Preparation of some 14C-labeled sugars by radiophotosynthesis using sugar beet whole plant

Uniformly labeled [¹⁴C]glucose, [¹⁴C]fructose, and [¹⁴C]sucrose with specific activities of several microcuries per millimole have been photosynthetically prepared using the whole sugar beet plant. Smaller amounts of high specific activity sugars have been found in the leaves while larger amounts with relatively lower specific activities have been found in the root. The specific activity of the products could be significantly increased by increasing the specific activity of the initially used radioactive carbon dioxide.     

Chain transfer in anionic polymerization. Determination of chain-transfer constants by using carbon-14-labeled chain transfer agents

A method is described in which ¹⁴C-labeled chain-transfer agents are employed to measure chain-transfer constants in anionic polymerization as low as 10^?6. Each chain-transfer step incorporates one molecule of the chain-transfer agent into the polymer so that measurement of the activity and conversion allows evaluation of the chain-transfer constant. This method is independent of the initiator concentration and efficiency, making the technique especially useful when problems with the initiator are encountered. The experimental procedure is described in detail for the case of chain transfer to toluene in the n-butyllithium-initiated polymerization of styrene, where C_RH was found to be 5 × 10^?6. A mathematical treatment is given showing the relationship between the degree of polymerization (DP _n) and chain transfer.     

Acceleration of carbon-13 spin-lattice relaxation times in amino acids by electrolytes

Measurements of the enhancement, by various electrolytes, of the spin-lattice relaxation time of carbon-13 at different locations in a number of amino acids are reported. Spin-lattice relaxation times T1 of all the carbons in amino acids generally tend to decrease with increase in the concentration of electrolytes, the largest effects often being observed for the charged carboxylate groups of the amino acids. Carboxylic carbons in amino acids are the sensitive 'acceptor' of the 13C spin-lattice relaxation accelerating effects offered by electrolytes, and the 13C spin-lattice relaxation accelerating ability of electrolytes decreases in the order Mg(ClO4)2 > MgCl2 > CaCl2 > NaCl > KCl > LiClO4 > NaOH. The mechanisms of the observed phenomena are discussed in terms of intermolecular interaction, paramagnetic impurities in electrolytes and other mechanisms; large contributions of intermolecular interactions with electrolytes are present on complex formation between amino acids and metal ions and the incoming 'unsaturation' of the primary solvation shell of cations with the increase in electrolyte concentration.     

Acceleration of carbon-13 spin-lattice relaxation times in amino acids by electrolytes

A series of amino acids and carboxylic acids were determined by 13C NMR spectroscopy.The results showed that addition of 3M MgCl2 led to the 13C NMR integral area of samples being well proportional to number of carbon atoms that produce the particular signal with reliability over 95%. Measurements of 13C spin-lattice relaxation times (T1's) are reported for a number of amino acids. T1's of all the carbons in amino acids generally tend to decrease with the increase of the concentration of electrolytes, and the presence of magnesium slats is of significant. Carboxylic carbons in amino acids are the most sensitive "acceptor" of the 13C spin-lattice relaxation accelerating effects in electrolytes, and the 13C spin-lattice relaxation accelerating ability of electrolytes is Mg(ClO4)2 ＞MgCl2 ＞CaCl2 ＞NaCl ＞KCl ＞LiClO4 ＞NaOH. In general, T1's of C1 carbons in nonpolar a-amino acids are higher than those in polar and basic a-amino acids both in aqueous and 3M MgCl2 medium. In aliphatic straight-chain amino acids, a-, a-, a-, ai- and a- amino acids, T1's of C1 carbons tend to reduce with the increase of inserted carbon numbers between amino and carboxylic groups compared with Gly. T1's can be decreased even more when amino acids are mixed in 3M MgCl2, but T1's of carbons in amino acids decrease slightly with increase of the concentration of amino acids in 3M MgCl2. The mechanisms of the observed phenomena are discussed in terms of intermolecular interaction and paramagnetic impurity in electrolytes, large contributions of intermolecular interaction which is enhanced in electrolytes concentrate on the incoming "unsaturation" of the primary solvation shell of cations with the increase of electrolytes concentration and complexes formation of amino acids with metal ions. In electrolytes, amino acids are "anchored" to cations and molecule tumbling is slowed down, molecular rigidity is increased and molecular size is "enlarged", all of these are helpful to accelerate the 13C spin-lattice relaxation. Atlast, MgCl2 is proposed as an efficient relaxation agent for analysis of amino acids and some carboxylic acids.Samples were dissolved with the aid of supersonic which has the effect of degassing, and they were degassed again with supersonic for 30 seconds right before determination. All of the 13C NMR was obtained with a Bruker DPX-300 NMR instrument, using NOE-suppressed inverse gated decoupling with a recycle delay 8.00s and a sweep width 30120.48Hz, experiment temperature is integral of the carbon with the smallest chemical shift is calibrated as 10.00. Spin-lattice relaxation times (T1's) were determined by using inversion recovery according to Bruker avance user's guide.The pulse sequence is (T-90.°-T-180°-o-90t°) n.     

