Reduction quinoline

The concept for the reduction of quinolines was successfully transferred to pyridine substrates by Rueping and Antonchick. It is important to point out that in contrast to the quinoline reduction, only few asymmetric methods to reduce pyridine derivatives are known. Hence, this method is a very valuable synthetic tool. 

The stock solution of quinoline-sulphur poison is prepared by refluxing I g. of sulphur with 6 g. of quinoline for 5 hours and diluting the resulting brown liquid to 70 nJ. with xylene which has been purified by distilling over anhydrous aluminium chloride. The addition of the quinoline - sulphur poison ensures that the reduction does not proceed beyond the aldehyde stage it merely slows up the reaction and has no harmful effects. 

Reduction. Quinoline may be reduced rather selectively, depending on the reaction conditions. Raney nickel at 70—100°C and 6—7 MPa (60—70 atm) results in a 70% yield of 1,2,3,4-tetrahydroquinoline (32). Temperatures of 210—270°C produce only a slightly lower yield of decahydroquinoline [2051-28-7]. Catalytic reduction with platinum oxide in strongly acidic solution at ambient temperature and moderate pressure also gives a 70% yield of 5,6,7,8-tetrahydroquinoline [10500-57-9] (33). Further reduction of this material with sodium—ethanol produces 90% of /ra/ j -decahydroquinoline [767-92-0] (34). Reductions of the quinoline heterocycHc ring accompanied by alkylation have been reported (35). Yields vary widely sodium borohydride—acetic acid gives 17% of l,2,3,4-tetrahydro-l-(trifluoromethyl)quinoline [57928-03-7] and 79% of 1,2,3,4-tetrahydro-l-isopropylquinoline [21863-25-2]. This latter compound is obtained in the presence of acetone the use of cyanoborohydride reduces the pyridine ring without alkylation. 

FrielA,nderSynthesis. The methods cited thus far all suffer from the mixtures which usually result with meta-substituted anilines. The use of an ortho-disubstituted benzene for the subsequent constmction of the quinoline avoids the problem. In the FrieWider synthesis (52) a starting material like 2-aminoben2aldehyde reacts with an CX-methyleneketone ia the presence of base. The difficulty of preparing the required anilines is a limitation ia this approach, but 2-nitrocarbonyl compounds and the subsequent reduction of the nitro group present a usehil modification (53). 

Mesophase formation in coal-tar pitch is encouraged by a reduction of the natural quinoline-insoluble matter content, which resembles carbon black but is not optically anisotropic and is characterized by an atomic carbon hydrogen ratio of 4 1. In contrast, the atomic carbon hydrogen ratio of mesophase is about 2 1. 

The catalyst commonly used in this method is 5 wt % palladium supported on barium sulfate inhibited with quinoline—sulfur, thiourea, or thiophene to prevent reduction of the product aldehyde. A procedure is found in the Hterature (57). Suitable solvents are toluene, benzene, and xylene used under reflux conditions. Interestingly, it is now thought that Rosenmund s method (59) originally was successful because of the presence of sulfur compounds in the xylene used, since the need for an inhibitor to reduce catalyst activity was not described until three years later (60). 

The synthesis of meconin has been referred to already (p. 201). Cotarnine has been synthesised by Salway from myristicin (I) as a starting-point. This was transformed into jS-3-methoxy-4 5-methylenedioxy-phenylpropionic acid (II), the amide of which was converted by Hofmann s reaction into )S-3-methoxy-4 5-methylenedioxyphenylethylamine, and the phenylacetyl derivative (HI) of this condensed, by heating it in xylene solution with phosphoric oxide, giving rise to the two possible dihydroiso-quinoline derivatives. The first of these substances, 8-methoxy-6 7-methylenedipxy-1-benzyl-3 4-dihydroiioquinoline (IV), on conversion into the methochloride and reduction with tin and hydrochloric acid, gave... 

Ewins has synthesised both substances from m-methoxybenzoic acid, which on nitration gave 2-nitro-3-methoxybenzoic acid, and this, on reduction and treatment with methyl iodide, yielded damasceninic acid, which, by esterification with methyl alcohol, furnished damascenine. Kaufmann and Rothlen found that the additive product of 8-methoxy-quinoline and methyl sulphate, on oxidation with permanganate, yields formyldamasceninic acid, MeO. CgH3(NMe. CHO). COOH, which can be transformed into damasceninic acid by warming with dilute hydrochloric acid. ... 

Other secondary amines such as pyrrolidine, di- -butylamine, tetrahydro-quinoline, n-benzylamine, and piperidine were also found to be capable of effecting this reduction. Interestingly, morpholine does not reduce enamines as readily (47) and its acid-catalyzed reaction with norbornanone was reported (45) to give only the corresponding enamine (93), although trace amounts of the reduction product were detected when cyclohexanone was treated with morpholine under these conditions (47a). The yield of morpholine reduction product was increased by using higher temperatures. 

Alteration of the relative reactivity of the ring-positions of quinoline is expected and observed when cyclic transition states can intervene. Quinoline plus phenylmagnesium bromide (Et20,150°, 3 hr) produces the 2-phenyl derivative (66% yield) phenyllithium gives predominantly the same product along with a little of the 4-phenylation product. Reaction of butyllithium (Et 0, —35°, 15 min) forms 2-butylquinoline directly in 94% yield. 2-Aryl- or 6-methoxy-quinolines give addition at the 2-position with aryllithium re-agents, and reaction there is so favored that appreciable substitution (35%) takes place at the 2-position even in the 4-chloroquinoline 414. Hydride reduction at the 2-position of quinoline predominates. Reaction of amide ion at the 2-position via a cyclic... 

Bromoisoquinoline can be aminated under vigorous conditions (concentrated NH4OH, 165°, 16 hr), - but attempted methoxyla-tion (methanolic methoxide, 235°, 7 hr) gave isoquinoline (50% yield) via the reductive reaction observed with 6- and 8-bromo-quinoline. ... 

Trimethyloxazolo[4,5-/]quinoline prepared from 2,7-dimethyl-6-methoxyquinoline using nitration, demethylation (or reversed), reduction, and cy-clization with acetic anhydride confirms unambigously the structure of the aromatic part of the antibiotic X-537A after nitration and alkaline degradation (71JOC3621). 

Subs tituted-1,2,3-oxadiazolo[4,5-/]quinoline 47 originated after nitration, reduction, and diazotization of alkaloid quinine during the study of its stmcture and reactions (53RZC495, 54RZC61). 

The 6-methylacetylamino-l,2,3,4-tetrahydroquinoline, after nitration and separation of isomers, following reduction and deprotection, gave the 7-amino-6-methylamino derivative, which cyclized with cyanogen bromide. Alkylation of the cyclization products afforded inhibitors of thymidylate synthase, 5-substituted 2-amino-l//-l-methyl-5,6,7,8-tetrahydroimidazo[4,5-g]quinolines 136, designed for use in iterative protein crystal analysis (Scheme 42) (92JMC847). 

Triazolo[4,5-/i]quinoline 143 and triazolo[4,5-/i]quinoline-5-arsonic acid 144 were isolated from mother liquors after reduction and bis-diazotization of 5,7-dinitro-8-(4-toluenesulfone)aminoquinoline in the presence of cupric sulfate with trisodium arsenite (32JCS2196). 

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