Benzo concentrations

Hydrolysis of p-tolunitrile to p-toluic acid. Boil a mixture of 5 g. of p-tolunitrile, 80 ml. of 10 per cent, aqueous sodium hydroxide solution and 15 ml. of alcohol under a reflux condenser. (The alcohol is added to prevent the nitrile, which volatUises in the steam, from crystalhsing in the condenser it also increases the speed of hydrolysis. The alcohol may be omitted in the hydrolysis of nitriles which are hquid at the ordinary temperature, e.g., benzo-nitrUe.) The solution becomes clear after heating for about 1 hour, but continue the boiling for a total period of 1 - 5 hours to ensure complete hydrolysis. Detach the condenser and boil the solution for a few minutes in the open flask to remove dissolved ammonia and incidentally some of the alcohol CAUTION /). Cool, and add concentrated hydrochloric acid until precipitation of the p-toluic acid is complete. When cold, filter off the p-toluic acid with suction and wash with a little cold water. Recrystallise from a mixture of equal volumes of water and alcohol (methylated spirit) or from benzene. The yield of p-toluic acid, m.p. 178°, is 5-5 g. 

Hydrolysis of benzonitrile to benzoic acid. BoU 5 -1 g. (5 ml.) of benzo-nitrUe and 80 ml. of 10 per cent, sodium hydroxide solution in a 250 ml. round-bottomed flask fitted with a reflux water condenser until the condensed liquid contains no oUy drops (about 45 minutes). Remove the condenser, and boU the solution in an open flask for a few minutes to remove free ammonia. Cool the liquid, and add concentrated hydrochloric acid, cautiously with shaking, until precipitation of benzoic acid is complete. Cool, filter the benzoic acid with suction, and wash with cold water dry upon filter paper in the air. The benzoic acid (5-8 g.) thus obtained should be pure (m.p. 121°). Recrystal-lise a small quantity from hot water and redetermine the m.p. 

Ben zotricbl oride is hydrolyzed to benzoic acid by hot water, concentrated sulfuric acid, or dilute aqueous alkaH. Benzoyl chloride [98-88-4] is produced by the reaction of benzotrichloride with an equimolar amount of water or an equivalent of benzoic acid. The reaction is catalyzed by Lewis acids such as ferric chloride and zinc chloride (25). Reaction of benzotrichloride with other organic acids or with anhydrides yields mixtures of benzoyl chloride and the acid chloride derived from the acid or anhydride (26). Benzo triflu oride [98-08-8] is formed by the reaction of benzotrichloride with anhydrous hydrogen fluoride under both Hquid- and vapor-phase reaction conditions. 

The use of free-radical reactions for this mode of ring formation has received rather more attention. The preparation of benzo[Z)]thiophenes by pyrolysis of styryl sulfoxides or styryl sulfides undoubtedly proceeds via formation of styrylthiyl radicals and their subsequent intramolecular substitution (Scheme 18a) (75CC704). An analogous example involving an amino radical is provided by the conversion of iV-chloro-iV-methylphenylethylamine to iV-methylindoline on treatment with iron(II) sulfate in concentrated sulfuric acid (Scheme 18b)(66TL2531). 

D. ci - -Thiabicyclo[4 .. Q]nonan S,S-Dioxide [Benzo[c]thiophene 2,2-dioxide, cis-octahydro-]. A solution of the sulfide (43.0 g., 0.303 mole) in 11. of ether is cooled to 0° and treated dropwise while magnetically stirred with 1.01. of 0.65iV ethereal monoperphthalic acid (0.65 mole). The mixture is kept overnight at 0°, after which time the precipitated phthalic acid is separated by filtration and the filtrate concentrated with a rotary evaporator. Bulb-to-bulb distillation of the residual oil at 0.05-0.1 mm. affords the sulfone as a eolorless liquid (48.5-50 g., 92-95%) (Note 11). This product is crystallized from ether-hexane to give a colorless solid, m.p. 39-41° (Note 12). 

The vapor pressure of a compound is important in determining the upper limit of its concentration in the atmosphere. High vapor pressures will permit higher concentrations than low vapor pressures. Examples of organic compounds are methane and benzo[fl]pyrene. Methane, with a relatively high vapor pressure, is always present as a gas in the atmosphere in contrast, benzo[fl]pyrene, with a relatively low vapor pres.surc, is. id-... 

Fig. 42 Chromatogram of polycyclic aromatic hydrocarbons on caffeine-impregnated precoated silica gel 60 HPTLC plates with concentrating zone (Merck). The following can be recognized in increasing Rf value. — 1. benzo(ghi)perylene, 2. indeno(l,2,3-cd)pyrene, 3 benzo(a)pyrene, 4. benzo(b)fluoranthene, 5. benzo(k)fluoranthene, 6. fluoranthene.

