Chemical and Pharmaceutical Bulletin 31 巻, 2 号

Mutual Correlation between Nonaqueous Oxidation-Reduction Potentials and Electronic Spectra, and Its Extension to describe the Substituent Effect on Electronic Spectra by Means of Substituent Constants

In order to confirm and to extend the scope of the equation (E^oxd_1/2-E^red_1/2)=k₁^{1, 3} E^UV_ho-lu+k₂, presented previously by us, the polarographic half-wave reduction (E^red_1/2) and oxidation (E^oxd_1/2) potentials in nonaqueous media and the electronic spectra of 4, 4'-disubstituted stilbenes have been measured and analyzed by means of the equation with reasonable results. The substituent effect on E^oxd_1/2 and E^red_1/2 values has been well described by using the Hammett-type substituent constants. This result has been combined with the above equation, and thus a general equation describing the substituent effect on electronic spectra in terms of substituent constants has been derived as E^UV_ho-lu=aF+bR+c, F and R being Swain and Lupton's substituent constants. This equation has been experimentally examined using the strong longest-wavelength π-π^* bands of 4, 4'-disubstituted stibenes and azoxybenzenes. The results were quite reasonable. Finally, the description of the substituent effect on electronic spectra in terms of substituent constants is discussed on the basis of molecular orbital theory.

Studies on Iodinated Compounds. I. Improved Procedure for Preparation of Monoiodohistidine

In order to obtain highly purified monoiodohistidine (MIH) in high yield, the optimum iodinating conditions for histidine were examined by HPLC. The isolation and purificaton of MIH from the reaction mixture were attempted by liquid chromatography (LC). The yields of iodohistidines [MIH and diiodohistidine (DIH)] were found to be dependent on the amount and type of the iodinating reagents ; that is, the molar ratio of histidine to iodinating reagent (I₂) should be exactly 1 : 1 for MIH and 1 : 2 for DIH for the maximum yield. Purification of MIH was successfully carried out by LC on Dowex 50 (0.05 M 2, 6-lutidine), SEP-PAK C₁₈ cartridge (Waters Associates), and Sephadex G-10 (0.1N AcOH). The overall yield of MIH·HCl obtained by the present method was 57%, which is the highest so far reported.

Configuration at the C-23 Position of 23-Hydroxy- and 23, 25-Dihydroxycholesterols

(23R)- and (23S)-23-Hydroxy- and 23, 25-dihydroxycholesterols were synthesized via 3β-tetrahydropyranyloxycholesta-5, 25-dien-23-ol (5) from cholenic acid acetate (1). The stereochemistry at the C-23 position of related steroids is also discussed.

Studies on Heterocyclic Enaminonitriles. III. Reactions of 2-Benzamido-3-cyano-4, 5-dihydrothiophenes with Amines

The reaction of 2-benzamido-3-cyano-4, 5-dihydrothiophene (I) with cyclohexylamine gave 4-cyclohexylamino-2-phenyl-5, 6-dihydrothieno [2, 3-d] pyrimidine (IVa) in 93% yield. Similarly, I reacted with morpholine, piperidine and pyrrolidine to yield the corresponding 4-amino-2-phenyl-5, 6-dihydrothieno [2, 3-d] pyrimidines (IVb-d). In a similar manner, 2-benzamido-3-cyano-5-methyl (or 4-phenyl)-4, 5-dihydrothiophene (II or III) reacted with amines to form the 4-amino derivatives (Va-d or VIa-d) corresponding to IVa-d. On the other hand, I, II and III were converted on treatment with dimethylamine hydrochloride in pyridine to the corresponding 2-phenyl-5, 6-dihydrothieno [2, 3-d] pyrimidin-4 (3H)-ones (VII-IX). Compounds IVa-d, Va-d and VIa-d were also synthesized from 4-chloro-2-phenyl-5, 6-dihydrothieno [2, 3-d] pyrimidines and appropriate amines.

Inhibition of Prostaglandin Biosynthesis by 4-O-Methylcryptochlorophaeic Acid ; : Synthesis of Monomeric Arylcarboxylic Acids for Inhibitory Activity Testing and X-Ray Analysis of 4-O-Methylcryptochlorophaeic Acid

In order to clarify the structure-activity relationship of 4-O-methylcryptochlorophaeic acid (1), which is a lichen meta-depside and a potent inhibitor of prostaglandin (PG) biosynthesis found in our previous screening work, arylcarboxylic acids (5-8) corresponding to the monomeric moieties of 4-O-methylcryptochlorophaeic acid (1) were synthesized and tested for inhibitory effect against PG biosynthesis by an enzyme system prepared from rabbit renal medulla. They were a hundred times less active than 4-O-methylcryptochlorophaeic acid (1), indicating that the dimeric structure of the meta-depside is essential for inhibitory activity against PG biosynthesis. Kinetic studies on the mechanism of inhibition revealed that 4-O-methylcryptochlorophaeic acid (1) inhibits PG biosynthesis competitively with respect to the substrate, arachidonic acid. The three dimensional structure of 4-O-methylcryptochlorophaeic acid (1), which is expected to have a molecular structure able to fit into an active site that accommodates arachidonic acid, was determined by single crystal X-ray analysis with the direct approach. The obtained structure reveals that 4-O-methylcryptochlorophaeic acid (1) maintains a rigid conformation by forming a strong hydrogen bond between a hydroxy group and a methoxy group. Based on these findings, a new active site model of fatty acid cyclooxygenase is proposed in order to explain the inhibition by the meta-depside and acidic non-steroidal antiinflammatory drugs.

Synthetic Studies on Pseudoguaianolides. II. A Total Synthesis of (±)-Carpesiolin

A total synthesis of (±)-carpesiolin (3) is reported starting from the hydroazulenone (2), which is a key intermediate of helenanolide synthesis. For the introduction of the C₆ to C₈ functionalities, 2 was converted to the epoxy-alcohol (5). Its structure was confirmed by chemical and spectroscopic evidence. After construction of the γ-lactone ring, the tert-butyl protective group was removed from the ester (15) by acid-catalyzed thermolysis. However, this reaction was unexpectedly accompanied by concomitant 1, 3-acyl migration with inversion of the configuration at C₄ to yield the hydroxy-ester (16), whose structure was established by analysis of its proton magnetic resonance spectrum and some chemical reactions. After manipulation of the protective group to give the tetrahydropyranyl ether (18), its conversion to (±)-carpesiolin was achieved by (i) introduction of the exo-methylene group onto the lactone ring, (ii) oxidation to the cyclopentanone (24), and (iii) deprotection of the C₆ hydroxyl group.

