Search results
Search for "epoxide" in Full Text gives 238 result(s) in Beilstein Journal of Organic Chemistry. Showing first 200.
One-pot synthesis of epoxides from benzyl alcohols and aldehydes
Beilstein J. Org. Chem. 2018, 14, 2308–2312, doi:10.3762/bjoc.14.205
- alcohols and aldehydes. Keywords: Corey–Chaykovsky; epoxide; heterocycle; one-pot; ylide; Introduction Epoxides have historically served as strategic functional groups in target-oriented synthesis [1][2][3][4]. Common examples of their utility include stereospecific ring opening [5][6][7], rearrangements
- (NaH) was the only base that successfully afforded the desired epoxide 3, typically in excellent and reproducible yields (other bases screened included KOt-Bu, LiHMDS, TBD [25], and KOH). Furthermore, diluting the reaction after formation of the sulfonium salt, and cooling it in an ice bath, proved
- at the betaine intermediate prior to epoxide formation through displacement of THT. This is supported by example 9 which contained a para-methoxy group at the aldehyde component but was isolated as a single diastereomer [28]. Functional groups that are not compatible with this method include phenols
Studies towards the synthesis of hyperireflexolide A
Beilstein J. Org. Chem. 2018, 14, 2106–2111, doi:10.3762/bjoc.14.185
- 5 could not only act as a surrogate for C-9 carbonyl but also facilitate installation of an angular methyl group. The retrosynthetic analysis for hyperireflexolide A is depicted in Scheme 1. We envisioned that hyperireflexolide A (1) could be synthesized by metal-catalyzed opening of the epoxide 2
- of the proposed synthetic sequence. Future studies will include the stereoselective epoxidation of 11 followed by opening of the epoxide and lactonization or 1,4-nucleophilic addition to the α,β-unsaturated ketone 11 followed by epoxidation of the resulted enolate with subsequent lactonization to
Functionalization of graphene: does the organic chemistry matter?
Beilstein J. Org. Chem. 2018, 14, 2018–2026, doi:10.3762/bjoc.14.177
- (RGO) have most commonly been investigated in terms of creating novel functional materials. GO is a product of oxidative exfoliation from bulk graphite [4]. GO’s structure (Figure 1a) comprises a large number of oxygen functionalities, including carboxyl (COOH), hydroxy (OH) and epoxide (see the
- alcohol. This leads to the formation of the desired ester bond (Figure 3, step e). DMAP acts both as a nucleophile and an acyl transfer reagent and suppresses the side reactions. The structure of GO includes a number of epoxide moieties, which are also reactive toward the nucleophilic reagents. The
- , (c) reaction with DMAP, (d and e) desired reaction pathway (ester or amide bond formation), (d and f) reaction of the activated carboxyl group with water molecules. Mechanism of the epoxide ring opening reaction with the GO/RGO. Generation of the free amine (nucleophile) from the corresponding amine
β-Hydroxy sulfides and their syntheses
Beilstein J. Org. Chem. 2018, 14, 1668–1692, doi:10.3762/bjoc.14.143
- ; epoxide thiolysis; β-hydroxy sulfides; sulfur-containing natural products; Review 1. Introduction Organosulfur compounds are widely distributed in nature, with marine organisms being the richest sources of these, since sulfur, as the sulfate ion, is the second most abundant anion in sea water after
- . Regioselective epoxide ring opening and 1,2-difunctionalization of alkenes are the commonly employed routes in the synthesis of such compounds. Both strategies are discussed below. 3.1 Synthesis of β-hydroxy sulfides via regioselective ring opening of epoxides The considerable ring strain present in epoxides
- thiols to give various β-hydroxy sulfides in good yields (Scheme 1) [20]. Both aryl and alkylthiols were found to be capable of opening the epoxide ring under the reaction conditions, and with respect to the epoxides, cycloalkane, alkene and 1-substituted alkene oxides were all amenable to the reaction
Glycosylation reactions mediated by hypervalent iodine: application to the synthesis of nucleosides and carbohydrates
Beilstein J. Org. Chem. 2018, 14, 1595–1618, doi:10.3762/bjoc.14.137