It would be expected that the stabilization of the adsorbed species by an extended conjugated system should increase with the number of aromatic rings in the adsorbed azahydrocarbon. However, data suitable for comparison are available only for phenanthridine, benzo-[/]quinoline, and benzo[h] quinoline. The large difference in the yields of biaryl obtained from the last two bases could be caused by steric interaction of the 7,8-benz-ring with the catalyst, which would lower the concentration of the adsorbed species relative to that with benzo[/]quinoline. The failure of phenanthridine to yield any biaryl is also noteworthy since some 5,6-dihydrophenanthridine was formed. This suggests that adsorption on the catalyst via the nitrogen atom is possible, but that steric inhibition to the combination of the activated species is involved. The same effect could be responsible for the exclusive formation of 5,5 -disubstituted 2,2 -dipyridines from 3-substi-tuted pyridines, as well as for the low yields of 3,3, 5,5 -tetramethyl-2,2 -bipyridines obtained from 3,5-lutidine and of 3,3 -dimethyl-2,2 -... 

Q Preparation of 2-Acetyi-3-Methyi-5-(2-Oxo-2,5-Dihydro-4-Furyi)Benzo[b]Furan (3556 CB) (1) A suspension of 2 grams of the compound prepared according to (B) in 20 ml of concentrated hydrochloric acid, is heated to about 50°C, just until it dissolves. Thereafter it is heated for 2 minutes to 70°C, just until precipitation commences. The mixture is allowed to cool, diluted with water, filtered, the residue washed, dried, and sublimed at 200°C and 0.1 mm pressure, 1.4 grams of product (Yield 70%) Is obtained, MPc = 218°-221°C. A second sublimation produces a chemically pure product, MP = 221°-222°C. 

B) Preparation of 7-Chloro-3-Methoxycarbony/-5-Phenyl-2-0xo-2,3-Dihydro-iH-Benzo [fl-1,4-Diazepine (4347 CB) A solution of 9.2 g (0.04 mol) of compound 4356 CB in 20 ml of methanol is added dropwise, in the course of one hour and 30 minutes, to a boiling solution of 9.2 g (0.05 mol) of the hydrochloride of methyl aminomalonate in 30 ml of methanol. When this is completed, heating under reflux is continued for 30 minutes and the product then concentrated to dryness under reduced pressure. The residue is taken up in water and ether, the ethereal layer separated, the product washed with water and dried over sodium sulfate. The solvent is evaporated under reduced pressure. The residue, which consists of the methyl ester, could not be obtained in the crystalline state. It is dissolved in 25 ml of acetic acid, heated under reflux for 15 minutes, the product evaporated to dryness and the residual oil taken up in ether. A colorless solid separates which... 

Removal of the solvent gave an oil which was taken up In ether and filtered through a pad of Woelm grade I alumina. The eluent was concentrated and the residue was crystallized from methylene chloride/hexane yielding 1-methyl-7-nitro-5-(2-fluorophenyl)-3H-1,4-benzo-diazepin-2(1 H)-one as pale yellow needles melting at 166° to 167°C. 

B) Preparation of 7-Chloro-1,2,3,4-Tetrahydro-1-Methyl-6H-1,4-Bemodiazepin-5-one A mixture of 25.25 g (0.1 mol) of 4-acetyl-7-chloro-1,2,3,4-tetrahydro-1-methyl-5H-1,4-benzo-diazepin-5-one, 33.3 ml (0.1 mol) of 3 N sodium hydroxide and 350 ml of ethanol was heated under reflux for 15 minutes and then concentrated to dryness in vacuo. The residue was treated with 500 ml of water, collected and washed with ethanol to give 20.2 g... 

Benzo-l,2,3-triazin-4-ones with the general structure 6.54 (X = O, S, or H2) are obtained by diazotization of the appropriate aniline derivatives 6.53 (Scheme 6-38). In polar aprotic solvents (e. g., nitrobenzene) the reverse reaction takes place to give the diazonium ion (for an example see Kullick, 1966). Diazotization of 1,8-diamino-naphthalene yields l-i/-naphthol[l,8-cfe]triazine (6.55 Tavs et al., 1967). In concentrated HC1 the triazine ring is opened again. 

Hydrogen iodide has also been used as a catalyst for hydrogen exchange581, rate coefficients (lO7 ) at 25 °C for reaction with [2H]C6H4R being (R =) 2,3-benzo(l position of naphthalene), 500 4-Me, 40 2-Me, 21 4-Ph, 42 2-Ph, 10. The reaction was catalysed by added iodine, the rate being directly proportional to the concentration of this, and for the latter compound rates were measured... 

