The hydrolysis and fluoride complexation behavior of Fe(III) at 25°C and 0.68 molal ionic strength

Fe(III) hydrolysis and fluoride complexation behavior was examined in 0.68 molal sodium perchlorate at 25°C. Our assessment of the complexation of Fe(III) by fluoride ions produced the following results: log_F1 = 5.15₅, log_F2 = 9.10₇, log_F3 = 11.96, log_F4 = 13.7₅, where log_Fn = 5.15₅=[FeF _n ^(3-n)+ ][Fe³⁺]^–1[F^–]^–n. The stepwise fluoride complexation constants,FK _n+1, obtained in our work (where log_F K _n+1 =log_Fn) indicate that K _n+1/K _n =0.072±0.01. Formation constants for equilibria, Fe³⁺+nH₂OFe(OH) _n ^(3–n)+ +nH⁺, expressed in the form _n ^* [Fe(OH) _n ^(3-n)+ ][H⁺]ⁿ ,[Fe ³⁺]^-1, were estimated as ₁ ^* = –2.754, and ₂ ^* –7. Our study indicates that the results of previous hydrolysis investigations include very large overestimates of Fe(OH) ₂ ⁺ formation constants.     

Rearrangement ofα -trifluoromethyl-β-dialkylamino-β-fluoroacrylic acid N.N-dialkylamides

Conclusions When heated in the presence of a catalytic amount of BF₃ etherate,-trifluoromethyl--diethylamino--fluoroacrylic acid N, N-dimethylamide is reversibly isomerized to-trifluoromethyl--dimethylamino--fluoroacrylic acid N, N-diethylamide. The methyl esters of-trifluoromethyl--diethylammo--fluoroacrylic acid and-trifluoromethyl--phenoxy--fluoroacrylic acid N,N-dimethylamide are not isomerized under the same conditions.Translated from Izvestiya Akademii Nauk SSSR, Seriya Khimicheskaya, No.1, pp.137–141, January, 1976.     

Improvement of Solubility and Dissolution of 19-Norprogesterone via Inclusion Complexation

In an effort to modify the solubility and dissolution rate of the contraceptive steroid, 19-norprogesterone in order to improve its bioavailability, the cyclodextrin complexation approach was chosen. In solution, the complex formation with -cyclodextrin (-CD), hydroxyethyl -cyclodextrin (HE--CD) and hydroxypropyl -cyclodextrin (HP--CD) was confirmed by using solubility, UV, IR and ¹H-NMR spectrophotometric techniques. The phase solubility diagrams were categorized as A_L-type. The complexing affinity of the CDs investigated were ranked as follows: -CD > HP--CD > HE--CD. The complexation thermodynamic parameters were obtained from the temperature dependence of the dissociation constants. In the solid state, differential scanning calorimetery (DSC) and optical microscopy methods were utilized to characterize the complexes. Dissolution studies showed that such molecularly encapsulated forms offered a marked improvement in the dissolution rate compared to the parent drug.     

Effect of 2-Hydroxypropyl-β-cyclodextrin on Release Rate of Metoprolol from Ternary Metoprolol/2-hydroxypropyl-β-cyclodextrin/Ethylcellulose Tablets

The effect of 2-hydroxypropyl--cyclodextrin (HP--CyD) on the release of a water-soluble ₁-selective adrenoreceptor antagonist, metoprolol (Met), from ternary Met/HP--CyD/ethylcellulose (EC) tablets was investigated. The release rate of Met from the ternary tablets was dependent on amounts of HP--CyD in the tablets, i.e., the rate decreased when small amounts of HP--CyD were added, while large amounts of HP--CyD accelerated the rate. The slowest rate was observed for the tablet consisted of a 30/10/60 weight ratio of Met/HP--CyD/EC. The analyses of the release rates by the Korsmeyer equation and their temperature dependence suggested that Met is released from the EC matrix containing HP--CyD according to the diffusion-controlled mechanism. The water penetration studies and the micro- and macroscopic observations suggested that the retarding effect of HP--CyD is attributable to a viscous gel formation in small pores on the surface of the tablets, where HP--CyD gels may work as a barrier for the water penetration into the tablets and the release of the drug from the tablets. The in-vitro release property of the ternary tablets was reflected in the in-vivo absorption profile in dogs. The results indicated that a combination of HP--CyD and EC is useful for the release control of water-soluble drugs such as Met.     

