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Inhibitory group

Formation of an 11-methoxybenzyl ether occurs in satisfactory yield during the preparation of a 17,21 -benzylidene derivative [e.ff., (26)]. The usefulness of this ether and of related mixed acetals in removing the inhibitory effect of the 11 j5-hydroxyl group on the 20-ketone reduction has been reported. ... [Pg.404]

The tjipanazoles (18, 19a-d, 20a-b) a group of A-glycosides of indolo-[2,3-a]carbazole, have been isolated from the moderately antifungal extract of the blue-green alga Tolypothrix tjipanasensis. These alkaloids do not exhibit antitumor or protein kinase C (PKC) inhibitory activity, which is in contrast with the... [Pg.5]

Philleo et al. (29) recently confirmed the inhibitory action of methylene dioxyphenyl groups on biological oxidations in insects, including epoxidation and hydroxylation of certain compounds. [Pg.52]

Coumarin, the lactone of o-hydroxycinnamic acid, and some of its derivatives have been isolated from many plant species 31). Thimann and Bonner 141) attributed the growth-inhibiting effects of coumarin to its action on enzyme sulfhydryl groups. Inhibitory effects of coumarin on Avena coleoptiles and pea stem sections could be overcome by 2,3-dimercaptopropanol (BAL). Coumarin has also been reported to disrupt mitosis 29,30). [Pg.130]

Leaves of Eucalyptus rostrata were shown to contain substances that inhibited growth and germination (90). Four active fractions were obtained from the crude leaf extract. Inhibitory constituents were shown to contain a carbonyl group and a carbon-carbon double... [Pg.135]

Cordes et al995 carried out alkaline hydrolyses of p-nitrophenylhexanoate 55 (PNPH) in the presence of poly-4-vinylpyridine partially quaternized with dodecyl-bromide and ethylbromide (QPVP). They also found that the polyelectrolytes are increasingly effective as catalysts with an increasing ratio of dodecyl to ethyl groups, and the hydrophobic interactions are important in determining the catalytic efficiency. They observed the inhibitory effects of several gegen-anions fluoride ions are the weakest inhibitor, and nitrate is the strongest (F- < Cl < S04 [Pg.159]

Table 3). For example, arabinose and xylose differ from ribose only in the orientation of the 2 - and 3 -OH groups yet exhibit markedly different potencies. Whereas 9-(tetrahydrofuryl)-Ade ( SQ 22,536) and 9-(cyclopentyl)-Ade are without hydroxyl groups and are less potent, they offer metabolic and biochemical stability useful for many types of studies. It is, however, the removal of two of the hydroxyl groups, that elicits the largest improvement in inhibitory potency, in particular the 2, 5 -dideoxy- modification (Table 3). With these improvements in potency, these cell permeable compounds, in particular 2, 5 -dd-Ado, have become useful research tools and have been used to inhibit adenylyl cyclases and to lower cAMP levels and alter function in numerous studies in isolated cells or intact tissues. [Pg.34]

Although the 3 - and 5 -polyphosphate derivatives mentioned above exhibit exquisite inhibitory potency these compounds are not cell permeable. To take advantage ofthepotency of such derivatives for studies with intact cells and tissues, there are two possibilities. One is chemically to protect the phosphate groups from exonucleotidases that also allows the compound to transit the membrane intact. The other is to provide a precursor molecule that is cell permeable and is then metabolized into an inhibitor by intracellular enzymes. The general term for such a compound is prodrug nucleotide precursors are also referred to as pronucleotides. Families of protected monophosphate derivatives were synthesized, based on (3-L- and 3-D-2, 5 -dd-3 -AMP, 3-L-2, 3 -dd-5 -AMP, and the acyclic 9-substituted adenines, PMEA and PMPA. Protective substituents were (i) -( -pivaloyl-2-thioethyl) ... [Pg.36]

Ribosomal Protein Synthesis Inhibitors. Figure 3 The chemical structure of tetracycline and possible interactions with 16S rRNA in the primary binding site. Arrows with numbers indicate distances (in A) between functional groups. There are no interactions obseived between the upper portion of the molecule and 16S rRNA consistent with data that these positions can be modified without affecting inhibitory action (from Brodersen et al. [4] with copynght permission). [Pg.1088]

See other pages where Inhibitory group is mentioned: [Pg.381]    [Pg.309]    [Pg.178]    [Pg.381]    [Pg.309]    [Pg.178]    [Pg.105]    [Pg.452]    [Pg.481]    [Pg.404]    [Pg.47]    [Pg.48]    [Pg.131]    [Pg.136]    [Pg.325]    [Pg.327]    [Pg.327]    [Pg.124]    [Pg.75]    [Pg.312]    [Pg.550]    [Pg.336]    [Pg.447]    [Pg.146]    [Pg.96]    [Pg.122]    [Pg.282]    [Pg.39]    [Pg.386]    [Pg.118]    [Pg.139]    [Pg.34]    [Pg.332]    [Pg.428]    [Pg.555]    [Pg.760]    [Pg.790]    [Pg.806]    [Pg.1088]    [Pg.1136]    [Pg.1139]    [Pg.1165]    [Pg.1295]    [Pg.530]   
See also in sourсe #XX -- [ Pg.207 ]



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