An Efficient Synthesis of 1, 1-Disubstituted Hydrazines

1, 1-Disubstituted hydrazines were prepared from the corresponding 1, 1-disubstituted ureas by means of the Hofmann rearrangement reaction. The yields were fairly good, except from the ureas susceptible to oxidation, and thus the present method represents an additional and efficient procedure for the synthesis of 1, 1-disubstituted hydrazines.

Application of the Remote Photocyclization with a Pair System of Phthalimide and Methylthio Groups. A Photochemical Synthesis of Crown Ether Analogs

Based on the regioselective remote photocyclization of a pair system consisting of a phthalimide group and a methylthio group, a homologous series of N-substituted phthalimides (4) possessing a terminal sulfide function in the poly-ether side chain afforded, on irradiation, seven- to fifteen-membered crown ether analogs (5-7) in moderate yields.

Plant Constituents biologically Active to Insects. II. Juvabione Analogs from Abies sachalinensis MAST. (1).

(+)-Juvabione (I) and two new analogs (III and IV) were isolated, together with trans-4-hydroxycinnamic acid (XIII) and vanillin (XIV), from the wood of Abies sachalinensis MAST. (Pinaceae). The structures of III and IV were established to be cis-4-[3 (S)-hydroxy-l (R), 5-dimethylhexyl] cyclohexane-l-carboxylic acid and trans-4-[3 (S)-hydroxy-l (R), 5-dimethylhexyl] cyclohexane-l-carboxylic acid, respectively, on the basis of chemical and spectral evidence.

Medium-ring Ketone Synthesis. Intramolecular Acylation of Sulfur-stabilized Carbanions : A Model Study

Intramoleclar acylation of the sulfur-stabilized carbanions of the acyclic ester 9 and amide sulfides 11 was carried out as a model study for developing an effective method for the construction of medium-ring ketones by ring closure. Reaction of 9a-c or 11a-g with lithium diisopropylamide (LDA) proceeded smoothly and the expected keto sulfides 10a-c or 12a-g, respectively, were obtained. In the cases where R₁ and/or R₂ in 11 were normal alkyl groups, the reaction did not take place. However, these difficulties were readily overcome either by introducing a methyl group next to the carbonyl group or by converting the sulfides into the corresponding sulfoxides or sulfones. Acylation in the allyl sulfides 11b, d, f and the allyl sulfone 20b takes place at the α-position to the sulfur atom, yielding β, γ-unsaturated ketones. A reductive removal of the sulfide moiety or its conversion into other functional groups was also examined.

Medium-ring Ketone Synthesis. Synthesis of Eight- to Twelve-membered Cyclic Ketones based on the Intramolecular Cyclization of Large-membered Lactam Sulfoxides or Sulfones

An effective general method for the construction of medium-ring ketones from the corresponding ω-bromocarboxylic acids is described. When the diamide disulfide 10 was treated with NaBH₄ and NaH in 2-propanol, reductive cleavage of the sulfur-sulfur bond and concomitant intramolecular coupling of the resulting thiolate anion with the terminal bromide took place and the large-ring lactam sulfide 7, which was the key intermediate for the synthesis of medium-ring ketones, was obtained. Although lithium diisopropyl amide (LDA) treatment of 11 followed by reductive desulfurization provided cycloundecanone (13d) in only 19.5 % yield, intramolecular cyclization of the α-methylated analogues 17 with LDA proceeded smoothly and the keto sulfoxides 18 were obtained in quantitative yields. In the case of the lactam sulfones 21, tert-BuOK was effective as a base for the intramolecular cyclization, affording the keto sulfones 22 in quantitative yields. The keto sulfoxides 18 and sulfones 22 were subjected to reductive desulfurization with Al-Hg to yield medium-ring ketones 19 and 13, respectively, in high yields.

Meta Functionalization of Anilines and Phenol

Base-promoted proton abstraction from π-(N-tert-butyldimethylsilyl-N-methylaniline) chromium tricarbonyl (3) took place predominantly at the meta position and variously meta-substituted N-methylacetanilides 4 were obtained after reactions with electrophiles followed by oxidative decomplexation and N-acetylation. Application of the present method to variously N, N-disubstituted anilines 5 and phenols 7 was then examined and the corresponding meta substituted anilines 6 and phenol 9 were obtained.

Acid-catalyzed Cyclization of Chalcones derived from Various Nitrogenous Heteroaromatic Compounds. II

1-Cinnamoylisoquinoline (I) was treated with perchloric acid in ethanol to give 2, 5-dihydro-1-oxo-3-phenyl-[1H] pyrrolo [2, 1-α] isoquinolinium perchlorate (V) in the yield of 48.1%. V was derived to 1-(4-nitrobenzoyloxy)-3-phenyl-[1H] pyrrolo [2, 1-α] isoquinoline (VI) by means of the Shotten-Baumann reaction. 3-Methylquinoxalin-2-yl 4-phenyl-1, 3-butadienyl ketone (VIIa) was treated with acid to give 3-hydroxy-4-methyl-1-styrylpyrrolo [1, 2-α] quinoxalinium perchlorate (VIIIa) in quantitative yield. VIIIa was treated with diazomethane to give 3-methoxy-4, 5-dimethyl-1-styrylpyrrolo [1, 2-α] quinoxalinium perchlorate (XI). VIIIa gave a monobromide (XIIa) on treatment with bromine in carbon tetrachloride. The rate of acid-catalyzed cyclization of 3-methylquinoxalin-2-yl 4-(4-nitrophenyl)-1, 3-butadienyl ketone (VIIb) was slower than that of VIIa. Attempts to cyclize XIV intramolecularly to 2, 5-dihydro-1-phenylpyrrolizin-3 [1H]-one (XVI) were unsuccessful under various conditions.