The effects of cyclodextrin inclusion of the ferrocenemonocarboxylate anion on the kinetics of its oxidation by bis(pyridine-2,6-dicarboxylato)cobaltate(III) in aqueous solution

The effects of -, -, dm-(heptakis(2,6-di-O-methyl)--) and -cyclodextrins (CD) on the kinetics of the electron-transfer reaction of the ferrocenemonocarboxylate anion (FCA^–) with bis(pyridine-2,6-dicarboxylato)cobaltate(III) have been investigated in aqueous solution (0.20 M Na₂HPO₄, pH 9.2) at 25.0°C. Substantial decreases in the rate constants for the electron-transfer reactions were observed upon cyclodextrin inclusion of the reductant, due to an increase in the FCA^0/– reduction potential and to the insulation of the reductant from oxidant. The inclusion stability constants for {FCA·CD}^– were evaluated from the¹H NMR and kinetic data, and the order of the stability constants was found to be -CDdm-CD-CD>-CD.     

Violurato complexes of nickel(II). Formation equilibria. Deprotonation equilibria of the coordinated ligands and related stereochemical changes

Summary The formation equilibria of nickel(II) violurato-complexes in water and dimethylsulphoxide-water (8020) as well as deprotonation of the coordinated ligands and related stereochemical changes are reported. The stability constants of the Ni²⁺-H₂V^– complexes log₁=5.06, Iog₂=9.38, log₃=12.98 as well as the acidity constants of the [Ni(H₂V)₃]^– complex, log_j1= 8.37, log_j2=15.76, log_j3=22.37 are determined at 25 °C and 0.1M NaClO₄. A new violurato-complex of Ni²⁺, Na₄[Ni(HV)₃]5H₂O, is isolated and characterized.     

The Coordination Number of Lu(III) in a Mixed System of Methanol and Water

The stability constants (_1(F)) of the monofluoro complex of Lu(III) and those (_1(Cl)) of the monochloride solvent-shared ion-pair of Lu(III) have been determined in mixed solvents of methanol and water at 0.10 and 1.00 mol·dm^–3 ionic strengths, respectively. The variation in ln_1(F) with an increase in the mole fraction of methanol (X _s) in the mixed solvent system showed an acute-angled convex inflection point at X _s 0.12, an acute-angled concave inflection point at X _s 0.22, and another acute-angled convex inflection point at X _s 0.27. It was concluded that the first and the second convex inflection points denoted the CN of Lu³⁺ from CN = 8 to a mixture of CN = 8 and 7 and from CN = 8 and 7 to a mixture containing CN = 6, respectively. The concave point is the starting point of a change in the CN of Lu(III) in LuF²⁺ from CN = 8 to a mixture of CN = 8 and 7. The values of two inflection points of the CN around Lu³⁺ are consistent with the inflection points of the variation in the values of ln_1(Cl) versus the dielectric constant of the mixed solvent.     

Complexation of the Non-steroidal Anti-inflammatory Drug Loxoprofen with Modified and Unmodified β-Cyclodextrins

The inclusion complex of the anti-inflammatory drug, loxoprofen, with -cyclodextrin-(CD), sulfated -CD, and glycerol ether -CD was studied by UV-VIS absorption and ¹H-NMR spectroscopy in solution. The inclusion complex of loxoprofen with -CDs was prepared by freeze-drying, and then characterized in the solid state by thermal analysis, X-ray diffraction, FT-IR and FT-Raman spectroscopy, and scanning electron microscopy (SEM). Furthermore, a physical mixture of loxoprofen/-CD (1/1, mol-%) in the solid state was also characterized. The solubility of the loxoprofen increased on addition of -CDs. The solubility enhancement of the loxoprofen with -CDs is in the following order: glycerol ether -CD > sulfated -CD > -CD.     

Ultrasonic study of the molecular encapsulation and the micellization processes of dodecylethyldimethylammonium bromide-water solutions in the presence of β-cyclodextrin or 2,6-di-o-methyl-β-cyclodextrin

