5-Amino-1-dimethylamino

Disregarding nonoxygen functional groups (amino, dimethylamino, and so on) only the 2,3,6-trideoxyhexoses were isolated from natural products. However, some of the isomeric trideoxyhexoses were chemically synthesized. Thus, the methyl a-glycosides of 3,4,6 - tr i de o xy - d - erj> f/ ro - he x o p y r a n o s e, 3,4,6-tri-deoxy-D-t/zreo-hexopyranose and 2,4,6-trideoxy-D-eryt/iro-hexopyranose were synthesized from methyl 4,6-dideoxy-a-D-xy/o-hexopyranoside via selective sub-... 

Bis-[dimethyl-hydro-silyl]-amino)-dimethylamino-phenyl- XIII/3b, 287... 

In normal-phase chromatography (NPC), the stationary phase is polar. A nonpolar mobile phase is used, such as n-hexane, methylene chloride, or chloroform. The stationary phase is a bonded siloxane with a polar functional group (polarity order cyano < diol < amino < dimethylamino). These phases retain polar compounds in preference to nonpolar compounds. 

The materials introduced initially, and still used most often, were silicas with apolar long chain alkylgroups (e.g., octadecylsilyl (ODS) groups) chemically bonded to the surface. Thus, the materials were intended for reversed phase chromatography (cf.. Fig. 4.4.7). Since then various materials have been introduced with bonded short chains carrying polar groups, e.g., nitril, amino, dimethylamino, dihydroxy, nitro. 

End groups include amino, dimethylamino, piperazine, carboxyl, ethylene oxide, and hydroxymethylene (Table 8). 

The preparation of twenty 1,3-dioxan derivatives with a 5-phenyl group and a nitro-, amino-, dimethylamino-, or piperidino-group also in position 5 has been reported. ... 

Efficiency data summarized in Table 9-8 (Telegdi et al., 1999) point to the importance of a double bond close to the phenyl ring. These chemicals exhibit increasing efficiency. The presence of nitrogen as a substituent (amino, dimethylamino, nitro groups)... 

This preparation illustrates the use of dimethyl sulphate to convert a primary amino group into the secondary monomethylamino group, without the methy-lation proceeding to the tertiary dimethylamino stage. The methylation of anthranilic acid is arrested at the monomethylamino stage by using i-i molecular equiN alents of sodium hydroxide and of dimethyl sulphate. The reactions can be considered as ... 

As improvements over P-methylumbeUiferone (55—57), 4-methyl-7-amino-coumarin [26093-31-2] (12a) and 7-dimethylamino-4-methylcoumarin [87-014] (12b) (58—61) were proposed. These compounds are used for brightening wool and nylon either in soap powders or detergents, or as salts under acid dyeing conditions. They are obtained by the Pechmaim synthesis from appropriately substituted phenols and P-ketocarboxyflc acid esters or nitriles in the presence of Lewis acid catalysts (see Coumarin). 

Many members of this series are known based on nitroparaffin condensations with aldehydes of longer chain length than formaldehyde. However, only the five primary amino alcohols discussed in the following are manufactured on a commercially significant scale. N-Substituted derivatives of these compounds also have been prepared, but only 2-dimethylamino-2-methy1-1-propanol has been available in commercial quantities (Table 1). 

The amino group is readily dia2oti2ed in aqueous solution, and this reaction forms a basis for the assay of sulfas. Aldehydes also react to form anils, and the yellow product formed with 4-(dimethylamino)hen2a1dehyde can be used for detection in thiu-layer and paper chromatography. Chromatographic retention values have been deterrnined in a number of thiu layer systems, and have been used as an expression of the lipophilic character of sulfonamides (23). These values have corresponded well with Hansch lipophilic parameters determined in an isobutyl alcohol—water system. 

In principle, aminopyrazine and 2-aminoquinoxaline are capable of existing in the form of the imino tautomers (81) and (82) however, comparison of the UV spectra of the amino, methylamino and dimethylamino derivatives indicates that in both systems the amino rather than the imino tautomer is favored (60JCS242, 58JCS108). 

In the case of the 2-dimethylamino- (or 2-amino-)methylene derivatives, the products were at first thought to be pyrimido[4,5-c]isoquinolines (267), but later work with 6-(N-substituted amino)uracils assigned the structures of the products (268) as belonging to the isomeric pyrimido[4,5-f>]quinoline system (74CB2537), in agreement with the regioselection rules above. 

The basic piSTa values, which have to be considered as equilibrium values, including those of anhydrous and hydrated species, reveal a destabilizing inductive effect of the 6- and 7-methyl group towards 3,4-hydrate formation, as do also the 2-methylamino and 2-dimethylamino groups for additional steric reasons. If the cation of 2-aminopteridine did not add water its value would be about 1.6, arrived at by substracting from the piSTa 2.6 of the essentially anhydrous 2-amino-4,7-dimethylpteridine cation 0.3 for the 7- and 0.7 for the 4-methyl group. The difference between the observed value of 4.29 and the... 

Benzothiazole, 2-amino-6-thiocyanato-azo dyes from, 1, 328 Benzothiazole, 2-aryl-synthesis, 6, 321 Benzothiazole, 2-arylamino-synthesis, 6, 323 Benzothiazole, 2-aryloxy-Fries rearrangement, 6, 289 Benzothiazole, 2-benzyl-picrate, 6, 252 Benzothiazole, 2-chloro-dyes from, 1, 321-322 synthesis, 6, 323 Benzothiazole, 2,3-dihydro-oxidation, 6, 272 Benzothiazole, 2-dimethylamino-synthesis, 5, 128... 

Folic acid, 4-amino-4-deoxy-10-methyl-, 1, 164 3, 325 as anticancer drug, 1, 263 biological activity, 3, 325 Folic acid, 4-amino-10-methyl-toxicity, 1, 141 Folic acid, 7,8-dihydro-biosynthesis, 3, 320 synthesis, 1, 161, 3, 307 Folic acid, 4-dimethylamino-hydrolysis, 3, 294 Folic acid, 5-formiminotetrahydro-biological activity, 3, 325 Folic acid, 5-formyl-5,6,7,8-tetrahydro-biological activity, 3, 325 chirality, 3, 281 occurrence, 3, 325 Folic acid, 10-forfnyltetrahydro-biological activity, 3, 325 Folic acid, 5,10-methenyl-5,6,7,8-tetrahydro-biological activity, 3, 325 chirality, 3, 281 Folic acid, 5-methyl-chirality, 3, 281 Folic acid, 9-methyl-toxicity, 1, 141... 

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