Efficient Total Synthesis of (S)‐14‐Azacamptothecin

An efficient total synthesis of (S)‐14‐azacamptothecin has been accomplished in 10 steps and 56 % overall yield from 5H‐pyrano[4,3‐d]pyrimidine 8 . A mild Hendrickson reagent‐triggered intramolecular cascade cyclization, a highly enantioselective dihydroxylation, and an efficient palladium‐catalyzed transformation of an O‐allyl into N‐allyl group are the key steps in the synthesis. This work provides a much higher overall yield than the previous achievement and shows sound flexibility for the further applications that will lead to new bioactive analogues.     

Short Chemoenzymatic Total Synthesis of ent‐Hydromorphone: An Oxidative Dearomatization/Intramolecular [4+2] Cycloaddition/Amination Sequence

A short synthesis of ent‐hydromorphone has been achieved in twelve steps from β‐bromoethylbenzene. The key transformations involved the enzymatic dihydroxylation of the arene to the corresponding cis‐dihydrodiol, Mitsunobu coupling with the ring A fragment, oxidative dearomatization of the C3 phenol, and the subsequent [4+2] cycloaddition to form ring B of the morphinan. The synthesis was completed by intramolecular amination at C9.     

First Synthesis and Utilization of Oripavidine – A Concise and Efficient Route to Important Morphinans and Apomorphines

The synthesis and transformation of oripavidine ( 8 ) offer an efficient and simple route to highly active dopamine agonist apomorphines and a variety of important 14β‐hydroxy‐morphinan derivatives. Natural origin thebaine ( 6 ), the starting compound of the procedure, was converted into its N‐{[1,2‐bis(ethoxycarbonyl)hydrazinyl]methyl} counterpart. L ‐Selectride was found to be an efficient agent to perform a one‐pot O‐ and N‐deprotection at positions 3 and 17, respectively.     

Stereoselective Total Synthesis of (11β)‐11‐Methoxycurvularin

A simple and highly efficient stereoselective total synthesis of (11β)‐11‐methoxycurvularin ( 5 ), a polyketide natural product, was achieved. The synthesis commenced with a Cu‐mediated regioselective opening of (2S)‐2‐methyloxirane ( 6 ) and comprised a Keck asymmetric allylation and intramolecular Friedel–Crafts acylation as key steps (Scheme 2).     

Inter‐ and intramolecular C—H...π interactions in morphine bis­(1‐naph­tho­ate)

The crystal structure of morphine bis­(1‐naph­tho­ate) [or 7,8‐di­de­hydro‐4,5‐epoxy‐17‐methyl­morphinan‐2,6‐diyl bis­(naph­thal­ene‐1‐carboxyl­ate)], C₃₉H₃₁NO₅, determined at 123 K, shows extensive C—H...π interactions in the crystal lattice. Of particular interest is an intramolecular C—H...π interaction within the unit cell between the two naphthoyl groups. Comparison of the opiate scaffolds of morphine bis­(1‐naph­tho­ate) and morphine shows only a small increase in strain due to the steric bulk of the naphthoyl groups. The crystal packing shows distinct areas of packing for the naphthalene/aromatic groups and the opiate backbone. Extensive inter‐ and intramolecular C—H...π interactions lead to a densely packed aromatic region in the crystal lattice.     

Two‐Step Synthesis of Multifunctional γ‐Lactams from γ‐Lactone

We present herein an efficient and rapid method for the synthesis of N,1‐dialkyl‐4‐(2‐hydroxyethyl)‐5‐oxopyrrolidine‐3‐carboxamides based on the conversion of γ‐lactone to γ‐lactam via the conjugate addition of primary amines to an ethyl α‐functionalized acrylate followed by intramolecular cyclization.     

Enantioselective Synthesis of (−)‐(R)‐Cordiachromene and (−)‐(R)‐Dictyochromenol Utilizing Intramolecular SNAr Reaction

A simple and efficient enantioselective synthesis of chromene, (?)‐(R)‐cordiachromene ( 1 ), and (?)‐(R)‐dictyochromenol ( 2 ) has been accomplished. This convergent synthesis utilizes intramolecular S_NAr reaction for the formation of chroman ring, and Seebach's method of ‘self‐reproduction of chirality’ should establish the (R)‐configuration of the C(2) side chain as key steps.     