- , the PMB-protected epoxide 121 was converted to diene 122. The dihydropyran ring of 123 was constructed by RCM of 122 catalyzed by a Grubbs 1st generation catalyst. The isomerization of the double bond in 123 by treatment with a Wilkinson catalyst under basic conditions afforded glycal 124 (Scheme 16
Recent applications of chiral calixarenes in asymmetric catalysis
Beilstein J. Org. Chem. 2018, 14, 1389–1412, doi:10.3762/bjoc.14.117
- reaction in the following order: phase-transfer catalysis, Henry reaction, Suzuki–Miyaura cross-coupling and Tsuji–Trost allylic substitution, hydrogenation, Michael addition, aldol and multicomponent Biginelli reactions, epoxidation, Meerwein−Ponndorf−Verley reduction, aza-Diels−Alder and epoxide ring
- exhibited the best result. Aza-Diels–Alder and epoxide ring-opening reaction Manoury et al. have very recently reported facile synthesis of an enantiomerically pure inherently chiral calix[4]arene phosphonic acid (cR,pR)-121 from the readily available (cS)-enantiomer of calix[4]arene acetic acid 119 or its
- important transformations: phase-transfer catalysis, Henry reaction, Suzuki–Miyaura cross-coupling and Tsuji–Trost allylic substitution, hydrogenation, Michael addition, aldol and multicomponent Biginelli reactions, epoxidation, Meerwein–Ponndorf–Verley reduction, aza-Diels–Alder and epoxide ring-opening
Novel unit B cryptophycin analogues as payloads for targeted therapy
Beilstein J. Org. Chem. 2018, 14, 1281–1286, doi:10.3762/bjoc.14.109
- pseudo-high-dilution conditions to afford 20 and 21 as described previously [16]. Then the diol was transformed into the epoxide following a three-step one-pot reaction as extensively used in the synthesis of cryptophycin analogues [46]. Cryptophycin analogues 22 and 23 were obtained in good purity after
- magenta. Docking of 22 to the vinca domain of β-tubulin. Surface and backbone of β-tubulin are shown in blue, GDP in yellow. No hydrogen bond formation was detected. The orientation of the azidoethoxy-ethoxyethyl substituent prevents the inhibitor from the correct interaction with the protein. The epoxide
- and benzyl group of subunit A are pointing away from the binding pocket. Docking of 24 to β-tubulin. Surface and backbone of β-tubulin are shown in blue, GDP in yellow. H-bonding (yellow dots) was detected with Lys176 and Asp179 in magenta. The benzyl group and the epoxide of subunit A are directed
One hundred years of benzotropone chemistry
Beilstein J. Org. Chem. 2018, 14, 1120–1180, doi:10.3762/bjoc.14.98
A stereoselective and flexible synthesis to access both enantiomers of N-acetylgalactosamine and peracetylated N-acetylidosamine
Beilstein J. Org. Chem. 2018, 14, 856–860, doi:10.3762/bjoc.14.71
- -catalyzed, stereo- and regioselective epoxide opening and subsequent nucleophilic substitution of an azide functionality. This approach enables the synthesis of the naturally D- and unnaturally L-configured GalNAc, as well as both enantiomers of the largely unknown N-acetylidosamine (IdoNAc). Keywords
- stereocenter on C4, resulting in the desired cis-selective epoxide opening and therefore, galacto-configured azido alcohols 7a and 7b (≥95% de) [22]. Initial limitations in reaction size and yield could have been overcome by switching the solvent from THF, as described in the Miyashita protocol, to EtOH. This
- approach opens up new perspectives for additional modifications: meso-tartaric acid as possible starting material or different epoxide opening protocols, as well as, the selective isotopic labelling are only a few to mention. This convertible synthetic route brings us a step closer to access the whole
Nanoreactors for green catalysis
Beilstein J. Org. Chem. 2018, 14, 716–733, doi:10.3762/bjoc.14.61
- epoxide with phenylboronic acid was realized with 2% of pincer catalyst, the rate was 100 times higher for the water-based micellar system compared to the same reaction in organic solvent with the unsupported Pd-complex. A 100 times lower amount of catalyst was also loaded (0.02%), and still the reaction
Volatiles from the tropical ascomycete Daldinia clavata (Hypoxylaceae, Xylariales)
