1.0 kcal mol(-1) and GB(298)(C5H5P) = 188.1 +/- 1.0 kcal mol(-1), in good agreement with previous results. We then derived a value of pK(a)(C5H6P+) = -16.1 +/- 1.0 in aqueous solution using three different approaches: the latter markedly differs from the currently available value of -10. The reason for such a discrepancy in the pK(a) of protonated phosphinine in solution is discussed. In the theoretical determination of PAs, evaluation of the basis set superposition error (BSSE) showed that this effect is quite small, being 0.1-0.2 kcal mol(-1) for phosphinine, when a density functional theory (DFT) method in conjunction with a large basis set were used.     

The co-stacking of a planar metal complex and a novel 1,3-dithiole: The synthesis and crystal structure of [Pt(mnt)(CNMe)2]·(NC)2C2S2

The reaction of [NBu₄ⁿ]2Cu(mnt)₂] with [Pt(CNMe)₄][PF₆]₂ gives [Pt(mnt)(CNMe)₂]·(NC)₂C₂S₂CNMe, an X-ray study of which reveals co-stacking of neutral planar metal and organic molecules.     

Synthesis and Characterisation of a Thiocarbonyl containing Osmium Cluster

Reaction of CS₂ with H₂Os₃(CO)₈(MeCN)S in cyclohexane yields a product H₂Os₃(CO)₇(CS)S₂. this has been characterised by NMR and mass spectroscopy, and by X-ray analysis, and has been shown to contain a terminal thiocarbonyl ligand.     

Synthesis of Phosphaformamidines and Phosphaformamidinates

A large‐scale synthetic route to a variety of phosphaformamidines and phosphaformamidinates, a type of derivative that was not accessible by the methods previously known for preparing phosphaamidines and phosphaamidinates, is reported. Thermally stable ethyl N‐arylformimidates 1 (ArN?CH(OEt), Ar=2,4,6‐(Me)₃Ph or 2,6‐(iPr)₂Ph) readily reacted with lithium dialkyl‐ and diarylphosphanides to afford the corresponding N‐aryl phosphaformamidines in 80 and 60 % yield, respectively, whereas with lithium (aryl)(silyl)phosphanide, the N‐aryl‐N‐silylphosphaformamidine (60 % yield) was obtained. Addition of primary lithium arylphosphanides to 1 followed by addition of a stoichiometric amount of nBuLi gave rise to the respective phosphaformamidinates (70–88 % yield). Methanolysis of the products afforded the N‐aryl‐N‐hydrogenophosphaformamidines (90–95 % yield). The solid‐state structure of one of the phosphaformamidinates is also presented.