Cyclic homooligomers of furanoid sugar amino acids

Cyclic homooligomers of mannose-derived furanoid sugar amino acid 1 [H-Maa(Bn(2))-OH] were synthesized by using BOP reagent in the presence of DIPEA under dilute conditions that converted the sugar amino acid monomer directly into its cyclic homooligomers 3a and 4a. The glucose-based sugar amino acid 2 [H-Gaa(Bn(2))-OH] under the same reaction conditions gave a bicyclic lactam 5a as the major product. Cyclic homooligomers of 2 were prepared by cyclizing their linear precursors 6 and 7 leading to the formation of cyclic peptides 8a and 9a, respectively. Conformational analysis by NMR and constrained MD studies revealed that all the cyclic products, 3, 4, 8, and 9, had symmetrical structures. The deprotected cyclic trimer of Maa 3b displayed a conformation in which all the C=O and the N-H bonds of the molecule point in opposite directions. In the deprotected cyclic tetramer of Maa 4b, the COs and NHs were in the plane of the ring with the former pointing to outside and the latter inside the ring. The structure of the cyclic Gaa dimer 8b displayed an unusual six-membered intramolecular hydrogen bond between NH(i)() --> C3-O(i)()(-)(1) and a syn orientation between the C2-H and CO. In this molecule, the C2-hydrogens and the COs can be seen on one side of the ring while the NHs point to the other side. Addition of the bicyclic lactam 5b resulted in the influx of Na(+) ions across the lipid bilayer leading to the dissipation of valinomycin-mediated K(+) diffusion potential.     

Preparation of tert-butoxycarbonyl derivatives of amino acids using di-tert-butyl pyrocarbonate

In order to optimize and individualize the process, the influence of conditions of the reactions on the synthesis of Boc derivatives of amino acids using di-tert-butyl pyrocarbonate on the yield of desired product has been studied.     

Preparation of tert-butoxycarbonyl derivatives of amino acids using di-tert-butyl pyrocarbonate

In order to optimize and individualize the process, the influence of conditions of the reactions on the synthesis of Boc derivatives of amino acids using di-tert-butyl pyrocarbonate on the yield of desired product has been studied.Institute of Biological and Medical Chemistry, Academy of Medical Sciences of the USSR, Moscow. NPO Biokhimreaktiv All-Union Scientific-Research Institute of Applied Biochemistry, Olaine. Translated from Khimiya Prirodnykh Soedinenii, No. 4, pp. 543–548, July–August, 1979.     