Combustion of wood or paper treated with pentachlorophenol resulted in no increase and more probably a decrease in octachlorodi-benzo-p-dioxin concentrations while octachlorodibenzo-p-dioxin increased slightly in paper treated with sodium pentachlorophenate. The pho-tolytic degradation of sodium pentachlorophenate at pH 8 is very rapid. Under these controlled conditions formation of no more than 0.03% octachlorodibenzo-p-dioxin was observed. The 2,3,7,8 isomer, one of the most active chloracnegens is seemingly stable towards air oxidation but... 

BCR Analytical Approach for the Certification of PAHs in Natural Matrix CRMs Prior to the certification analyses for the CRM, each participating laboratory has to prepare standard solutions of the analytes to be determined from certified reference compounds (purity >99.0 %) to calibrate their instruments for response and response linearity (multiple point calibration), detection limit, and reproducibility. In the case of PAH measurements, reference compounds of certified purity are used as internal standards, which are not present at a detectable concentration in the matrix to be analyzed (e.g. indeno[i,2,3-cd]fluoranthene (CRM 267), 5-methylchrysene (CRM 081R), benzo[f ]chry-sene (CRM 046), picene (CRM 168), and/or phenanthrene-dio). 

Each plant tissue tends to have an obviously distinctive profile of flavonoids. The flavonoid content can reach about 0.5% in pollen, 10% in propolis, and about 6 mg/kg in honey. Havonoid aglycones appear to be present only in propolis and honey, while pollen contains flavanols in herosidic forms. The flavonoids in honey and propolis have been identified as flavanones and flavanones/flavanols (Campos et ah, 1990). The antimi-crobially active flavanone pinocembrine was foimd to be a major flavonoid in honey (Bogdanov, 1989). Amiot et ah (1989) studied two blossom and two honeydew Swiss honey samples and foimd that pinocembrine was the main flavonoid. Pinocembrine concentration varied between 2 and 3 mg/kg (Bogdanov, 1989). Berahia et ah (1993) analyzed sunflower honey samples and detected six flavone/flavols, four flavanone/ flavols, and pinocembrin, of which pinocembrin is the main flavonoid. The flavonoids in sunflower honey and propolis were characterized and assessed for their effects on hepatic drug-metabolizing enzymes and benzo [fl]pyrene-DNA adduct formation (Sabatier et ah, 1992 Siess et ah, 1996). 

Charge transfer reactions at ITIES include both ET reactions and ion transfer (IT) reactions. One question that may be addressed by nonlinear optics is the problem of the surface excess concentration during the IT reaction. Preliminary experiments have been reported for the IT reaction of sodium assisted by the crown ether ligand 4-nitro-benzo-15-crown-5 [104]. In the absence of sodium, the adsorption from the organic phase and the reorientation of the neutral crown ether at the interface has been observed. In the presence of the sodium ion, the problem is complicated by the complex formation between the crown ether and sodium. The SH response observed as a function of the applied potential clearly exhibited features related to the different steps in the mechanisms of the assisted ion transfer reaction although a clear relationship is difficult to establish as the ion transfer itself may be convoluted with monolayer rearrangements like reorientation. 

If the photoequilibrium concentrations of the cis and trans isomers of the photoswitchable ionophore in the membrane bulk and their complexation stability constants for primary cations are known, the photoinduced change in the concentration of the complex cation in the membrane bulk can be estimated. If the same amount of change is assumed to occur for the concentration of the complex cation at the very surface of the membrane, the photoinduced change in the phase boundary potential may be correlated quantitatively to the amount of the primary cation permeated to or released from the membrane side of the interface under otherwise identical conditions. In such a manner, this type of photoswitchable ionophore may serve as a molecular probe to quantitatively correlate between the photoinduced changes in the phase boundary potential and the number of the primary cations permselectively extracted into the membrane side of the interface. Highly lipophilic derivatives of azobis(benzo-15-crown-5), 1 and 2, as well as reference compound 3 were used for this purpose (see Fig. 9 for the structures) [43]. Compared to azobenzene-modified crown ethers reported earlier [39 2], more distinct structural difference between the cis... 

Hemoglobin is another heme-containing protein, which has been shown to be active towards PAH, oxidation in presence of peroxide [420], This protein was also modified via PEG and methyl esterification to obtain a more hydrophobic protein with altered activity and substrate specificity. The modified protein had four times the catalytic efficiency than that of the unmodified protein for pyrene oxidation. Several PAHs were also oxidized including acenaphthene, anthracene, azulene, benzo(a)pyrene, fluoranthene, fluorene, and phenanthrene however, no reaction was observed with chrysene and biphenyl. Modification of hemoglobin with p-nitrophenol and p-aminophenol has also been reported [425], The modification was reported to enhance the substrate affinity up to 30 times. Additionally, the solvent concentration at which the enzyme showed maximum activity was also higher. Both the effects were attributed to the increase in hydrophobicity of the active site. 

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