Beilstein J. Org. Chem. 2018, 14, 135–147, doi:10.3762/bjoc.14.9
- with DIBAl-H to 26 that was converted into the epoxide 27a by Sharpless epoxidation with (+)-L-DET. Treatment with TBSOTf and Hünig’s base resulted in opening of the epoxide with concomitant hydride migration to yield 28a. The stereochemical course for this reaction has been reported by Jung and
The synthesis of the 2,3-difluorobutan-1,4-diol diastereomers
Beilstein J. Org. Chem. 2017, 13, 2883–2887, doi:10.3762/bjoc.13.280
- substituents is of interest. Here we describe optimisation efforts in the synthesis of anti-2,3-difluorobutane-1,4-diol, as well as the synthesis of the corresponding syn-diastereomer. Both targets were synthesised using an epoxide opening strategy. Keywords: acetal isomerization; deoxyfluorination; epoxide
- -difluorobutane-1,4-diol (anti-5) starting from commercially available cis-but-2-ene-1,4-diol (Scheme 1) [17]. The vicinal-difluoride group was introduced by a two-step sequence, with initial nucleophilic epoxide [18] opening by a fluoride source [19], followed by nucleophilic deoxyfluorination [9][10][11]. In
- 1 was high-yielding [17], two disadvantages were apparent. First, the epoxide opening takes 2.5 days at 115 °C and uses an expensive fluoride source (Landini’s reagent [18]: Bu4NH2F3). It was found that Bu4NH2F3 made in-house gave significantly reduced yields. Second, the use of the benzyl ether
Synthesis of ergostane-type brassinosteroids with modifications in ring A
Beilstein J. Org. Chem. 2017, 13, 2326–2331, doi:10.3762/bjoc.13.229
- preparation of BS 4 and 5 with a 2,3-epoxide moiety (Scheme 1). To date, only the corresponding 6-ketones were found in natural sources (2,3-diepisecasterone [10] with an α-oriented epoxide 4 and two BS with a β-oriented epoxide 5: secasterone [10][17] and 24-episecasterone [18]). The synthesis of both
- [19]. The 7-membered B ring in 21 had no influence on the stereochemical outcome of the reaction with MCPBA which resulted in the formation of the α-epoxide 22. The same was true for the electrophilic addition of Br+ to the olefinic unit of 21. It produced the trans-diaxial bromohydrine 23 that was
- transformed, on treatment with KOH, into the epoxide 24. The structures of isomeric epoxides 22 and 24 were confirmed by their NOESY spectra as shown in Scheme 4. The obvious NOE correlation between H-3 and H-5 in 24 suggested the spatial vicinity of these two protons, thus the epoxide ring was β-oriented. On
Homologated amino acids with three vicinal fluorines positioned along the backbone: development of a stereoselective synthesis
Beilstein J. Org. Chem. 2017, 13, 2316–2325, doi:10.3762/bjoc.13.228
- have previously reported a concise method for synthesising compounds that contain three vicinal C–F bonds [34]; their method commences with an epoxy alcohol, which undergoes three successive nucleophilic substitutions with fluoride (i.e., deoxyfluorination of the alcohol, epoxide ring opening with
- Et3N·3HF according to O’Hagan’s method [34] (Scheme 3). This did effect epoxide-opening to some extent, but the reaction was rather unsatisfactory because it was low-yielding and non-regioselective, which made full characterisation of the product mixture (32/33) impossible. Nevertheless, an analytical
- it was found that the inclusion of the additive TMS-morpholine [36][37] was also required to ensure a high diastereoisomeric excess of 38a. The epoxide 38a was then ring-opened using Et3N·3HF to deliver the difluorodiol 39a as a mixture of regioisomers. This mixture subsequently converged during the
Synthesis of substituted Z-styrenes by Hiyama-type coupling of oxasilacycloalkenes: application to the synthesis of a 1-benzoxocane
Beilstein J. Org. Chem. 2017, 13, 2122–2127, doi:10.3762/bjoc.13.209
- have recently been reviewed [34]. We have previously reported syntheses of heliannuols C, D, and E via intramolecular epoxide opening reactions [35][36], but this approach did not translate well to the synthesis of heliannuol A. One of our alternative strategies for the synthesis of heliannuol A was an
The chemistry and biology of mycolactones