Semisynthetic β-Lactam Antibiotics. IX. Synthesis and Antibacterial Activity of 7-[2-(2-Aminothiazol-4-yl)-2-sulfoacetamido]-cephalosporanic Acid and Its Derivatives

Novel 2-(2-aminothiazol-4-yl)-2-sulfoacetyl cephalosporins (10a-c) were synthesized by two routes : A, acylation of 7-aminocephalosporanic acid (8a) or its analogs (8b, c) with an active derivative of 2-(2-aminothiazol-4-yl)-2-sulfoacetic acid, and B, side chain sulfonation of γ-chloroacetoacetyl cephalosporins (13a, b) with SO₃-dioxane and subsequent thiazole ring formation by treatment with thiourea. The cephalosporin with 4-carbamoylpyridiniomethyl at the 3-position (10c) showed a potent antipseudomonal activity but had poor activity against other gram-negative bacteria, while the cephalosporin with 1-methyltetrazol-5-ylthiomethyl at the 3-position (10b) showed a broad spectrum but caused no inhibition of Pseudomonas aeruginosa.

Chaetoglobosins, Cytotoxic 10-(Indol-3-yl)-[13] cytochalasans from Chaetomium spp. IV. ¹³C-Nuclear Magnetic Resonance Spectra and Their Application to a Biosynthetic Study

Assignments of the ¹³C-nuclear magnetic resonance signals of eight naturally occurring chaetoglobosins were established. Incorporations of [1-¹³C]-, [2-¹³C]-, and [1, 2-¹³C₂]-acetate, [¹³C-methyl]-L-methionine, and [1-¹³C]-and [2-¹³C]-DL-tryptophan into chaetoglobosins A and C by Chaetomium globosum demonstrated that the molecules were formed from nine units of acetate/malonate, three C₁ units, and one unit of tryptophan.

Pectic Substances. I. The Major Pectin from the Fruits of Zizyphus jujuba MILLER var. inermis REHD.

The major acidic polysaccharide, named Zizyphus-pectin A, was isolated from the fruits of Zizyphus jujuba MILLER var. inermis REHD. The final preparation was homogeneous as determined by ultracentrifugal analysis, cellulose acetate and glass-fiber electrophoresis, and gel chromatography. It was composed of D-galacturonic acid, L-rhamnose, D-galactose, and L-arabinose in the molar ratio of 35 : 1 : 1 : 4, and its molecular weight was estimated to be 263000. The major part (58%) of D-galacturonic acid exists as the methyl ester. O-Acetyl groups were identified and the content amounted to 2.3%. Partial acid hydrolysis gave 2-O-(α-D-galactopyranosyluronic acid)-L-rhamnose, and di- to penta- saccharides consisting of α-1→4-linked D-galactopyranosyluronic acid units. In addition, reduction of carboxyl groups followed by methylation analysis showed that the pectin possesses a backbone chain consisting of α-1→4-linked D-galactopyranosyluronic acid residues which are interspersed with α-1→2-linked L-rhamnopyranose residues having side chains at position 4. The pectin has β-1→4-linked D-galactopyranosyl linear side chains and α-1→5-linked L-arabinofuranosyl highly branched side chains having 1→3-linked branching points.

Facile Formation of 1, 3-Disubstituted 2, 3, 5, 6-Tetrahydro-2-thioxopyrimidin-4 (1H)-ones and 2-N, 3-Disubstituted 2, 3, 5, 6-Tetrahyro-2-imino-1, 3-thiazin-4-ones from Thioureas and β-Haloacyl Halides

The reaction of 1, 3-disubstituted thioureas (1) with β-haloacyl halides (2) was carried out in 5% NaOH-CH₂Cl₂ to afford 1, 3-disubstituted 2, 3, 5, 6-tetrahydro-2-thioxopyrimidin-4 (1H)-ones (3) or 2-N, 3-disubstituted 2, 3, 5, 6-tetrahydro-2-imino-1, 3-thiazin-4-ones (4) in yields of 51-63 or 54-68%, respectively.

Studies on Transfer Ribonucleic Acids and Related Compounds. XLI. Synthesis of tRNA Fragments containing Modified Nucleosides

tRNA fragments containing modified nucleosides have been synthesized either by condensation of nucleotides containing a modified base or by modification of oligonucleotides. Ribothymidine 3'-phosphate was prepared by condensation of the silylated base with protected D-ribose followed by phosphorylation. Ribothymidine-containing trimer, T-Ψ-C, was synthesized by the phosphodiester method. A ribothymidine-containing hexamer T-U-C-A-A-A and a 2'-O-methylcytidine containing hexamer C-G-G-G-Cm-Up were synthesized by the phosphotriester method. A dihydrouridine-containing trimer D-A-G and a 7-methylguanosine-containing trimer m⁷G-U-C were obtained by modification of the trimers by reduction and methylation, respectively.

Synthesis and Structure-Activity Relationship of Spiro [isochroman-piperidine] Analogs for Inhibition of Histamine Release. III

Several 1-alkyl-4-piperidylidene analogs were synthesized and tested for inhibitory activity on the compound 48/80-induced release of histamine from mast cells. 4-(4-Isochromanylidene) (12b) and 4-(diphenylmethylene) (14) derivatives of 1-benzylpiperidine were much more active than the lead compounds, 1-benzylspiro [isochroman-piperidines] (1b and 2b).

