Direct mass spectrometry of polymers. XIII.. Thermal fragmentation processes in copoly-α-amino acids

The thermal fragmentation processes in L-Proline—Sarcosine and in L-Proline—L-Alanine copolymers have been investigated by direct pyrolysis—mass spectrometry. The mass spectral data show that proline—sarcosine copolymers decompose in three steps, yielding cyclic oligomers. The first step is characterized by the presence of the Sar—Sar, Sar—Pro, and Pro—Pro cyclic dimers. In the second step the formation of several series of cyclic oligomers up to nonamers—decamers can be observed, while the third step of thermal decomposition process leads to the almost exclusive formation of Pro—Pro cyclic dimer. The proline—alanine copolymers, instead, show a single-step thermal degradation process leading to the formation both of cyclic oligomers and compounds with olefin and nitrile end-groups. Our results show that the thermal decompostion of alanine units is affected by the neighboring units along the polymer chain. Sarcosine units act as thermally labile probes, causing the selective thermal cleavage of the Pro—Sar copolymer.     

Two chrome derivatives from the brown alga Zonariatournefortii

Two minor lipid components of the brown seaweed $\text{Zonaria}$$\text{tournefortii}$ were characterized as (all Z) - 5′,7′-dihydroxy-2′-nonadeca-4,7,10,13,16-pentenyl-chrome chromone ($\text{3}$) and 5′,7′-dihydroxy-2′-pentadecylchrome ($\text{4}$).     

Crystallizable elastomers by chemical modification of transtactic polydiolefins. Hydrochlorination

Solutions of crystalline, high-melting trans-1,4 polybutadiene (trans-PB), trans-1,4 mix 1,2 butadiene-piperylene copolymer (BPC, low piperylene content), and isotactic trans-1,4 piperylene (trans-PP) were partly hydrochlorinated under mild conditions with gaseous HCl. Glass transition and melting temperatures were strongly affected by the addition of HCl. Several hydrochlorinated trans-PB and -BPC were semicrystalline or amorphous elastomers, susceptible to reversible crystallization when stretched. The straininduced crystallinity was similar to that shown by trans-polybutadiene sequences, particularly in the form that is unstable in bulk at room temperature (form II). The addition of HCl to the asymmetric double bond in trans-PP occurs in a stereoselective way, according to ¹³C-NMR. under the experimental conditions of the present study the occurrence of side reactions was observed; these reactions decrease the polymer unsaturation to a lower level than that calculated by the amount of HCl added to the polymer.     

Synthesis of some 2,3-Dihydro-11bH-thiazolo[3,2-d][1,4]benzoxazepin-5-(6H)one derivatives. A new heterocyclic ring system

Condensation of (S)-penicillamine methyl or ethyl ester hydrochloride with salicylaldehyde and its C-5 derivatives, provided the diastereomeric thiazolidine derivatives 1 and 2 . The resulting amino function was acylated to afford the amides 3 and 4. Cyclization of the latter led to the 2,3-dihydro-11bH-thiazolo[3,2-d]-[1,4]benzoxazepin-5-(6H)ones 5 and 6. Conformational data for these heterocyclic compounds are discussed.     

The radical trap in atom transfer radical polymerization need not be thermodynamically stable. A study of the MoX(3)(PMe(3))(3) catalysts

The molybdenum(III) coordination complexes MoX(3)(PMe(3))(3) (X = Cl, Br, and I) are capable of controlling styrene polymerization under typical atom transfer radical polymerization (ATRP) conditions, in conjunction with 2-bromoethylbenzene (BEB) as an initiator. The process is accelerated by the presence of Al(OPr(i))(3) as a cocatalyst. Electrochemical and synthetic studies aimed at identifying the nature of the spin trap have been carried out. The cyclic voltammogram of MoX(3)(PMe(3))(3) (X = Cl, Br, I) shows partial reversibility (increasing in the order Cl < Br < I) for the one-electron oxidation wave. Addition of X(-) changes the voltammogram, indicating the formation of MoX(4)(PMe(3))(3) for X = Cl and Br. On the other hand, I(-) is more easily oxidized than the MoI(3)(PMe(3))(3) complex; thus, the putative MoI(4)(PMe(3))(3) complex is redox unstable. Electrochemical studies of MoI(3)(PMe(3))(3) in the presence of X(-) (X = Cl or Br) reveal the occurrence of facile halide-exchange processes, leading to the conclusion that the MoI(3)X(PMe(3))(3) products are also redox unstable. The oxidation of MoX(3)(PMe(3))(3) with (1)/(2)Br(2) yields MoX(3)Br(PMe(3))(3) (X = Cl, Br), whose molecular nature is confirmed by single-crystal X-ray analyses. On the other hand, the oxidation of MoI(3)(PMe(3))(3) by I(2) slowly yields a tetraiodomolybdate(III) salt of iodotrimethylphosphonium, [Me(3)PI][MoI(4)(PMe(3))(3)], as confirmed by an X-ray study. This product has no controlling ability in radical polymerization. The redox instability of MoI(3)X(PMe(3))(3) can be reconciled with its involvement as a radical trapping species in the MoI(3)(PMe(3))(3)-catalyzed ATRP, given the second-order nature of its decomposition rate.     

Angle-resolved photoelectron spectroscopy of randomly oriented 3-hydroxytetrahydrofuran enantiomers.

