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Synthesis and catalytic properties of chiral amphiphilic dendritic organocatalysts. / CUHK electronic theses & dissertations collectionJanuary 2008 (has links)
Several series of amphiphilic dendritic organocatalysts 100--112 containing an optically active, polar proline-derived core, bearing [G1]--[G3] nonpolar hydrocarbon dendrons were synthesized by a convergent approach. These compounds were characterized by NMR spectroscopy, mass spectrometry, elemental analysis and size exclusion chromatographic analysis. Such proline-based organocatalysts have been found to give products in high enantioselectivities in asymmetric aldol reactions and Michael additions in emulsion systems. The incorporation of hydrophobic dendrons in our catalyst has the advantages of promoting emulsion formation in water, enhancing the reactivity and selectivity of the asymmetric reactions, and facilitating catalyst recovery after the reactions. / This thesis describes the syntheses of chiral amphiphilic dendritic organocatalysts and their catalytic applications in asymmetric aldol reactions, Michael additions, and Mannich reactions. / Lo, Chui Man. / Adviser: Hak-Fun Chow. / Source: Dissertation Abstracts International, Volume: 70-06, Section: B, page: 3511. / Thesis (Ph.D.)--Chinese University of Hong Kong, 2008. / Includes bibliographical references (leaves 158-179). / Electronic reproduction. Hong Kong : Chinese University of Hong Kong, [2012] System requirements: Adobe Acrobat Reader. Available via World Wide Web. / Electronic reproduction. [Ann Arbor, MI] : ProQuest Information and Learning, [200-] System requirements: Adobe Acrobat Reader. Available via World Wide Web. / Abstracts in English and Chinese. / School code: 1307.
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The use of glycoside uloses in asymmetric epoxidation.January 2003 (has links)
by Yeung Kwan Wing. / Thesis submitted in: 2002. / Thesis (M.Phil.)--Chinese University of Hong Kong, 2003. / Includes bibliographical references (leaves 68-73). / Abstracts in English and Chinese. / Contents --- p.i / Acknowledgement --- p.ii / Abstract --- p.iii / Abbreviation --- p.v / Chapter 1. --- Introduction --- p.1 / Chapter 1-1 --- Background --- p.1 / Chapter 1-2 --- Sharpless Epoxidation --- p.2 / Chapter 1-3 --- Mn-Salen Complexes for Epoxidation --- p.4 / Chapter 1-4 --- Oxaziridinium Salts --- p.6 / Chapter 1-5 --- Dioxiranes --- p.7 / Chapter 1-6 --- Asymmetric Epoxidation by Dioxirane --- p.11 / Chapter 2. --- Results and Discussion --- p.28 / Chapter 2-1 --- C-Glycoside Ulose Catalyst derived from L-arabinose --- p.28 / Chapter 2-2 --- Dioxirane epoxidation catalyzed by L-arabino-4-uloses --- p.30 / Chapter 3. --- Experimental Section --- p.51 / Chapter 4. --- References --- p.68 / Chapter 5. --- Appendix --- p.74
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Studies on asymmetric reactions and catalysis using axially chiral 2-substituted N, N-dialkyl-1-naphthamides and p-chiral secondary phosphine oxides /Yeung, Ka Yim. January 2003 (has links)
Thesis (Ph. D.)--Hong Kong University of Science and Technology, 2003. / Includes bibliographical references (leaves 196-207). Also available in electronic version. Access restricted to campus users.
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Design of new ligands for asymmetric catalysis /Tong, Ka Pui. January 2003 (has links)
Thesis (M. Phil.)--Hong Kong University of Science and Technology, 2003. / Includes bibliographical references (leaves 107-111). Also available in electronic version. Access restricted to campus users.
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Asymmetric reactions induced by phase-tagged phosphoric acid organocatalysts and copper hydride-catalyzed reductions of unsaturatedthioestersOu, Jun, 欧军 January 2011 (has links)
Two syntheses of non-cross-linked polystyrene-supported TADDOL-based
phosphoric acid organocatalyst have been developed. The optimal polymer-supported
catalyst 2.29d exhibited comparable catalytic activity to its small molecule
counterpart in asymmetric Mannich-type reactions, and the syntheses of several chiral
β-amino esters were demonstrated using 2.29d as catalyst. However, when this
TADDOL-based phosphoric acid was immobilized on a polystyrene cross-linked with
1,4-bis(4-vinylphenoxy)butane, ie. JandaJelTM, the catalytic activity diminished in the
first recycling and reuse of the catalyst.