Nucleotides. XIX. Synthesis and Properties of Poly-2-alkyladenylic Acids. II. Interactions with Poly (br⁵U) or Poly (I)

Contrary to earlier reports on the interaction between polyadenylic acid (poly (A)) and poly-5-bromouridylic acid (poly (br⁵U)), poly (A) was demonstrated to form both 1 : 1 and 1 : 2 complexes with poly (br⁵U) in 0.1 MNa⁺, pH 7.3, at 25°C by reconstructing mixing curves. Under comparable conditions, newly synthesized poly-2-methyladenylic acid (poly (m²A)) and poly-2-ethyladenylic acid (poly (e²A) formed only 1 : 1 complexes with poly (br⁵U), possibly having non Watson-Crick base pairing due to steric hindrance between the C (2)-alkyl substituents of adenine and the C (2)-carbonyl oxygen of bromouracil in polynucleotides, whereas poly-2-isopropyladenylic acid (poly (iso-pr²A)) did not interact with poly (br⁵U). On the other hand, with polyinosinic acid (poly (I)), poly (m²A) formed a 1 : 2 complex with hydrogen bonding at both N (1) and N (7) of 2-methyladenine, similar to the structure of poly (A)·2poly (I), whereas poly (e²A) formed only a 1 : 1 complex, possibly having non Watson-Crick type base pairing due to steric hindrance of a bulkier substituent which blocks pairing at the N (1) bonding site of 2-ethyladenine to hypoxanthine, and poly (iso-pr²A) again gave no complex at all. The ultraviolet (UV) and circular dichroism (CD) spectra and thermal stabilities of these duplexes and triplexes were compared under various conditions.

Studies on Ketene and Its Derivatives. CXII. Reaction of Ketene with Schiff Bases to give α-Unsubstituted β-Lactams

The reaction of ketene with Schiff bases was investigated. Heating of ketene with Schiff bases (1a-l) without solvent gave α-unsubstituted β-lactams (2a-l). The reaction of ketene with ethyl N-furfurylideneglycinate (1k) to give the β-lactam 2k was carried out at various temperatures, and it was found that the yield of 2k was not much influenced by the reaction temperature. β-Lactams (2d, f, k, l) were treated with 10% aqueous sodium hydroxide in dioxane to give the corresponding carboxylic acids (4d, f, k, l) in good yields. Compounds 4d, f, l reacted with various amines in the presence of dicyclohexylcarbodiimide (DCC) to give the corresponding amides (5a-c, 8a-d).

Hard Acid and Soft Nucleophile System. VI. A Convenient Synthesis of Alkylthiopolycyclic Aromatics with a Metal Halide and Thiol System

On treatment with a metal halide and alkanethiol system, polycyclic aromatics having various substituents such as hydroxy, alkoxy, phenoxy, acetoxy, and halogen were easily converted into alkylthiopolycyclic aromatics in high yields. The chemo and regioselectivity are described for the reaction of disubstituted naphthalenes.

Marine Natural Products. XI. An Antiinflammatory Scalarane-type Bishomosesterterpene, Foliaspongin, from the Okinawan Marine Sponge Phyllospongia foliascens (PALLAS)

On the basis of chemical and physicochemical evidence, the chemical structure of foliaspongin, an antiinflammatory active principle of the Okinawan marine sponge Phyllospongia foliascens (PALLAS), was elucidated as a new scalarane-type bishomosesterterpene (3).

The Structures of 15-Dehydro-prostaglandin B₁ Dimers

Prostaglandin Bx (PGBx), a complex mixture of closely related oligomers of Prostaglandin B₁ (PGB₁) or 15-dehydro-PGB₁ which has unique biological activities, is formed under basic conditions. For mechanistic studies of the oligomerization, two dimers of 15-dehydro-PGB₁ were prepared under mild conditions and their structures were determined by means of nuclear magnetic resonance (NMR) spectroscopic studies.

Antiulcer Activity of 5-Benzylthiazolidine-2, 4-dione Derivatives

5-Benzylthiazolidine-2, 4-dione derivatives were prepared and examined for antisecretory and antiulcer activities using pylorus-ligated rats and water-immersion stress rats. Some of these compounds, in particular, 5-(2, 4, 5-tripropoxybenzyl) thiazolidine-2, 4-dione (4) and 5-(2, 4-dimethoxybenzyl) thiazolidine-2, 4-dione (23), exhibited pronounced pharmacological activities. Structure-activity relationships are discussed.

Studies on Angiotensin-converting Enzyme Inhibitors. I. Syntheses and Angiotensin-converting Enzyme Inhibitory Activity of 2-(3-Mercaptopropionyl)-1, 2, 3, 4-tetrahydroisoquinoline-3-carboxylic Acid Derivatives

(3S)-2-[(2S)-3-Mercapto-2-methylpropionyl]-1, 2, 3, 4-tetrahydroisoquinoline-3-carboxylic acid [(3S), (2S)-6a] was prepared by the reaction of (3S)-1, 2, 3, 4-tetrahydroisoquinoline-3-carboxylic acid tert-butyl ester [(3S)-2a] or benzyl ester [(3S)-2b] with 3-benzoylthio-2-methylpropionyl chloride (3a), followed by fractional crystallization and removal of the protective group. The absolute configuration of (3S), (2S)-6a was confirmed by X-ray diffraction analysis of the thiazepino [4, 3-b] isoquinoline compound (7) derived from 6a. Resolution of 3-benzoylthio-2-methylpropionic acid (8) was completed by using optically active phenylalanine amide as a resolving agent. The other optical isomers of (3S), (2S)-6a were prepared by the reaction of (3S)- or (3R)-2b with optically active 3a. The in vitro ACE inhibitory activity of each isomer of 6a was evaluated. Among them, (3S), (2S)-6a was found to be the most potent inhibitor with an IC₅₀ value of 8.6×10^-9M. Compound (3S), (2S)-6a induced a dose-dependent inhibition of the pressor response to angiotensin I after oral administration to normotensive anesthetized rats. Moreover, (3S), (2S)-6a markedly reduced the systolic blood pressure in renal hypertensive rats (RHR) and spontaneously hypertensive rats (SHR). The in vivo ACE inhibitory activity and the hypotensive effects of (3S), (2S)-6a were comparable to those of captopril.

The Structure of Paeoniflorigenone, A New Monoterpene isolated from Paeoniae Radix

A biologically active monoterpene, paeoniflorigenone (2), was isolated from the roots of Paeonia albiflora PALLAS. The structure of 2 was elucidated by means of chemical and spectral studies and its absolute structure was determined by X-ray analysis, by the direct method.