Aqueous solutions of -cyclodextrin (-CD) or 2,6-di-o-methyl--cyclodextrin (DM--CD) and dodecylethyldimethylammonium bromide (D₁₂EDMAB) have been studied from speed of sound (u) data at 298.15 K, using a pulse-echo-overlap technique. The molecular encapsulation process of the surfactant monomer into the cyclodextrin cavity and its effect in the micellization process of the surfactant have been analyzed from theu measurements: I) as a function of [D₁₂EDMAB] in the presence of several initial cyclodextrin concentrations (-CD or.DM--CD); II) as a function of [cyclodextrin] (-CD or DM--CD), for an initial micellar solution of D₁₂EDMAB and; III) as a function of the [cyclodextrin]/[surfactant] stoichiometric concentrations. Both inclusion complexes formed (-CDD₁₂EDMAB) and (DM--CDD₁₂EDMAB) have stoichiometries of 11, and their association constantK have been determined using a model proposed in this work, based on the additivity of the different contributions of the involved species to the speed of sound. The apparent critical micellar concentration, cmc^*, of D₁₂EDMAB is found to increase linearly upon the addition of cyclodextrin (-CD or DM--CD). The free surfactant concentration in the micellar region, [D₁₂EDMAB]_f, decreases in the presence of -CD and slightly increases in the presence of DM--CD. The influence of the parcial methylation of the -cyclodextrin (-CDDM--CD) and of the polar head of the surfactant (D₁₂TAB D₁₂EDMAB) on the complextion and micellar parameters are also discussed.Supplementary material available: Tables of speed of sound (14 pages) are available from the authors.     

Chemistry of acetals

Summary -Ethoxyacrolein, -ethoxy--methylacrolein, -ethoxy--amylacrolein, the sodium enolate of malonic dialdehyde, bromomalonic dialdehyde, and octatrien-2,4,6-dial-1,8 were reduced at a dropping mercury electrode. The reduction waves had diffusion character.     

Composition and stability constants of iron- and copper-oxytetracycline chelates

Summary The composition and stability constants of iron and copper oxytetracycline chelates are determined by spectrophotometric and pH-metric methods. The stepwise stability constants are log ₁ 9.79, log ₂ 7.08, log ₃ 5.92 and log ₁ 7.28 and log ₂ 5.29 for iron and copper chelates, respectively. The thermodynamic parameters of these reactions and the site of chelation in oxytetracycline are also investigated. The reaction of iron(III) has been used for the spectrophotometric determination of oxytetracycline in some pharmaceutical preparations. Results with a coefficient of variation in the range of 1.6% and a mean recovery of 98.6% are obtained.

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Zusammensetzung und Stabilitätskonstanten der Eisen- und Kupferkomplexe mit Oxytetracyklin

Zusammenfassung Spektrophotometrische Methoden und pH-Messung ermöglichten die Bestimmung der im Titel angeführten Größen. Die Stabilitätskonstanten für die Eisen- bzw. Kupfer-Chelate sind: log/gb₁ 9,79; log ₂ 7,08; log ₃ 5,92; bzw. log ₁ 7,28; log ₂ 5,59. Die thermodynamischen Parameter dieser Reaktionen und die Art der Chelatbildung des Oxytetracyklin-Moleküls wurden ebenfalls untersucht. Die Reaktion mit Eisen(III) wurde für die Bestimmung von Oxytetracyklin verwendet. Ergebnisse mit einem Variationskoeffizienten 1,6% und einer mittleren Wiederfindungsrate von 98,6% wurden erzielt.

     

The Cyclodextrins as Modelling Agents of Drug Controlled Release

The controlled release of nicardipine (NC) was achieved by hybridizing its hydrophilic and hydrophobic cyclodextrin (CDs) complexes, i.e., those with hydroxypropyl--cyclodextrin (HPCD) andtriacetyl--cyclodextrin (TACD),respectively. ¹H-nuclearmagnetic resonance (¹H-NMR) was performed to examine the interaction between both CDs and NC in solution. The solid complexes of NC : HPCD and NC : TACD were prepared, in a 1 : 1 molar ratio by the spray-drying method. Complexation in the solid state was demonstrated by differential scanning calorimetry (DSC) and powder X-ray diffractometry. In vitro dissolution studies were carried out in simulated gastric (pH 1.2) and intestinal (pH 6.8) fluids, according to the USP basket method. The ¹H-NMR studies provided clear evidence of an interaction between the CDs and the aromatic rings of NC. The DSC thermograms of the solid complexes showed no endothermic peak due to NC melting and their diffraction pattern was completely diffuse, which suggested the formation of a novel type solid phase with an amorphous character. The low dissolution rate of NC, a weak basic drug, in alkaline medium was significantly improved by complexation with HPCD. In contrast, the in vitro release of this drug from the NC : TACD complexes was markedly retarded in both dissolution media. An optimal formulation was then designed by the combination, in different molar ratios, of these two complexes. The release behavior of these preparations was investigated and it was observed that the retarding effect was dependent on the amount of the NC : TACD complex. In addition, the initial release rate became faster as the molar ratio of the NC : HPCD complex increased.     