Total Synthesis of (−)‐Daphenylline

A concise and highly stereoselective total synthesis of the Daphniphyllum alkaloids (?)‐daphenylline has been accomplished. The synthesis was started from (S)‐carvone and proceeded via a stereoselective Mg(ClO₄)₂‐catalyzed intramolecular amide addition cyclization, an intramolecular Diels–Alder reaction to construct the ABCD tetracyclic core architecture, and a Robinson annulation coupled with an oxidative aromatization sequence. Finally, the DF ring system was installed through an intramolecular Friedel–Crafts cyclization. The total synthesis of (?)‐daphenylline is achieved in 19 steps in the longest reaction sequence and in 7.6 % overall yield.     

Asymmetric Total Synthesis of (−)‐Maoecrystal V

The asymmetric total synthesis of (?)‐maoecrystal V, a novel cytotoxic pentacyclic ent‐kaurane diterpene, has been accomplished. Key steps of the current strategy involve an early‐stage semipinacol rearrangement reaction for the construction of the C10 quaternary stereocenter, a rhodium‐catalyzed intramolecular O?H insertion reaction, and a sequential Wessely oxidative dearomatization/intramolecular Diels–Alder reaction to forge the pentacyclic framework of maoecrystal V.     

Asymmetric Total Synthesis of (−)‐Kravanhin B

The first asymmetric total synthesis of kravanhin B has been accomplished with a linear reaction sequence of 13 steps starting from (R)‐(?)‐carvone. The synthesis features an intramolecular aldol cyclization to construct the desired cis‐fused decalin skeleton and an acid‐catalyzed dehydration and olefin isomerization to install the γ‐butenolide ring.     

A Concise Stereoselective Synthesis of (R)‐2‐Benzylmorpholine and ML398 from (R)‐(−)‐2‐Phenylglycinol

We describe here an efficient stereoselective method for the preparation of (R)‐2‐benzylmorpholine and ML398. The present method features a high diastereocontrol using an endocyclic oxidation of phenylglycinol‐derived morpholine and a stereoselective alkylation of chiral non‐racemic morpholin‐3‐one as key steps.     

First Total Synthesis of (±)‐Celaphanol A

The first total synthesis of (±)‐Celaphanol A was accomplished starting from α‐cyclocitral and 3,4‐dimethoxy benzyl chloride in six steps. The intramolecular cyclization with BF₃·Et₂O and enolization in t‐BuOK/t‐BuOH were the key steps. The process of intramolecular cyclization afforded an all‐cis isomer intermediate for synthesis of aromatic tricyclic diterpenes.     

Copper‐Catalyzed Domino Synthesis of 2‐Imino‐1H‐imidazol‐5(2H)‐ones and Quinoxalines Involving CC Bond Cleavage with a 1,3‐Dicarbonyl Unit as a Leaving Group

Although 2‐imino‐1H‐imidazol‐5(2H)‐ones have important biological activities in metabolism, their synthesis has rarely been investigated. Quinoxalines as “privileged scaffolds” in medicinal chemistry have been extensively investigated, but the development of novel and efficient synthetic methods remains very attractive. Herein, we have developed two copper‐catalyzed domino reactions for the synthesis of 2‐imino‐1H‐imidazol‐5(2H)‐ones and quinoxalines involving C?C bond‐cleavage with a 1,3‐dicarbonyl unit as a leaving group. The domino sequence for the synthesis of 2‐imino‐1H‐imidazol‐5(2H)‐ones includes aza‐Michael addition, intramolecular cyclization, C?C bond‐cleavage, 1,2‐rearrangement, and aerobic dehydrogenation reaction, whereas the domino sequence for the synthesis of quinoxalines includes aza‐Michael addition, intramolecular cyclization, elimination reaction, and C?C bond‐cleavage reaction. The two domino reactions have significant advantages including high efficiency, mild reaction conditions, and high tolerance of various functional groups.     