Building on the success of the immobilization of chiral phosphoric acid, a more
robust phase-tagged BINOL-based phosphoric acid organocatalyst was developed.
By taking advantage of a tetraarylphosphonium salt as a solubility-controlling group,
a widely-used BINOL-based phosphoric acid, TRIP (3.1), was introduced onto a
tetraphenylphosphonium salt to produce a phosphonium salt-tagged phosphoric acid
catalyst 3.3e. After systematic optimizations of reaction conditions, it was found that
the catalyst 3.3e with PF6
as counteranion exhibited the best performance in terms of
enantioselectivity. Catalyst 3.3e was proved to be highly effective in asymmetric
Friedel-Crafts reaction of indoles because it was shown to be recyclable and reusable
after six cycles without loss of catalytic activity.
Based on our previous studies on the reduction of unsaturated thioesters catalyzed
by (BDP)CuH, further investigation of ligand effects revealed that in addition to BDP,
dppf was also an effective ligand for the simple reduction of 5.8. In the
stoichiometric reduction of unsaturated thioester 5.8, dppe and dppf were both
efficient ligands for copper hydride that could convert 5.8 to aldehyde 5.18 in the
presence of TMSCl, without the formation of the undesired enol ester 5.17, which was
a major product when stoichiometric amounts of Stryker’s reagent was employed.
When 5.30 bearing both a saturated and unsaturated thioester was reduced under these
conditions, only the enethioate functional group underwent reaction to yield the
mono-reduced product 5.31 while the saturated thioester functional group remained
inert.
The desymmetrizing reductive aldol reactions of symmetrical keto-enethioates
6.19, 6.22, 6.24 and 6.26 catalyzed by in situ generated chiral copper hydride were
investigated. After a screening of the reaction conditions, TaniaPhos L8 was found to
be the most effective chiral ligand to achieve high ee and yields. Under the optimum
reaction condition (5 mol% Cu(OAc)-H2O and L8 with 2.0 eq. PhSiH3), a range of
keto-enethioates smoothly underwent desymmetrizing reductive aldol cyclizations,
offering bicyclic or polycyclic β-hydroxythioesters (6.28a-6.32a, 6.37a-6.47a) in 35-
84% yield and 30-97% ee with high diastereoselectivity. The addition of 5 mol% of
bipyridine as additive resulted in an accelerated reaction rate in all of the reductions of
keto-enethioates. The crystal structure of the L8-copper bromide complex allowed
the rationalization of the major enantiomer (eg. 6.48a), in which all of the substituents
are cis, to be a result of a reductively generated (Z)-thioester enolate reacting through
a Zimmerman-Traxler transition state.
This stereochemical outcome is in contrast to the reduction of the analogous
oxoesters, which yield trans β-hydroxyesters, (eg. 6.54b), as the major products.
Several proposals to explain the divergent stereochemistry, including the
predominance of a Zimmerman-Traxler transition state of (E)-enolates or subsequent
retroaldol rearrangements, were discussed. The retroaldol rearrangement has been
observed in the conversion of 6.48a to 6.57c, in which there was retention of the
configuration at C5 and a perfect conservation of enantiomeric purity. / published_or_final_version / Chemistry / Doctoral / Doctor of Philosophy
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Organocatalytic asymmetric synthesis of dihydrodibenzofurans and asymmetric aziridination of α-nitroalkenesWang, Ziyu, 汪子玉 January 2012 (has links)
The synthesis of useful chiral skeletons from simple achiral starting materials is always the dream of organic chemists. In the past decades, organocatalysis has been rapidly developed and has become one of the most important methods in asymmetric catalysis. The aim of this thesis is to develop asymmetric methods for the construction of useful chiral skeletons based on organocatalytic chemistry.
Many natural products and biologically important compounds contain the hydrogenated dibenzofuran (Figure 1) as a common sub-structure. In the first part of this thesis, the first amine-catalysed asymmetric synthesis of a dihydrodibenzofuran species from bisenal substrates has been demonstrated.