Semiquantitative determination of some amino acids using the Weisz ring oven

Summary The semiquantitative determination of the amino acids glycine,dl-alanine,-alanine,l-asparagine,dl-aspartic acid andl-glutamic acid, using theWeisz ring oven, is described. The determination is carried out by forming a spot of cupric hydroxide in the centre of a round filter paper. The spot is then partly dissolved by covering it with several drops of the solution of the amino acid to be determined. The green-blue complex formed is washed on the ring oven with water into rings, and the intensity of the rings is compared with a standard scale, prepared from solutions of known concentration of the appropriate amino acid.

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Zusammenfassung Die halbquantitative Bestimmung der Aminosäuren Glycin,dl-Alanin,-Alanin,l-Asparagin,dl-Asparaginsäure undl-Glutaminsäure nach der Ringofenmethode vonWeisz wird beschrieben.Die Bestimmung wird so ausgeführt, daß zuerst in der Mitte eines Rundfilters ein Fleck von Kupfer(II)-hydroxyd ausgefällt wird. Dieser wird dann zum Teil durch das Aufbringen der zu bestimmenden Aminosäurelösung gelöst.Die entstandene grün-bläuliche, wasserlösliche Komplexverbindung wird auf dem Ringofen mit Wasser in die Ringzone gewaschen und mit Standardringen verglichen, die in gleicher Weise aus Lösungen mit bekanntem Gehalt an betreffender Aminosäure hergestellt wurden.

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Résumé On décrit le dosage semiquantitatif d'acides aminés: le glycocolle, ladl-alanine, la-alanine, lal-asparagine, l'acide aspartiquedl et l'acide glutamiquel, au moyen du four annulaire deWeisz. On réalise le dosage en formant une tache d'hydroxyde cuivrique au centre d'un papier filtre rond. On dissout alors partiellement la tache en la recouvrant de plusieurs gouttes de la solution de l'acide aminé à doser. On lave sur le four annulaire le complexe bleu-vert formé, avec de l'eau sur les anneaux, et l'on compare l'intensité des anneaux à une échelle d'étalons, préparée à partir de solutions de concentration connue de l'acide aminé approprié.

     

Asymmetric synthesis of the carbon-14-labeled selective glucocorticoid receptor modulator using cinchona alkaloid catalyzed addition of 6-bromoindole to ethyl trifluoropyruvate

We describe in this study the asymmetric synthesis of radioisotope (RI)-labeled selective glucocorticoid receptor modulator. This synthesis is based on optimization of the cinchona alkaloid catalyzed addition of 6-bromoindole to ethyl trifluoropyruvate and Negishi coupling of zinc cyanide to the 6-bromoindole moiety. [1?C] Labeled (-)-{4-[(1-{2-[6-cyano-1-(cyclohexylmethyl)-1H-indol-3-yl]-3,3,3-trifluoro-2-hydroxypropyl}piperidin-4-yl)oxy]-3-methoxyphenyl}acetic acid (-)-1 was synthesized successfully with high enantioselectivity (>99% ee) and sufficient radiochemical purity.     

Preparation of radioactive enantiomers of amino acids using labelled racemates only

It is shown from experiments on leucine, that is possible to obtain pure enantiomer tracers of amino acids by using radioactive racemates only. The resolution takes place in a single crystallization step after mixing the active racemate with the inactive enantiomer, due to an absolute stereoselection.     

Synthesis of orthogonally protected cyclic homooligomers from sugar amino acids

Two new families of orthogonally protected cyclic homooligomers with two to four sugar units were synthesized from pyranoid sugar amino acids. Cyclic oligomers composed of amide-linked sugar amino acids (1-3) were prepared by cyclization of linear oligomers of the novel orthogonally protected pyranoid sugar amino acid 12 using a solution-phase coupling method. These orthogonally protected cyclic molecules can be selectively or fully deprotected, affording the macrocycles ready to further functionalization. The straightforward reduction of the amide bonds in the cyclic oligomers 1-3 gave the corresponding amine-linked macrocycles 4-6. This kind of amine-linked carbohydrate-based cyclic oligomer has never been reported before. These flexible molecular receptors could be studied as molecular hosts for molecular, cationic, and anionic recognition. Conformational analysis by molecular modeling (AM1) showed that all of the deprotected cyclic trimers and tetramers preferred a (4)C(1) chair conformation with oxygen atoms of the sugar ring located on the interior of the cavity and the secondary hydroxyl groups outward. In the amide-linked macrocycles, all of the amide bonds are in s-trans conformation. The estimated size of the internal cavity is about 4.5 A for the cyclic trimer and 6.9 A for the cyclic tetramer. The amine-linked macrocycles displayed similar conformational behavior with a slight decrease in internal cavity.     