Studies on Membrane Transport in Sensitized Rats. I. Absorption of Horseradish Peroxidase from the Intestine of Sensitized and Non-sensitized Rats

It was demonstrated by electronmicroscopy and by the determination of enzymic activity in the mesenteric perfusate that horseradish peroxidase (HRP) was absorbed from adult rat intestine. When 1200 units of HRP was infused into the intestinal lumen of normal rats, 2.8 units of the enzyme was recovered in the mesenteric perfusate collected for 90 min. On the other hand, the absorption of HRP decreased specifically in rats immunized with HRP. In an in vitro experiment using everted gut sac, the effect of intraperitoneal immunization (three times) on HRP influx was 2-to 3-fold greater than that of subcutaneous immunization (six times). Although the influx was unchanged in the rats injected subcutaneously three times, the recovery of HRP in the perfusate after the same sensitization decreased significantly compared with the control rats. These results suggest that the absorption of antigen decreases after active sensitization and that the effect of immunization on the intestinal absorption depends on the administration route of antigen.

Oxidation of Sesamol Dimer by Active Species produced in the Interaction of Peroxide and Hemoglobin

Sesamol dimer (I) was converted into the quinone (II) having an absorption maximum at 550 nm by treatment with hydrogen peroxide, linoleic acid hydroperoxide or tert-butyl hydroperoxide in the presence of hemoglobin. The order of the color-forming activity was linoleic acid hydroperoxide»hydrogen peroxide>tert-butyl hydroperoxide. Methemoglobin was much more effecive than oxyhemoglobin for coloration. Hydrogen peroxide and methemoglobin produced a complex which generated singlet oxygen and hydroxyl radical, the latter being effective for coloration of I. The reaction of linoleic acid hydroperoxide with methemoglobin produced a complex which generated peroxy free radical and then the keto acid and singlet oxygen ; the peroxy free radical was found to be the active species for oxidation of I. Sesamol dimer (I) may be useful for chromogenic assay of hydroxyl and peroxy free radicals.

Kinetic Study on Ureolysis in Rats

After the oral and intraperitoneal administration of urea-¹⁴C and sodium bicarbonate-¹⁴C to rats, the radioactivity of carbon dioxide expired in breathing air and that of urea transported into the blood were measured. Ureolysis was examined quantitatively on the basis of a compartment model analysis, where the hydrolysis and transport of substances were assumed to be first-order processes. Ureolysis in vivo was found not only in the lumen, but also in other tissues such as juxtamucosa, kidney and liver ; the former rate constant (h^-1) was 0.759 (k) and the latter 0.0122 (k'). The constant k observed in normally fed rats was 9.5-fold higher than k in fasted rats, but k' was low in both cases. The administration of nicotino-hydroxamic acid as a urease inhibitor completely depressed k, but k' was not affected. On the bases of 71.0 mg·kg^-1·h^-1 of urea excreted in urine and the rate constants obtained for transport and hydrolysis of urea, the amounts of urea hydrolyzed in the lumen and other tissues were estimated to be 4.92 and 5.04 mg·kg^-1·h^-1, respectively. Consequently, it was calculated that urea hydrolyzed in the body corresponded to 12.3% of urea synthesized in the liver.

Properties of Thiobarbituric Acid-reactive Materials obtained from Lipid Peroxide and Tissue Homogenate

In order to classify the 2-thiobarbituric acid (TBA)-reactive materials in various tissues, control and CCl₄-intoxicated rat liver homogenates as well as methyl linoleate hydroperoxide (MLHPO) and malonaldehyde were subjected to the TBA reaction under both aerobic and anaerobic conditions. The TBA reaction of malonaldehyde proceeded regardless of the absence of oxygen, while the TBA value obtained from MLHPO catalyzed by tissue under anaerobic conditions was as low as 15% of the aerobic value, and tissue homogenate, even prepared from CCl₄-intoxicated rat liver, gave practically no color development under anaerobic conditions. However, after an aerobic preincubation, MLHPO and tissue homogenate produced TBA-reactive materials which could react with TBA even under anaerobic conditions. These TBA-reactive materials are not malonaldehyde itself but seem to be some further-oxidized and more polar lipid hydroperoxide. The addition of Fe to the TBA reaction medium seems to negate the requirement for oxygen. The magnitude of the TBA value obtained anaerobically from tissue with Fe addition was similar to the TBA value obtained aerobically from tissue without Fe addition.

Studies on Heart. XXIII. Distribution of [1-¹⁴C] Acetamidino-antiarrhythmic Peptide (¹⁴C-AAP) in Mice

The distribution of [1-¹⁴C] acetamidino-antiarrhythmic peptide (¹⁴C-AAP) in mice was studied by direct counting and whole-body autoradiography. Intravenously injected ¹⁴C decreased rapidly in blood during 1 to 20 min and gradually during 20 to 180 min. At 180 min 68% of the radioactivity had appeared in the urine. At 60 min unmetabolized ¹⁴C-AAP was present in the urine. At 1 min the radioactivity was highest in the kidney, followed by the lung, liver, and myocardium in that order. Radioactivity increased in the kidney and myocardium during 1 to 6 min, while the radioactivity in the lung and liver decreased rapidly from 1 to 60 min. Autoradiograms revealed that at 6 min after injection (i.v.) the highest radioactivities were seen in the kidney, urine, heart, lung, submaxillary gland, bone and gut wall. No radioactivity was present in the brain, spinal cord, gut contents or fetus. At 20 to 60 min the radioactivity levels in the organs were much less than those seen at 6 min, except for the kidney and urine. In mice orally given ¹⁴C-AAP, the maximum plateau levels of radioactivity were found in the myocardium (0.04% of dose) and blood (2.5%) at 40 to 120 min. In serum at 60 min, ¹⁴C-AAP was still present in the original molecular form, unbound to macromolecules. Thus, ¹⁴C-AAP accumulates in the myocardium of the target organ for a short time immediately after injection (i.v.), corresponding to the period of the QTc interval prolongation by AAP. ¹⁴C-AAP does not accumulate for long in any organ except for the kidney, and is largely excreted in urine within 60 min.