Two new triterpene glycosides from the holothurian Duasmodactyla kurilensis

Two new glycosides have been isolated from the total triterpene glycosides of the holothurianDuasmodactyla kurilensis: kurilosides A (III) and C (IV). It has been established that (III) is 16-acetoxy-3-{[O--D-glucopyranosyl-(1 4)-O--D-quinovopyranosyl-(1 2)]-[O-(3-O-methyl--D-glucopyranosyl)-(1 3)-O-(6-O-(sodium sulfato)--D-glucopyranosyl)-(1 4)]--D-xylopyranosyloxy}-4,4,14-trimethylpregen-9(11)-en-20-one, while the minor glycoside (IV) is 16-acetoxy-3-{O--D-quinovopyranosyl-(1 2)-[O-(3-O-methyl--D-glucopyranosyl-(1 3)-O-(6-O-(sodium sulfato)--D-glucopyranosyl)-(1 4)]--D-xylopyranosyloxy}-4,4,14-trimethylpregn-9(11)-en-20-one.Pacific Ocean Institute of Bioorganic Chemistry, Far Eastern Branch, Academy of Sciences of the USSR, Vladivostok. Translated from Khimiya Prirodnykh Soedinenii, No. 2, pp. 221–226, March–April, 1991.     

Reaktion der Azlactone mit Aminoverbindungen, 3. Mitt.: Über die Herstellung der Phenylhydrazide und 4-Nitrophenylhydrazide einiger α,β-disubstituierter Acrylsäuren

Zusammenfassung Ungesättigte Azlactone spalten sich mit Phenylhydrazin bzw. 4-Nitro-phenylhydrazin auf unter Bildung der Phenylhydrazide (1a–1o) bzw. 4-Nitro-phenylhydrazide (2a, 2b) der entsprechenden ,-disubstituierten Acrylsäuren. Zum Unterschied von den durch die Hydrazinolyse entstandenen Hydraziden der ,-disubstituierten Acrylsäuren, die sich leicht zu 3,5-disubstituierten 6-Hydroxy-1,2,4-triazinen^{1, 2} bzw. zu Pyrazolderivaten^{3, 4, 5} cyclisieren lassen, ist es nicht gelungen, unter gleichen Bedingungen die Phenylhydrazide bzw. 4-Nitro-phenylhydrazide zu cyclisieren. Zum Strukturbeweis dienten NMR-Spektren.

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Reaction of azlactones with amino compounds, III: Preparation of the phenylhydrazides and 4-nitrophenylhydrazides of several ,-disubstituted acrylic acids

The reaction of phenylhydrazine and 4-nitrophenylhydrazine with several unsaturated azlactones has resulted in their cleavage to the phenylhydrazides (1a–1o) and 4-nitrophenylhydrazides (2a, 2b), respectively, of the corresponding ,-unsaturated acrylic acids. In contradistinction to the hydrazides of ,-unsaturated acrylic acids, which had previoulsy been obtained by hydrazinolysis of unsaturated azlactones and had easily undergone cyclisation to 3,5-disubstituted 6-hydroxy-1,2,4-triazines^{1, 2} or pyrazole derivatives^3–5, the phenylhydrazides and 4-nitrophenylhydrazides could not be cyclised under comparable conditions. NMR spectroscopy was used to ascertain the structures of the reaction products.

     

Complexation of Eu3+ and Am3+ with soil humic acid extracted from Okchon Basin of Korean Peninsula

The complexation of Eu³⁺ and Am³⁺ ions with the humic acids has been investigated at various pH (4.0, 4.5, 5.0, 5.4) in 0.1M NaClO₄ solution using solvent extraction technique. Two humic acids are used in this study: humic acid extracted from the soil of Taejon on the Okchon Basin of Korea (TJHA) and commercially available one from Aldrich Chemical Co. (AHA). The total carboxylate group concentrations were determined to be 3.58 meq/g and 4.59 meq/g for Taejon and Aldrich humic acids, respectively. The conditional stability constants (log ₁ and log ₂), dependent on the pH of the solution, of the complexes of Eu³⁺ and Am³⁺ ions with the humic acids have been determined at the ionic medium of 0.1M NaClO₄. The values of stability constants with the degree of ionization of TJHA for Eu and Am complexes are quite well agreed with those of Lake Bradford humic acid (LBHA), indicating that structural characteristics of TJHA and LBHA may be quite similar to one another.     

