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Pyrimidines ring synthesis

A major type of reaction in this class is the cyclization of 4-amino- or 4-halo-pyrimidines carrying 5-cyanoethyl or 5-ethoxycarbonylethyl groups, which cyclize to 7-amino or 7-oxo derivatives of 5,6-dihydropyrido[2,3- f]pyrimidine, e.g. (131)->(63). The intermediates may sometimes be prepared by reaction of 4(6)-aminopyrimidines with acrylonitrile, or even via a pyrimidine ring synthesis from an amidine and a cyanoacetic ester or malononitrile derivative, e.g. (132) -> (133) (7lJOC2 85, 72BCJ1127). [Pg.217]

The answer is a. (Murray, pp 375-401. Scriver, pp 2513-2570. Sack, pp 121-138. Wilson, pp 287-320.) During purine ring biosynthesis, the amino acid glycine is completely incorporated to provide C4, C5, and N7. Glutamine contributes N3 and N9, aspartate provides Nl, and derivatives of tetrahydrofolate furnish C2 and C8. Carbon dioxide is the source of C6. In pyrimidine ring synthesis, C2 and N3 are derived from carbamoyl phosphate, while Nl, C4, C5, and C6 come from aspartate. [Pg.236]

The most general pyrimidine ring synthesis involves the combination of a 1,3-dicarbonyl component with an N-C-N fragment snch as a urea, an amidine or a guanidine. [Pg.275]

Potassium hypobromite Pyrimidine ring synthesis s. 2, 468 KOBr O... [Pg.390]

A variation of this procedure is used for sulfisomidine because of the different character of the amino group in the 4-position of a pyrimidine ring. Two moles of the sulfonyl chloride are condensed with one mole of 4-amino-2,6-dimethy1pyrimidine in the presence of triethylamine. The resulting bis(acetylsulfanilyl) derivative is readily hydrolyzed to the product. The formation of the bis(acetylsulfanilyl) derivative has also been employed for other heterocycHc amines, eg, for synthesis of sulfathiazole and sulfamoxole (44), but the 1 1 reaction is probably preferable. [Pg.468]

In many pyrimidine ring syntheses, it is possible or even desirable to isolate an intermediate ripe for ring-closure by the formation of just one bond. For example, ethyl 3-aminocrotonate (502) reacts with methyl isocyanate to give the ureido ester (503) which may be isolated and subsequently converted into 3,6-dimethyluracil (504) by the completion of one bond. However, viewed pragmatically, the whole synthesis involves the formation of two bonds and therefore is so classified. On such criteria, only two pyrimidine/quinazoline syntheses involve the formation of only one bond. [Pg.106]

Examination of the pyrazino[2,3-rf]pyrimidine structure of pteridines reveals two principal pathways for the synthesis of this ring system, namely fusion of a pyrazine ring to a pyrimidine derivative, and annelation of a pyrimidine ring to a suitably substituted pyrazine derivative (equation 76). Since pyrimidines are more easily accessible the former pathway is of major importance. Less important methods include degradations of more complex substances and ring transformations of structurally related bicyclic nitrogen heterocycles. [Pg.309]

For the preparation of triazolopyrimidines three main types of synthesis are in use. The first of these proceeds from a pyrimidine derivative (especially the 4,5-diamino derivatives) and closes the triazole ring. The second method proceeds, on the contrary, from derivatives of u-triazole to close the pyrimidine ring. The third method finally is one which yields the derivatives through substitution or replacement of substituents in compounds prepared by one of the first-named procedures. [Pg.239]

A combination of the preceding type of synthesis and of cyclization of 4-amino-5-arylazopyrimidine can be seen in the novel procedure of Richter and Taylor. Proceeding from phenylazomalonamide-amidine hydrochloride (180), they actually close both rings in this synthesis. The pyrimidine ring (183) is closed by formamide, the triazole (181) one by oxidative cyclization in the presence of cupric sulfate. Both possible sequences of cyclization were used. The synthetic possibilities of this procedure follow from the combination of the two parts. The synthesis was used for 7-substituted 2-phenyl-l,2,3-triazolo[4,5-d]-pyrimidines (184, 185). An analogous procedure was employed to prepare the 7-amino derivatives (188) from phenylazomalondiamidine (186). [Pg.246]

Of greater versatility is an extension of Albert and Royer s acridine synthesis. The first successful use of this in the quinazoline series was for the removal of the chlorine atom in 2-chloro-4-phenylquin-azoline, although it had been used previously to prepare 8-nitro-6-methoxyquinazoline in very poor yield. The 4-chloroquinazoline is converted to its 4-(A -toluene-p-sulfonylhydrazino) quinazoline hydrochloride derivative which is decomposed with alkali in aqueous ethylene glycol at lOO C (Scheme 13). The yields are high (60-70%) when R is Me, Cl, OMe but low when R is NO2, and in the latter case it is preferable to use dilute sodium carbonate as the base. This reaction is unsatisfactory if the unsubstituted pyrimidine ring is unstable towards alkali, as in 1,3,8-triazanaphthalene where the pyrimi-... [Pg.299]

This is the first synthesis of pyrido[2,3-d]pyrimidines in which both nitrogen atoms of the pyrimidine ring have been supplied by the reagent. In view of the success of similar syntheses of pyrido[4,3-d]-pyrimidines this route would appear to be capable of wide extension. [Pg.159]

B. Synthesis by Annulation of the Pyrimidine Ring ONTO A 1,2,4-Triazole Structure... [Pg.354]

C. Synthesis by Concurrent Formation of Both of THE 1,2,4-Triazole and Pyrimidine Rings... [Pg.359]

Replacement of heterocyclic rings in nucleosides by ring systems which do not occur in nature represents another approach to compounds which may have activity against viral and neoplastic diseases. One of the early successes in this category involves replacement of a pyrimidine ring by a triazine. The synthesis starts with a now classical glycosidation of a heterocycle as its silylated derivative (146) with a protected halosugar (145), in this case a derivative of arabinose... [Pg.121]

The pyrimidine ring is formed from [4+2] atom fragments in the synthesis of 114 from 3-chloro-6-arylpyridazine 113 and anthranilic ester <2000HC0147> or acid <2001RRC649, 2003MOL322> (Equation 13). [Pg.273]

Synthesis of the annulated thicno[3, 2 5,6]pyndo[4,3-z/]pynmidinoncs 74 and 75 involves the formation of the outer six-membered (pyrimidine) ring via a carbodiimide (Scheme 23) <2006HCA1337>. [Pg.876]

Formation of the outer pyrimidine ring, by a different route, is also the final step in the synthesis of the benzothi-azolopyrimidopyrimidine 264 (Equation 82) <1997JIC818>, and similarly the outer six-membered ring is formed in the final step which leads to the thiadiazole-fused compounds 265 and 266 (Scheme 64) <1995RCB1957,1999RCB364>. [Pg.908]

See other pages where Pyrimidines ring synthesis is mentioned: [Pg.467]    [Pg.973]    [Pg.106]    [Pg.136]    [Pg.618]    [Pg.772]    [Pg.80]    [Pg.183]    [Pg.467]    [Pg.973]    [Pg.106]    [Pg.136]    [Pg.618]    [Pg.772]    [Pg.80]    [Pg.183]    [Pg.57]    [Pg.80]    [Pg.106]    [Pg.304]    [Pg.242]    [Pg.167]    [Pg.291]    [Pg.344]    [Pg.345]    [Pg.62]    [Pg.262]    [Pg.16]    [Pg.560]    [Pg.271]    [Pg.277]   


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