Evaluation of the Strength of a Scored Oblong Tablet

In order to evaluate the resistance of an oblong tablet with a center groove to breaking into halves, various tests for measuring the tablet breaking load were performed. The results were compared with those of a shock test which was considered to simulate the impacts occurring in the processes of packaging, handling and transport. It was found that the hardness values obtained from the Monsanto hardness tester were independent of the shock test data. This may be due to the difference in mechanism of tablet fracture between the two tests. In the bending test, all the test tablets cleanly fractured into halves. However, the values of breaking load obtained from a Kiya hardness tester were, on the whole, too small to be useful for distinguishing between tablets having different strengths. Since this result seemed to be caused by the high loading rate in this test, the influence of the loading rate was examined by the use of a material testing machine. When the rate of loading was sufficiently slow, higher breaking load values were obtained and differences in mechanical strength between the different tablets were easily detected. The flexure breaking loads obtained from the tester with a spring balance were in good agreement with the corresponding shock test data. In this test, the actual loading rate may be reduced by the buffer action of the spring, resulting in both higher breaking load values and greater apparent differences in strength between the test tablets. It is thought that this instrument is suitable as a conventional device for evaluating the fracture resistance of this type of tablet.

The Rate of Elimination and Distribution Volume of Rabbit Muscle Creatine Phosphokinase

An in vivo study on the elimination of rabbit muscle creatine phosphokinase (CPK) following intravenous administration has been carried out with nine rabbits selected for low endogeneous CPK fluctuation character. A two-compartment open model is proposed for the disposition of CPK. The equation C_p=Ae^-α1+Be^-β1 was employed to fit the profile of CPK activity in the plasma. The pharmacokinetic parameters of CPK in rabbits were determined at low, medium and high dose levels, and the factors which affect the estimation of pharmacokinetic parameters are discussed. The elimination of CPK appeared to be independent of the injected dose, but the intersubject variability was significant. The pharmacokinetic parameters α and β at high injected dose (860 U/kg body weight, n=9) were estimated to be 0.432±0.274 h^-1 and 0.099±0.031 h^-1. This value for β in vivo is significantly larger than the inactivation rate constant of CPK in vitro. Hence, there must be some other mechanism involved in vivo in addition to simple inactivation in the circulation by the body temperature. The distribution volume of injected CPK in the steady state was estimated to be approximately 4.3±1.1% of body weight. The result suggests that injected CPK is distributed into a major compartment (plasma) and a minor one (assumed to be interstitium).

Thermal, Physicochemical, and Micromeritic Properties of Freeze-dried Chloramphenicol Palmitate

The size reduction of chloramphenicol palmitate to a submicron level was accomplished by the freeze-drying of a solution composed of chloramphenicol palmitate and benzene. The crystal form of the resulting powder was characterized by using X-ray diffractometry, infrared spectroscopy, and differential scanning calorimetry (DSC). The first two methods showed the powder to be polymorph B, but DSC measurements indicated that it contains a trace (or seeds) of polymorph A. This was confirmed by hot-stage microscopy. The dissolution rates and solubilities of freeze-dried powders and polymorph A were determined.

Factors Affecting the in Vitro Stability of ¹⁴C-Urea in the Urine of Rats

To assess possible factors affecting the degradative reaction of urea (ureolysis) catalyzed by urease, the in vitro stability of urea in rat urine was investigated by changing the reaction temperature and pH or amount of added urease or by masking the reaction mixture from the atmosphere. The fraction of the radioactivity spiked as ¹⁴C-urea which was decomposed to ¹⁴CO₂ in rat urine at 15 and 25°C for 24 h was only about 1.5 and 3.3%, respectively, while that at 35°C was as much as 42%. The activation energy for this reaction was estimated to be approximately 25 kcal/mol. Added urease enhanced the degradation of ¹⁴C-urea, the initial apparent rate constant was proportional to the amount of the added enzyme (0.01 to 5.0 U/ml) to yield an approximate catalytic constant of 1.7×10^-2 ml/U/h. When urease was added at 5.0 U/ml, the highest degree of ureolysis was observed at neutral to very slightly alkaline pH. Covering the surface of the reaction mixture of rat urine with a layer of liquid paraffin appeared to depress almost completely the capture of radioactivity as ¹⁴CO₂. It is, therefore, suggested that two precautions, i.e., keeping the urine isolated from the atmosphere and keeping the metabolic cage at a temperature below 25°C, should be taken in disposition experiments with urea which involve the measurement of expiratory excretion of radioactivity.

Absorption and Metabolism of γ-Oryzanol in Rats

The metabolism and lymphatic transport of γ-oryzanol in rats were investigated following oral administration of the ¹⁴C-labeled compound (triterpenyl esters of ferulic acid-3-¹⁴C). Redioactivity excreted in the urine during 72 h after oral administration was 9.8% of the dose (50 mg/kg). Unchanged γ-oryzanol was not detected at all in the urine, but an in situ intestinal absorption experiment suggested that more than 80% of the absorbed radioactivity was transferred into the mesenteric vein as an intact form, though a part was metabolized in the small intestine during absorption. Ferulic acid, dihydroferulic acid, m-hydroxyphenylpropionic acid, m-coumaric acid, m-hydroxyhippuric acid and hippuric acid were identified as the major urinary metabolites. These metabolites, with the exception of hippuric acid, were also excreted in the form of glucuronide or sulfate. The radioactivity transported into the thoracic duct was only 0.3% of the dose, and of this, more than 80% was found to be γ-oryzanol by thin-layer chromatography. From these results, it is considered that γ-oryzanol administered orally is absorbed mainly into the blood via the portal vein system, not into the lymph via the thoracic duct.

Stimulation of Bile Acid Biosynthesis by Clofibrate

The hypocholesterolemic effect of clofibrate (ethyl p-chlorophenoxyisobutyrate) was investigated in rats under conditions of severe hypercholesterolemia produced by administering relatively large amounts of cholesterol. The rats were fed a normal chow (control rats) or a chow containing 0.25% clofibrate (treated rats) for 14 d, then Triton WR-1339 was administered intraperitoneally (100 mg/100 g body weight). Four days after this administration, the blood cholesterol level of the control rats was markedly higher at 9335 mg/dl serum, while the level of the treated rats was about 30% lower than that of the control. The bile acid level in pooled 24-h bile was proportionally higher (about 1.3-fold) in the treated rats than that in the control. In the initial bile (within 4 h after bile duct cannulation), the bile acid level in the treated bile was 2.4 times higher than in the control bile. [4-¹⁴C] Cholesterol and 100 mg non-labeled cholesterol were injected intraperitoneally into the control and clofibratetreated rats, and the radioactivities excreted into the bile were determined. The early bile (within 8 h) of the treated rats contained 5.6-fold higher radioactivity than the control bile, and the radioactivities were largely recovered in the bile acid fraction ; scarcely any radioactivity was found in the cholesterol fraction. From these results, we conclude that one of the mechanisms by which the hypocholesterolemic effect of clofibrate is mediated is stimulation of the degradation of cholesterol, that is, stimulation of the biosynthesis of bile acids.