Polymorphism of (+)N-tosyl-L-glutamic acid

It has been shown that polymorphism is the reason for the occurrence of (+)N-tosyl-L-glutamic acid 1 with various melting points. 1 occurs in two crystalline forms: and . Form -1 (prisms) having a melting point of 145–147°C is chemically pure and stable. Form -1, however, is unstable and is formed as a result of the stabilizing effect of an organic solvent not introduced into the structure of the crystal. At about 125°C the forms is transformed to the form. The melting point of the form depends on the amount and type of solvent contained in the crystal, which, during measurement cannot leave the system.     

Radiation-induced reactions of cholesterol in an aqueous medium

⁶⁰Co -ray radiolysis of cholesterol /3-hydroxy-5-cholestene/ /I/ in the two-phase system /water-ethyl acetate/ and in the presence of air has been studied using TLC and GC methods. The following products were observed in the irradiated mixture: 3, 7-dihydroxy-5-cholestene /II/, G O. 36, 3-hydroxy-7-keto-5-cholestene /III/, G 1.48, 3-hydroxy-7-keto-5-cholestane /IV/, G 0.22, 3,5,6-trihydroxy-5-cholestane /V/, G 0.83, 5,6-epoxy-3-hydroxy-5-cholestane /VIa/, G 0.26, 5,6-epoxy-3-hydroxy-5-cholestane /VIb/, G 0.24, and 2, 3-dihydroxy-5-cholestene /VII/, G 0.22. The dose dependence of the formation of these products shows that the cholesterol derivatives substituted in the position 7 /II–IV/ are formed from a common precursor — the radical Ia. On the other hand, the products of the 5–C=C double bond reactions /V and VI/ are formed independently. Also the product VII is formed independently. A reaction scheme that is in agreement with these results is proposed.     

The role of excited states in the photolysis of n-butyraldehyde, II. Intersystem crossing quantum yields

Singlet triplet intersystem crossing quantum yields were determined for n-butyraldehyde, using the photosensitized cis-trans isomerization of piperylene to monitor the process. At room temperature and 313 nm, 0.58±0.05 and 0.72±0.05 were obtained for the triplet yield in the vapor phase and in isooctane, respectively.

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- - - . 0,58±0,05 0,72±0,05 313 .

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For Part I, see Ref. /1/     

New polyhydroxysteroids from the far-eastern starfish Henricia sp.

From the far-eastern starfishHenricia sp. we have isolated and characterized the new polyhydroxysteroid (24S)-5-cholestane-3,4,6,8,15,24-hexaol and three new glycosides: (24S)-5-cholestane-3,4,6,8,15,24-hexaol 3-O-(2,4-di-O-methyl--D-xylopyranoside) (henricioside H₁), 24-methyl-5-cholesta-4,22E-diene-3,6,8,15,16,26-hexaol 3-O-(2,3-di-O-methyl--D-xylopyranoside) (henricioside H₂), and the 22,23-dihydro derivative of henricioside H₂ (henricioside H₃).Pacific Ocean Institute of Bioorganic Chemistry, Far-Eastern Scientific Center, Russian Academy of Sciences, Vladivostok. Translated from Khimiya Prirodnykh Soedinenii, No. 2, pp. 249–253, March–April, 1993.     

Transformations of solasodine

Solasodine (I) has been subjected to a number of transformations. The following compounds have been obtained from it by described procedures: 3-acetoxypregna-5,16-dien-20-one (II), 3-acetoxypregn-5-en-20-ol (III), and 3-acetoxypregn-5-en-20-ol (IV). The oxidation of (III) and (IV), the formation of an oxime, and the reduction of the oxime with sodium in ethanol, followed by Hess methylation, has led to 20-dimethylaminopregn-5-en-3-ol (IX) and to 20-dimethylaminopregn-5-en-3-ol (X). From compounds (IX) and (X), by analogy with (III) and (IV) by their oxidation and the preparation of oximes, which were then reduced and methylated, the following were obtained: 3,20-bisdimethylaminopregnane (XVII) and 3,20-bisdimethylaminopregnane (XVIII), and also quaternary salts of the latter.Institute of the Chemistry of Plant Substances, Academy of Sciences of the Uzbek SSR, Tashkent. Translated from Khimiya Prirodnykh Soedinenii, No. 3, pp. 370–374, May–June, 1980.