Preparation and reactions of stannylated amino acids

Hydrostannations of propargylic glycine esters with the new hydrostannation catalyst [Mo(CO)3(CNtBu)3] (MoBI3) gave rise to alpha-stannylated allylic esters in good yield and with high regioselectivity. The chelate Claisen rearrangements of these esters allow the syntheses of gamma,delta-unsaturated amino acids with a vinylstannane moiety in the side chain. The amino acids obtained can be further modified by cross-coupling with various types of electrophiles.     

Synthesis and conformational studies of peptidomimetics containing furanoid sugar amino acids and a sugar diacid

Furanoid sugar amino acids (1) were synthesized and used as dipeptide isosteres to induce interesting turn structures in small linear peptides. They belong to a new variety of designed hybrid structures that carry both amino and carboxyl groups on rigid furanose sugar rings. Four such molecules, 6-amino-2,5-anhydro-6-deoxy-D-gluconic acid (3, Gaa) and its mannonic (4, Maa), idonic (5, Iaa), and a 3,4-dideoxyidonic (6, ddIaa) congeners were synthesized. The synthesis followed a novel reaction path in which an intramolecular 5-exo S(N)2 opening of the hexose-derived terminal aziridine ring in 2 by the gamma-benzyloxy oxygen with concomitant debenzylation occurred during pyridinium dichromate oxidation of the primary delta-hydroxyl group to carboxyl function, leading to the formation of furanoid sugar amino acid frameworks in a single step. Incorporation of these furanoid sugar amino acids into Leu-enkephalin replacing its Gly-Gly portion gave analogues 8-11. Detailed structural analysis of these molecules by circular dichroism (CD) and various NMR techniques in combination with constrained molecular dynamics (MD) simulations revealed that two of these analogues, 8a and 10a, have folded conformations composed of an unusual nine-membered pseudo beta-turn-like structure with a strong intramolecular H-bond between LeuNH --> sugarC3-OH. This, in turn, brings the two aromatic rings of Tyr and Phe in close proximity, a prerequisite for biological activities of opioid peptides. The analgesic activities of 8a,b determined by mouse hot-plate and tail-clip methods were similar to that of Leu-enkephalin methyl ester. The syn disposition of the beta-hydroxycarboxyl motif on the sugar rings appears to be the driving force to nucleate the observed turn structures in some of these molecules (8 and 10). Repetition of the motif on both sides of a furanose ring resulted in a novel molecular design of sugar diacid, 2,5-anhydro-D-idaric acid (7, Idac). Bidirectional elongation of the diacid moieties of 7 with identical peptide strands led to the formation of a C2-symmetric reverse-turn mimetic 12 which displayed a very ordered structure consisting of identical intramolecular H-bonds at two ends between LeuNH --> sugar-OH, the same as in 8 and 10.     

Low frequency vibrational spectra of some amino acids

Far-IR absorption and reflection spectra, as well as laser Mandelshtam–Brillouin and Raman scattering spectra of -glycine, β-alanine, -histidine, -tryptophane single crystals in the 0.2–400 cm⁻¹ range were investigated. It was revealed that the far-IR and Raman spectra of the amino acids under study contain more bands than predicted by factor-group analysis, thus indicating a possible contribution of low-energy intramolecular vibrations and overtones, as well as an emergence of forbidden vibrations. Some of the low-frequency bands have never, to our knowledge, been detected previously.