Odorous Metabolites of Fungi, Chaetomium globosum KINZE ex FR. and Botrytis cinerea PERS. ex FR., and a Blue-green Alga, Phormidium tenue (MENEGHINI) GOMONT

Two strains of earthy-musty smelling fungi, identified as Chaetomium globosum KINZE ex FR. and Botrytis cinerea PERS. ex FR., were isolated from soil samples collected at Sugadaira, Nagano Prefecture. Geosmin, having a strong earthy-musty smell, and 2-phenylethanol were detected as volatile metabolites of Chaetomium globosum, while furfural, benzaldehyde, phenylacetaldehyde, and benzyl cyanide were identified as metabolites of Botrytis cinerea. On the other hand, 2-methylisoborneol (with an earthy-muddy smell) was detected in the culture of Phormidium tenue (MENEGHINI) GOMONT, a blue-green alga isolated from water in Sengari Reservoir (Kobe City Water Supply Bureau). Another compound was also detected and identified as 2, 6-di-tert-butyl-p-benzoquinone, which would be a minor component in tap water. The present results suggest that, besides actinomycetes and blue-green algae, fungi may also be responsible for the objectionable earthy-musty odor and taste sometimes apparent in public water supplies.

Saponin and Sapogenol. XXXI. Chemical Constituents of the Seeds of Vigna angularis (WILLD.) OHWI et OHASHI. (1). Triterpenoidal Sapogenols and 3-Furanmethanol β-D-Glucopyranoside

3-Furanmethanol β-D-glucopyranoside (1) and (+)-catechin 7-O-β-D-glucopyranoside (3) were isolated from azuki beans, the seeds of Vigna angularis (WILLD.) OHWI et OHASHI (Leguminosae) and their structures were substantiated. The saponin mixture designated as total azukisaponin was also isolated from azuki beans. By means of enzymatic hydrolysis, acidic hydrolysis, and photochemical degradation, four genuine sapogenols, which included three known sapogenols, sophoradiol (7), soyasapogenol B (8), gypsogenic acid (9), and a new sapogenol named azukisapogenol (10), were isolated from total azukisaponin and the structure of 10 was elucidated. As one of the artifact sapogenols which were liberated by acidic hydrolysis of total azukisaponin, a new sapogenol named anhydrosophoradiol (5) was isolated and its structure was elucidated.

Saponin and Sapogenol. XXXII. Chemical Constituents of the Seeds of Vigna angularis (WILLD.) OHWI et OHASHI. (2). Azukisaponins I, II, III, and IV

Six oleanene-oligoglycosides named azukisaponins I (1), II (2), III (3), IV (4), V, and VI were isolated from azuki beans, the seeds of Vigna angularis (WILLD.) OHWI et OHASHI (Leguminosae). Among them, the structures of azukisaponins I, II, III, and IV were elucidated as 3-O-[β-D-glucopyranosyl (1→2)-β-D-glucuronopyranosyl] sophoradiol (1), 3-O-[β-D-glucopyranosyl (1→2)-β-D-glucuronopyranosyl] soyasapogenol B (2), 3-O[β-D-glucopyranosyl (1→2)-β-D-glucuronopyranosyl] azukisapogenol (3), and 3-O-(β-D-glucopyranosyl)-28-O-[β-D-glucopyranosyl (1→6)-β-D-glucuronopyranosyl] gypsogenic acid (4), respectively on the basis of chemical and physicochemical evidence.

Saponin and Sapogenol. XXXIII. Chemical Constituents of the Seeds of Vigna angularis (WILLD.) OHWI et OHASHI. (3). Azukisaponins V and VI

The chemical structures of azukisaponins V (1) and VI (5), two of the six oligoglycosidic ingredients of total azukisaponin isolated from azuki beans, the seeds of Vigna angularis (WILLD.) OHWI et OHASHI (Leguminosae), were investigated. By means of photochemical degradation and chemical analyses, the structures of azukisaponins V and VI were elucidated to be 3-O-[α-L-rhamnopyranosyl (1→2)-β-D-glucopyranosyl (1→2)-β-D-glucuronopyranosyl]-soyasapogenol B (1) and 3-O-[β-D-glucopyranosyl (1→2)-β-D-glucuronopyranosyl]-29-O-[β-D-glucopyranosyl (1→6)-β-D-glucuronopyranosyl] azukisapogenol (5), respectively. Azukisaponin VI (5) is the first reported example of a 3, 29-bisdesmoside of an oleanene oligoglycoside.

Saponin and Sapogenol. XXXIV. Chemical Constituents of Astragali Radix, the Root of Astragalus membranaceus BUNGE. (1). Cycloastragenol, the 9, 19-Cycloanostane-type Aglycone of Astragalosides, and the Artifact Aglycone Astragenol

Triterpene-oligoglycoside constituents of Astragali Radix, the root of Korean Astragalus membranaceus BUNGE (Leguminosae), were isolated. By means of enzymatic and chemical degradations, the 9, 19-cyclolanostane-type triterpene named cycloastragenol (1), which was the common genuine aglycone of ten of eleven astragalosides, and the lanost-9 (II)-ene-type counterpart named astragenol (5), which was an artifact aglycone secondarily formed from 1, were isolated. On the basis of chemical and physicochemical evidence, the structures of cycloastragenol and astragenol were elucidated as (20R, 24S)-3β, 6α, 16β, 25-tetrahydroxy-20, 24-epoxy-9, 19-cyclolanostane (1) and (20R, 24S)-3β, 6α, 16β, 25-tetrahydroxy-20, 24-epoxy-lanost-9 (11)-ene (5), respectively.