After a systematic screening of various reaction parameters, the optimal conditions have been found to be as follows: 0.1 M of substrate in solution with toluene with 0.2 equiv of (S)-di(2-naphthyl)pyrrolinol TMS ether (C2.8) and 0.2 equiv of 2-nitrobenzoic acid at 50 ℃ for 7 h under an argon atmosphere (Scheme 1). The first step product, an aldehyde, can be reduced in one pot to an alcohol by NaBH4. This two-step protocol gives exclusive cis selectivity. Many chiral cis-dihydrodibenzofuran species have been synthesized from the corresponding bisenal substrates in moderate to good yield with good to excellent ee (Scheme 1). The resulting cis-dihydrodibenzofuran species have promising synthetic applications. As shown in Scheme 2, the less hindered face of the newly formed C ring is more reactive and highly regioselective functionalizations of the C ring have been achieved.
In the second part of this thesis, the first asymmetric aziridination of trans-α-nitroalkenes via a phase-transfer catalysis strategy has been systematically studied. The chiral phase-transfer catalysts screened are derivatives of the cinchona alkaloids. The new cinchonidine-derived phase-transfer catalyst CD17 has been found to be optimal for the aziridination (Figure 2). Addition of a small amount of water is crucial to achieve complete conversion of the reaction. Both trans-1-nitro-2-arylalkenes and trans-1-nitro-2-alkylalkenes are suitable substrates (Scheme 3). The reaction can be run on the gram-scale without significant loss of efficiency and ee. Mechanistic studies have revealed that the aziridination proceeds through an aza-Michael addition followed by an intramolecular SN 2 type three-membered ring formation (Scheme 4). / published_or_final_version / Chemistry / Doctoral / Doctor of Philosophy
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Chiral phosphonium ion tagged and spiroindane-based organocatalystsHermeke, Julia January 2011 (has links)
The research on asymmetric organocatalysis has been intensifying since the
beginning of 2000. The growing interest in this research area is driven by the
importance of the chemical synthesis of enantiomerically pure products. While
the general field of asymmetric organocatalysis has been explored intensively, the
recyclability of organocatalysts has not really been considered.
The attachment of phosphonium ion phase tags to chiral binaphthyl-based
phosphoric acid catalyst and the use of these materials in a range of
organocatalytic asymmetric Friedel-Crafts reactions of indoles have been studied.
Placement of tags at the 3 and 3’ positions of the binaphthyl core, so that they
could serve as steric blocking groups, failed to produce an active catalyst.
However, moving the phosphonium ion groups to the 6 and 6’ positions produced
an efficient and enantioselective catalyst. Aided by the presence of the phase tags,
the chiral catalyst was easily recovered at the end of the reactions, and could be
reused several times, albeit with somewhat decreased efficiency and
enantioselectivity.
Furthermore, the synthesis of 1,1’-spirobiindane-7,7’-diol and their
spiroindane-based derivatives have been explored. The (R)-1,1’-spirobiindane-
7,7’-diamine was successfully applied in exo selective asymmetric Diels-Alder
reactions of -unsaturated aldehyde with cyclopentadiene. However, moderate
results aspire further studies in assay of (R)-1,1’-spirobiindane-7,7’-diamine
derivatives, which bear various bulky groups at the 6 and 6’ positions. Moreover,
the conversion of the SPINOL into a spiroindane ketone unfortunately failed,
which was caused by the sterically crowded structure of the SPINOL skeleton. / published_or_final_version / Chemistry / Master / Master of Philosophy
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Electrophilic trapping of enolates in tandem reaction processes and (1,3-diketonato)metal templates for asymmetric catalysisBocknack, Brian Matthew 28 August 2008 (has links)
Not available / text
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Enones and enals as latent enolates in catalytic C-C bond forming processes: total synthesis of (-)-paroxetine (Paxil®)Koech, Phillip Kimaiyo 28 August 2008 (has links)
Not available / text
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Enones and enals as latent enolates in catalytic C-C bond forming processes : total synthesis of (-)-paroxetine (Paxil®)Koech, Phillip Kimaiyo, 1974- 24 August 2011 (has links)
Not available / text
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