Circular dichroism in the angular distribution of valence photoelectrons emitted from randomly oriented 3-hydroxytetrahydrofuran enantiomers (ThS and ThR) has been observed in gas-phase experiments using circularly polarized vacuum ultraviolet (VUV) light. The measured dichroism for both ThS and ThR, acquired at the single magic angle theta=234.73 degrees and at photon energies of 22, 19, 16, and 14 eV, points to an asymmetric forward-backward scattering of the photoelectrons from their highest occupied molecular orbitals (HOMO) HOMO-1 and HOMO-2, of up to 5%, depending on the photon energy. The asymmetry reverses on exchange of either the helicity of the radiation or the configuration of Th. The photoionization dichroic D parameters of ThS and ThR have been measured and their values discussed in the light of LCAO B-spline density functional theory (DFT) predictions. While an acceptable agreement is found between the dichroic parameter measured and calculated at the highest photon energy for the HOMO and HOMO-2 orbitals of Th, a significant discrepancy is observed for the HOMO-1 state which is attributed to the floppiness of Th, in particular to the comparatively large sensitivity of the size and shape of its HOMO-1 on nuclear vibrational motion.     

Thermodynamics of transfer of non-ionic solutes between immiscible liquid phases. I. Transfer of normal alcohols fromn-octane to water at 25°C

A recently developed calorimetric method has been employed to estimate the thermodynamic functions for transfer of 1-propanol, 1-butanol, 1-pentanol, 1-hexanol and 1-heptanol from n-octane to water at 25°C. A linear correlation for G _t ^o as a function of the number of carbon atoms of the alchohol molecule has been found but for H _t ^o and S _t ^o the dependence gave well defined minima.     

Investigation on the isomerization of 2-amino-3-aziridino-1,4-naphthoquinones to benzo[g]quinoxalines

The course of the hydriodic acid-catalysed and iodide-catalysed isomerization of various 2-amino-3-substituted-aziridino-1,4-naphthoquinones (I) to 1,2,3,4,5,10-hexahydrobenzo[g]-quinoxaline-5,10-diones (III) is investigated, and steric aspects of the reaction are also considered. Only in the case of the phenylaziridino derivative (Ie) does hydriodic acid afford direct cyclization to the corresponding benzoquinoxalinedione (IIIe); in all other cases the hydriodides (V) of the cleavage products (II) are obtained, and liberation of the free bases (II) results in cyclization to the corresponding benzoquinoxalinediones (III) when the aziridine ring is monosubstituted or trans disubstituted, with retention of configuration in the latter case. In contrast, the free bases (II) obtained from cis disubstituted (I) are relatively stable and cyclize with excess iodide yielding trans disubstituted (III). Correspondingly, monosubstituted and trans disubstituted I undergo iodide-catalysed isomerization to III whereas cis disubstituted I do not react.     

Palladium(II) and platinum(II)-C(3)-substituted 2,2′-bipyridines

Reaction of Pd(OAc)₂ with HL¹ and HL² (HL¹=6-iso-propyl-2,2-bipyridine; HL²=6-neo-pentyl-2,2-bipyridine), followed by treatment with LiCl or KI, gives [PdCl(L¹)]₂, (1), [PdCl(L²)]₂ (2), and [PdI(L²)]₂ (3), respectively. The chloride bridge in complexes1 and2 is split by PPh³ to give the mononuclear species PdCl(L¹)(PPh₃) (4) and PdCl(L²)(PPh₃) (5). Spectroscopic data provide evidence for coordination of the deprotonated ligands through a nitrogen and the C₍₃₎ atom of the 6-substituted pyridine. An analogous platinum complex PtCl(L³)(SMe₂) (6) (HL³=6-tert-butyl-2,2-bipyridine) was obtained from trans-PtClMe(SMe₂)₂ and HL³. The crystal structures of compounds1 and6 have been solved by X-ray diffraction analysis.Dipartimento di Chimica, Universita di Sassari, via Vienna 2, I-07100 Sassari, Italy; Dipartimento di Chimica Strutturale e Stereochimica Inorganica, Universita di Milano, Centro CNR, I-20133 Milano, Italy; Published in Khimiya Geterotsiklicheskikh Soedinenii, No. 8, pp. 1127–1137, August, 1999.     

Posttranslational hydroxylation of human phenylalanine hydroxylase is a novel example of enzyme self-repair within the second coordination sphere of catalytic iron

Phenylalanine hydroxylase, a mononuclear non-heme iron enzyme, catalyzes the hydroxylation of phenylalanine to tyrosine in the presence of oxygen and reduced pterin cofactor. X-ray structural studies have established the coordination around the iron metal center and point to significant interactions within the second coordination sphere. One such interaction involves Tyr325 in human phenylalanine hydroxylase (hPAH), which forms a hydrogen-bonding network with an aqua ligand on iron and the pterin cofactor. The full-length tetramer (1-452) and truncated dimer (117-424) Tyr325Phe hPAH mutant enzymes showed similar kinetics, thermal stabilities, and oligomerization profiles as their corresponding wild-type proteins. The possibility of in vivo posttranslational hydroxylation that would restore the activity of hPAH was examined by mass spectrometry on the trypsin digested full-length (1-452) hPAH Tyr325Phe point mutant. The amino acid tags obtained by ESI-MS/MS confirmed the presence of a Phe325 in the peptide corresponding to the doubly charged precursor ion at m/z 916.4 (L A T I F W F T V E F G L C K), and its hydroxylated counterpart in the peptide corresponding to the m/z 924.4 (L A T I F-OH W F T V E F G L C K) byproduct ion series comprising the fragments y(5)-y(12). Furthermore, the point mutation Tyr325Ala resulted in an enzyme that was totally inactive and did not display any evidence of hydroxylation. These results demonstrate the importance of Tyr325 for proper conformation of the active site, substrate binding, and catalysis. The rescue of the Tyr325Phe mutant in hPAH via self-hydroxylation presents a novel example of oxidative repair on the molecular level.