Saponin and Sapogenol. XXXV. Chemical Constituents of Astragali Radix, the Root of Astragalus membranaceus BUNGE. (2). Astragalosides I, II and IV, Acetylastragaloside I and Isoastragalosides I and II

Twelve triterpene-oligoglycosides were isolated from the glycosidic constituents of Astragali Radix, the root of Korean Astragalus membranaceus BUNGE. (Leguminosae). They were acetylastragaloside I (3), isoastragalosides I (5) and II (7), astragalosides I (4, major), II (6), III, IV (8), V, VI and VII, which contain a 9, 19-cyclolanostane cycloastragenol (1) as the aglycone, and astragaloside VIII and soyasaponin I (9), which possess an oleanene-type aglycone, soyasapogenol B. By means of chemical degradations, which included a selective cleavage method for the glucuronide linkage, and ¹³C-NMR examinations, the structure of astragaloside IV was elucidated as 3-O-β-D-xylopyranosyl-6-O-β-D-glucopyranosylcycloastragenol (8). In addition, the structures of five acetyl derivatives of 8 : acetylastragaloside I, astragaloside I, isoastragaloside I, astragaloside II and isoastragaloside II, were elucidated as 3-O-β-(2', 3', 4'-tri-O-acetyl)-D-xylopyranosyl- (3), 3-O-β-(2', 3'-di-O-acetyl)-D-xylopyranosyl- (4), 3-O-β-(2', 4'-di-O-acetyl)-D-xylopyranosyl- (5), 3-O-β-(2'-O-acetyl)-D-xylopyranosyl- (6) and 3-O-β-(3'-O-acetyl)-D-xylopyranosyl-6-O-β-D-glucopyranosylcycloastragenol (7), respectively.

Saponin and Sapogenol. XXXVI. Chemical Constituents of Astragali Radix, the Root of Astragalus membranaceus BUNGE. (3). Astragalosides III, V, and VI

Based on chemical and physicochemical investigations including carbon-13 nuclear magnetic resonance (¹³C-NMR) examinations and methylation analyses, the structures of three astragalosides, which were isolated from Astragali Radix, the root of Korean Astragalus membranaceus BUNGE (Leguminosae), were elucidated : astragaloside III is 3-O-[β-D-glucopyranosyl (1→2)-β-D-xylopyranosyl] cycloastragenol (3), astragaloside V is 3-O-[β-D-glucopyranosyl (1→2)-β-D-xylopyranosyl]-25-O-β-D-glucopyranosyl-cycloastragenol (5) and astragaloside VI is 3-O-[β-D-glucopyranosyl (1→2)-β-D-xylopyranosyl]-6-O-β-D-glucopyranosyl-cycloastragenol (6).

Saponin and Sapogenol. XXXVII. Chemical Constituents of Astragali Radix, the Root of Astragalus membranaceus BUNGE. (4). Astragalosides VII and VIII

By means of enzymatic degradation and by application of a selective cleavage method for the glucuronide linkage, as well as by the carbon-13 nuclear magnetic resonance (¹³C-NMR) analysis, the structures of two astragalosides, which were isolated as two of eleven astragalosidesfrom Astragali Radix (the root of Korean Astragalus membranaceus, Leguminosae), were elucidated : astragaloside VII is 3-O-β-D-xylopyranosyl-6-O-β-D-glucopyranosyl-25-O-β-D-glucopyranosyl-cycloastragenol (4) and astragaloside VIII is 3-O-[α-L-rhamnopyranosyl (1→2)-β-D-xylopyranosyl (1→2)-β-D-glucuronopyranosyl] soyasap-ogenl B (8). Astragaloside VII (4) is an unprecedented example of a triterpene-tridesmoside.

Synthesis of 1-Isocyanomethyl Azoles and Related Compounds

1-Isocyanomethyl azoles (14a-f) were synthesized by the reaction of the corresponding azoles (11a-f) with trimethylformamidomethylammonium iodide (8), followed by dehydration of the resulting 1-formamidomethyl azoles (13a-f) using phosphorus oxychloride or triphenylphosphine/carbon tetrachloride. Furthermore, 1-substituted methyl-5-piperidinomethyltetrazoles (15a-f) were prepared by means of the four-component condensation of 14a-f with formaldehyde, sodium azide, and piperidine.

Syntheses of 2-Acetamido-2-deoxy-4-O-β-D-galactopyranosyl-D-glucopyranose (N-Acetyllactosamine) Derivatives

In order to provide useful key intermediates for syntheses of complex oligosaccharides, anomeric 1, 2', 3', 4', 6, 6'-hexa-O-acetyl-N-acetyllactosamines (8 : α, and 9 : β) and the corresponding 3-O-benzyl ethers (5 : α, and 6 : β) were synthesized. Condensation of 1, 6-anhydro-3-O-benzyl-β-N-acetylglucosamine with acetobromogalactose by a conventional Koenigs-Knorr procedure, followed by selective acetolysis of the 1, 6-anhydro-β-linkage, provided 5 and 6. Debenzylation of 5 and 6 gave 8 and 9, respectively.

Studies on Tetrahydroisoquinolines. XX. A Novel Synthesis of 8-Aryl-1, 2, 3, 4-tetrahydroisoquinolines

Treatment of a mixture of the p-quinol acetate (4) and aryl ethers with trifluoroacetic acid gave 8-aryl-1, 2, 3, 4-tetrahydroisoquinolines (1a-f) in good yields. Similar reaction of 4 and corypalline (3) afforded a corypalline dimer (5).

Reaction of Benzoxazoline-2-thiones with Alkyl Halides

The effect of the solvent on the reaction of benzoxazoline-2-thiones with alkyl halides was studied. The reaction of 1 with alkyl halides and potassium carbonate in dimethylformamide (DMF) gave the corresponding 2-alkylthiobenzoxazoles (2), but the same reaction gave 2-methoxybenzoxazoles (4a) when methanol was used in place of DMF as the solvent. On the other hand, the reaction of 1, methyl iodide, alcohol, and sodium hydride in tetrahydrofuran (THF) gave 2-[N-(dialkoxymethylene) amino] phenols (5).