Beilstein J. Org. Chem. 2017, 13, 1596–1660, doi:10.3762/bjoc.13.159
- the C1–C20 seco acid via formation of the C9–C10 bond by an epoxide-opening reaction with an alkyne-derived alkenyl trialkylaluminate. A distinct strategy was also chosen by the Aggarwal group, which connected the linear C1–C11 fragment to the C12–C20 fragment employing their lithiation–borylation
- obtained according to literature procedures [133], thus setting the stereochemistry at C12. The five-step sequence from 20 to vinyl iodide 21 included a (poorly diastereoselective) epoxidation, epoxide opening with a propynyl anion and a hydrozirconation/iodination reaction to generate the vinyl iodide
- iodide 21. As illustrated in Scheme 2, the nine-step synthesis of the latter proceeded via key epoxide 30 and comprised a diastereoselective alkylation of diethyl (S)-malate according to Seebach and Wasmuth [136] to introduce the C12-methyl group (dr = 8:1). Although being longer than the 1st generation
Strategies toward protecting group-free glycosylation through selective activation of the anomeric center
Beilstein J. Org. Chem. 2017, 13, 1239–1279, doi:10.3762/bjoc.13.123
- by participation of the C2–OH group to release 1,3-dimethylimidazolidin-2-one (DMI), the anomeric leaving group. The epoxide is then opened by the nucleophile when added to the reaction mixture. In pathway C the α-DMC complex is displaced directly by the added nucleophile to liberate DMI, once again
Exploring endoperoxides as a new entry for the synthesis of branched azasugars
Beilstein J. Org. Chem. 2017, 13, 644–647, doi:10.3762/bjoc.13.63
- allow in-depth exploration of the chemistry of this class of azasugar precursors. Some preliminary experiments were performed to assess the possibilities that these building blocks grant. Endperoxide 19 was epoxidized under standard conditions to provide the desired epoxide 25 and the anti-diol 26 as a
- by-product. Likely, diol 26 is formed by ring-opening of the epoxide by water present in the mCPBA and the reaction could be optimised by performing the reaction under anhydrous conditions. Attempts at cleaving the endoperoxide bond of 20 and 21 by catalytic hydrogenation resulted in rapid
Studies directed toward the exploitation of vicinal diols in the synthesis of (+)-nebivolol intermediates
Beilstein J. Org. Chem. 2017, 13, 571–578, doi:10.3762/bjoc.13.56
- that a large number of racemic and asymmetric syntheses of nebivolol and their intermediates have been described in the literature, however, the Sharpless asymmetric dihydroxylation has never been employed as the sole source of chirality for this purpose. Keywords: dihydroxylation; epoxide-ring
- opening; heterocycles; nebivolol; syn-epoxide; Findings Chiral chromans are prevalent components of a large number of natural products, natural product-like molecules and pharmaceutical drugs, possessing diverse biological activities [1]. In view of their wide spectrum of biological profiles, chiral
- 1, method 1). For this purpose, the necessary epoxide 6 could be obtained from the parent E-allylic alcohol through Sharpless asymmetric epoxidation (SAE) [11]. However, the corresponding parent Z-allylic alcohol appears to be not suitable to provide 7 under SAE conditions [20]. This has eliminated
Contribution of microreactor technology and flow chemistry to the development of green and sustainable synthesis
Beilstein J. Org. Chem. 2017, 13, 520–542, doi:10.3762/bjoc.13.51
- 1). The use of an integrated microflow system allowed the preparation of functionalized α-ketoamides by a three-component reaction between carbamoyllithium, methyl chloroformate and organolithium compounds bearing sensitive functional groups (i.e., NO2, COOR, epoxide, carbonyl) (Scheme 2). It should
Secondary metabolome and its defensive role in the aeolidoidean Phyllodesmium longicirrum, (Gastropoda, Heterobranchia, Nudibranchia)
Beilstein J. Org. Chem. 2017, 13, 502–519, doi:10.3762/bjoc.13.50
- ]) and from those of the epoxy-secosterol reported by Anta et al. (δC 65.5 and δC 58.1, respectively; [24]). The downfield shift, observed for these carbons in 1, results from the cleavage of the epoxide ring, and 13C values around δC 70–80 as observed for 1 are characteristic for hydroxylated carbons
