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Search for "cyclic sulfate" in Full Text gives 7 result(s) in Beilstein Journal of Organic Chemistry.
Stereoselective syntheses of 3-aminocyclooctanetriols and halocyclooctanetriols
Beilstein J. Org. Chem. 2021, 17, 705–710, doi:10.3762/bjoc.17.59
- the corresponding cyclic sulfate via the formation of a cyclic sulfite in the presence of catalytic RuO4. The reaction of this cyclic sulfate with a nucleophilic azide followed by the reduction of the azide group provided the target, 3-aminocyclooctanetriol. The second key compound, bromotriol, was
- stereospecifically new chlorocyclooctanetriols. Keywords: aminocyclitols; aminocyclooctanetriol; chlorocyclooctanetriol; cyclic sulfate; cyclitols; Introduction The synthesis of aminocyclitols has attracted attention because they contain substructures of many biologically active natural products [1][2][3]. They
- with sodium azide of the corresponding cyclic sulfate intermediate 9, which contains the only stereocentre. The cyclic sulfate 9 could be synthesized from diacetatediol 7 [33]. For this purpose, the reduction of the endoperoxide 5 with zinc followed by acetylation of the hydroxy group and OsO4/NMO
Vicinal difluorination as a C=C surrogate: an analog of piperine with enhanced solubility, photostability, and acetylcholinesterase inhibitory activity
Beilstein J. Org. Chem. 2020, 16, 2663–2670, doi:10.3762/bjoc.16.216
- ] was protected as the benzyl ether then subjected to a Sharpless asymmetric dihydroxylation reaction to furnish the diol 8 in modest yield. The diol 8 was then converted into the cyclic sulfate 9, which was ring-opened using TBAF to furnish the fluorohydrin 10. A Mosher ester analysis of the
- moiety throughout (Scheme 3). Thus, the α,β-unsaturated ester 15 [25] was carried through a similar sequence to that previously described, i.e., dihydroxylation, cyclic sulfate formation, ring-opening with TBAF (although note the regioselectivity [31]), deoxyfluorination, and deprotection to deliver the
The use of 4,4,4-trifluorothreonine to stabilize extended peptide structures and mimic β-strands
Beilstein J. Org. Chem. 2017, 13, 2842–2853, doi:10.3762/bjoc.13.276
- ] from propargylic alcohol in ten steps, based on the trifluoromethylation key step of 1-(((E)-3-bromoallyloxy)methyl)benzene to obtain (E)-1-benzyloxy-4,4,4-trifluoro-2-butene. The sequence then involved Sharpless asymmetric dihydroxylation, nucleophilic opening of cyclic sulfate with NaN3, palladium
Multigramme synthesis and asymmetric dihydroxylation of a 4-fluorobut-2E-enoate
Beilstein J. Org. Chem. 2013, 9, 2660–2668, doi:10.3762/bjoc.9.301
- the method, but for molecules of this type, it appears highly effective. To make our route stereodivergent, we sought access to the two anti diastereoisomers 35a and 35b via cyclic sulfate methodology (Scheme 7) [36][37]. Cyclic sulfate 32b was prepared via literature procedures [36][37], monitoring
- the steps closely by 19F{1H} NMR spectroscopy which distinguishes all the species effectively. In 32b, C-3 is primed for regioselective nucleophilic attack [38]. Crude cyclic sulfate 32b was taken up in acetone, treated with solid ammonium benzoate and allowed to stir at room temperature overnight
- . Nucleophilic ring opening reactions were performed on the crude cyclic sulfate mixtures because avoiding column chromatography at this stage led to a vast improvement in the overall yields. After ring opening, sulfate ester cleavage was achieved by stirring the concentrated residue in acid (20% H2SO4) and
Synthesis and ring openings of cinnamate-derived N-unfunctionalised aziridines
Beilstein J. Org. Chem. 2012, 8, 1747–1752, doi:10.3762/bjoc.8.199
- dihydroxylation, conversion to a cyclic sulfate, ring opening with azide, and finally ring closure to afford the NH-aziridine [18]. We recently reported [21][22] a nucleophilic aziridination methodology [23][24][25][26][27][28][29][30] that allows access to NH-aziridines in a single step from α,β-unsaturated
Metathesis access to monocyclic iminocyclitol-based therapeutic agents
Beilstein J. Org. Chem. 2011, 7, 699–716, doi:10.3762/bjoc.7.81
- obtained after artful manipulation of routine protocols (diastereoselective dihydroxylation and protection/deprotection). To access 1-deoxyaltronojirimycin (65) and 1-deoxyidonojirimycin (93), introduction of an additional step involving a cyclic sulfate was necessary. A similar methodology was used by Han
- ring closure (89%) under milder conditions (CH2Cl2): all attempts to employ the 1st-generation Grubbs catalyst 2 in RCM failed, supposedly because of an unfavourable steric environment during generation of the Ru–carbene species from 109, as compared to 98 (distinct N-protective groups). Cyclic sulfate
Synthesis and glycosidase inhibitory activity of new hexa- substituted C8-glycomimetics
Beilstein J. Org. Chem. 2005, 1, No. 12, doi:10.1186/1860-5397-1-12
- enzymes. The synthesis of these new C8-glycomimetics is described from enantiomerically pure C2-symmetrical polyhydroxylated cyclooctenes. Their obtention notably involved a syn-dihydroxylation, and more extended functionalization through formation of a cis-cyclic sulfate followed by amination and
- subsequent reductive amination. This strategy involving the nucleophilic opening of a cis-cyclic sulfate by sodium azide is to our knowledge the first example in C8-series. It revealead to be an efficient alternative to the nucleoplilic opening of an epoxide moiety which proved unsuccessful in this
- side of the bulky TBDMS group in β-position. However, it has to be pointed out that more hindered nucleophiles, such as primary amines, revealed unable to open the cyclic sulfate 9 or 10. The absolute configurations of 11 and 12 were established by NMR studies. 1H signals were assigned (Table 1) using
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