Big Chemical Encyclopedia

Chemical substances, components, reactions, process design ...

Articles Figures Tables About

Fluoro group

One of the first indications that the antiinflammatory potency of the corticoids could be increased was the observation that incorporation of a 9a-fluoro group in hydrocortisone resulted in a tenfold increase in activity. Treatment of hydrocortisone acetate (170a) with phosphorus oxychloride in pyridine yields the corresponding olefin, 172. This, on being subjected to the reaction sequence depicted in the transformation of 104 to 108 (addition of HOBr, closure to the epoxide and ring opening with HF),... [Pg.191]

The potentiation obtained with 6a-fluoro group was found to be additive to that of the 16 hydroxy group, just as in the case of the corresponding methyl compounds. The synthesis of these agents relies on introduction of the corresponding hydroxyl group... [Pg.201]

The oxygen atom at 21 is similarly an expendable group. Reaction of 241 (obtained from 185 by the usual procedure for introduction of the 9a-fluoro group) with methanesulfonyl chloride affords the 21 mesylate (242a). Replacement of the leaving group at 21 with iodine by means of potassium iodide in acetone followed by reduction of the halogen with zinc in acetic acid leads to fluorometholone (243). ... [Pg.203]

Friedel-Crafts acylation of fluorobenzene with thiophene-l-carboxylic acid gives the ketone 7. Nitration proceeds ortho to the fluoro group to give the intermediate Nucleophilic displacement by means of... [Pg.176]

The synthesis of polyether quinoxaline by nucleophilic displacement discussed in Section 5.4.2.2 has also been used for the preparation of hyperbranched polyquinoxaline based on AB2 or A2B monomers. In the AB2 monomer the focal point is a single fluoro group (Fig. 5.42)172 in the A2B the focal point is a single... [Pg.312]

The 2 -chloro and 2 -bromo congeners of either 748 (FIAC) or 758 (FMAU) are more cytotoxic than FIAC and FMAU, suggesting that these chloro and bromo nucleosides, in contrast to the 2 -fluoro compounds, are comparatively better substrates for deoxycytidine kinase of human lymphocytes than the substrates for viral-specific thymidine kinase. The disposition of the 2 -fluoro group may also be important from the biological viewpoint. It should be noted that the structural difference between RNA and DNA is at the 2 -position. The ribo type of analog (738) of FIAC is 10 times less effective in suppression of HSV replication than is FIAC. Thus Fox, and Watanabe and coworkers concluded that the 2 - up fluorine disposition and the species of the substituent at C-5 are the two important factors influencing antiviral activity. Nevertheless, the mechanism of action of 2 -deoxy-2 -fluorocytidine (737) on certain herpes viruses, including HSV-1... [Pg.249]

This reaction is basically similar to [OS 1], but is expected to differ in reactivity owing to the I- and M-effects of the fluoro group. [Pg.419]

The 9-fluoro group of the pyrimido[l,6,5-, tf][l,4]benzoxazine 312 has been exchanged for an amino group upon reaction with primary amines <2001W02001/053273>. [Pg.302]

Although highly reactive, 2/7-azirines are of considerable synthetic interest and serve as a source of the 3-fluoro-4//-l, 3-diazepines 86. Reaction of 80 with difluorocarbene in the presence of furfural gave 86, rather than the expected furfural-derived products 83. Rearrangement of the initial 1,3-dipolar intermediate 81 to 84 and then cycloaddition of 84 with 80 are proposed as key steps in the reaction the intermediate cycloadduct 85 gave 86 on base-induced elimination of HF. Nucleophilic displacement of the fluoro group in 86 provided access to further substituted 1,3-diazepines <06TL639>. [Pg.449]

It was clear, from even a qualitative inspection of the data, that the presence of a methyl or fluoro group in the meta position had the effect of not only increasing activity versus the design insect, the southern armyworm, but also lead to dramatic increases in level of topical activity against other species. [Pg.308]

The nomenclature of the RP is not consequent. The RP most often used contains octyl (RP C8) or octadecyl (RP C18) groups. There is no differentiation even when two methyl groups are introduced additionally with the silane (as with monofunctional silanes) or only one (difunctional) or none (trifunctional silane). Some manufacturer use silanes with bulky side groups (e.g., isopropyl groups) to improve the hydrolytic stability of the bonded phases, but here also, only the longest alkyl group is used in nomenclature. RP C8 and RP C18 are the work horses in HPLC. Shorter chains (RP4) are used in protein separations, and special selectivity can be obtained with bonded phenyl, cyano, amino or fluoro groups. [Pg.53]

Here, the change in bond length (in A multiplied by 1000) is from Hartree-Fock 6-3IG calculations. Included are methyl and tert-butyl groups (both weak n donors), the cyano group (both a strong a and n acceptor), the methoxy and fluoro groups (both a acceptors and n donors) and the trimethylsilyl group (a a donor and n acceptor). [Pg.117]

See other pages where Fluoro group is mentioned: [Pg.2543]    [Pg.413]    [Pg.212]    [Pg.163]    [Pg.202]    [Pg.90]    [Pg.868]    [Pg.144]    [Pg.147]    [Pg.245]    [Pg.243]    [Pg.250]    [Pg.176]    [Pg.437]    [Pg.173]    [Pg.129]    [Pg.129]    [Pg.482]    [Pg.172]    [Pg.252]    [Pg.102]    [Pg.266]    [Pg.197]    [Pg.197]    [Pg.282]    [Pg.30]    [Pg.221]    [Pg.679]    [Pg.1225]    [Pg.1438]    [Pg.93]    [Pg.767]    [Pg.364]    [Pg.368]    [Pg.363]    [Pg.335]   
See also in sourсe #XX -- [ Pg.369 ]



SEARCH



© 2024 chempedia.info