- downfield resonances resulting from the lack of a carbon–carbon double bond. Instead, two characteristic 13C NMR shifts at δC 66.4 and 62.3, attributable to an epoxide moiety were present. 13C NMR data of 12 and the specific optical rotation were identical with those reported by Bowden et al. [37], ([α]D20
- and NOESY; all NMR spectral data in Supporting Information File 1, Figures S32–36 and Table S4) experiments and propose the absolute configuration of bisepoxide 12. Bisepoxide 12 has five stereogenic centers, found at the epoxide moieties between C-3 and C-4, and C-11 and C-12, as well as C-2 of the
Synthesis of 1-indanones with a broad range of biological activity
Beilstein J. Org. Chem. 2017, 13, 451–494, doi:10.3762/bjoc.13.48
- synthesize dihydroxy substituted 1-indanones [91]. All reactions have been completed within 2–3 min at 0 °C in the presence of the catalyst Sn(IV)Cl4 (225) and gave products in excellent yields (90–98%). For example, 1-indanone derivative 224 has been obtained from the THP/MOM protected chalcone epoxide 223
- been proposed by Krawczyk et al. [93]. For example, optically active 1-indanone 230 was obtained from the cyclic enol phosphate 228 which next was reacted with a fructose-derived dioxirane 232 generated in situ from the ketone 231, to provide the epoxide 229 (Scheme 64). Then, the latter was hydrolyzed
Solid-phase enrichment and analysis of electrophilic natural products
Beilstein J. Org. Chem. 2017, 13, 405–409, doi:10.3762/bjoc.13.43
- . Results and Discussion In order to evaluate whether the CARR approach is suitable for epoxide detection, we azidated commercially available trans-stilbene oxide as representative model compound for 1 affording the vicinal azido alcohol, 2-azido-1,2-diphenylethanol (Supporting Information File 1, Figure S2
- product could be directly detected in the base-peak chromatogram (BPC) showing the characteristic fragmentation pattern of the CARR adducts (Supporting Information File 1, Figure S3) [15]. Additionally, the detection limit of the model epoxide was investigated in a complex environment. For this, defined
- amounts of trans-stilbene oxide were added to liquid Lysogeny Broth (LB) medium. The obtained methanolic Amberlite XAD-16 extracts were azidated, enriched and analyzed. Up to a final concentration of 5 µg/L (≈25 nmol/L) the epoxide could be detected (Supporting Information File 1, Figure S4). Following
New approaches to organocatalysis based on C–H and C–X bonding for electrophilic substrate activation
Beilstein J. Org. Chem. 2016, 12, 2834–2848, doi:10.3762/bjoc.12.283
- attributed to their ability to form a hydrogen bond with the oxygen of epoxide. In 2015 Shirakawa and Maruoka demonstrated that ammonium salts L5 and L6 could serve as effective catalysts for isoquinolinium and pyridinium salt Mannich reactions (Scheme 7) [50]. Catalysts L5 and L6 were selected due to their
cis-Diastereoselective synthesis of chroman-fused tetralins as B-ring-modified analogues of brazilin
Beilstein J. Org. Chem. 2016, 12, 2816–2822, doi:10.3762/bjoc.12.280
- literature reports on bioactivities of brazilin, haematoxylin and their analogues and our fruitful experience [22][23][25][26] in intramolecular epoxide ring-opening chemistry including IFCEA cyclization, we became interested in the possibility of extending the IFCEA cyclization protocol to the
- that the [6,5]-ring system in brazilin and related natural products 1–4 remains cis-fused, its corresponding [6,6]-ring system in 5 can have cis or trans stereochemistry at the ring junction. In our previous work, we observed a cis relationship (both in concerted or/and stepwise-epoxide ring opening
- ) between the 4-aryl group and H atom at the C-3 position of 4-arylchroman-3-ols (thus giving rise to trans-4-arylchroman-3-ols) [22][23]. But it was not obvious how the planned IFCEA cyclization onto the pre-existing 6-membered ring, in case of stepwise-epoxide ring opening, would influence the product
Other Beilstein-Institut Open Science Activities