Heteronuclear NMR spectroscopic investigations of hydrogen bonding in 2‐(benzo[d]thiazole‐2′‐yl)‐N‐alkylanilines

The 2‐(benzo[d]thiazole‐2′‐yl)‐N‐alkylanilines have previously revealed the presence of a strong intramolecular hydrogen bond. This in turn gives rise to a more complicated multiplet for the protons attached to the carbon adjacent to the amino group. This intramolecular hydrogen bond was investigated by a deuterium exchange experiment using heteronuclear NMR spectroscopy (¹H, ¹³C, ¹⁵ N and ²H). We observed changes in the multiplet structure and chemical shifts providing further evidence that the deuterium replaces the hydrogen in the intramolecular hydrogen bond. A time course study of the D₂O exchange confirmed the presence of a strong hydrogen bond. The comparison of the structures obtained by X‐ray crystallography showed a very small difference in planarity between the two‐substituted and four‐substituted amino compounds. In both the cases, the phenyl ring is not absolutely coplanar with the thiazole unit. The existence of this intramolecular hydrogen bond in 2‐(benzo[d]thiazole‐2′‐yl)‐N‐alkylanilines was further confirmed by single crystal X‐ray crystallography. Copyright © 2015 John Wiley & Sons, Ltd.     

Synthesis of a Benzannulated Pyrrolizidine by a Copper‐Catalyzed Intramolecular α‐Arylation Reaction

A synthetic route to the pyrrolo[1,2‐a]indole ring system (benzannulated pyrrolizidine) involving a base‐induced intramolecular aza‐Michael reaction as the key C? N bond‐forming penultimate step, followed by a Cu‐catalyzed intramolecular α‐arylation reaction, to provide the tricyclic framework over six steps is described.     

A Cascade Strategy Enables a Total Synthesis of (−)‐Gephyrotoxin

A concise and efficient synthesis of (?)‐gephyrotoxin from L ‐pyroglutaminol has been realized. The key step in this approach is a diastereoselective intramolecular enamine/Michael cascade reaction that forms two rings and two stereocenters and generates a stable tricyclic iminium cation. A hydroxy‐directed reduction of this intermediate plays a key role in establishing the required cis‐decahydroquinoline ring system, enabling the total synthesis of (?)‐gephyrotoxin in nine steps and 14 % overall yield. The absolute configuration of the synthetic material was confirmed by single‐crystal X‐ray diffraction and is consistent with the structure originally proposed for material isolated from the natural source.     

Charge Transfer Through Dithieno[2,3‐a:3′,2′‐c]phenazine: Effect of Substitution Pattern on the Optoelectronic Properties of Regioisomeric Luminophores

Two series of regioisomeric luminophores that contained a dithieno[2,3‐a:3′,2′‐c]phenazine (DTP) unit as an electron acceptor have been designed and synthesized. To investigate the effect of substitution pattern on the optoelectronic properties of these luminophores, electron donors (N,N‐dihexylaniline or N,N‐dihexyl‐4‐vinylaniline) were incorporated at the 2,5‐, 8,11‐, and 9,10‐positions of the DTP unit. We found that the optoelectronic properties of the regioisomeric luminophores were greatly affected by the substitution pattern: functionalization at the 8,11‐positions of the DTP unit was superior to the other two substitution patterns in extending the effective π‐conjugation and strengthening the intramolecular charge‐transfer interactions. Moreover, the insertion of vinyl groups between the DTP and N,N‐dihexylaniline units narrowed the energy band‐gap for isomers 4 and 5 . However, hypsochromically shifted absorption and photoluminescence maxima were observed for isomeric luminophore 6 , in which electron donors were substituted at the 2,5‐positions of the DTP unit. These results should facilitate greater understanding of the structure–property relationships in regioisomeric semiconductors and present a new way to design optoelectronic materials with effective substitution patterns.     

Asymmetric Synthesis of the C(33) – C(37) Fragment of Amphotericin B

We have devised an expeditious, efficient, asymmetric synthesis of the C(33) – C(37) fragment of amphotericin B that proceeds in 14 steps and 16% overall yield from tiglic aldehyde ((E)‐2‐methylbut‐2‐enal) with complete stereocontrol. The route described herein relies on the application of recently developed methods in catalytic asymmetric synthesis for stereocontrol through enantio‐ and diastereoselective functionalization of a substituted sorbate derivative.     

Chiral Cp‐Rhodium(III)‐Catalyzed Asymmetric Hydroarylations of 1,1‐Disubstituted Alkenes

Metal‐catalyzed functionalizations at the ortho position of a directing group have become an efficient bond‐forming strategy. A wide range of transformations that employ Cp*Rh^III catalysts have been described, but despite their synthetic potential, enantioselective variants that use chiral versions of the Cp* ligand remain scarce (Cp*=pentamethyl cyclopentadienyl). Cyclopentadienyl compounds with an atropchiral biaryl backbone are shown to be suitable ligands for the efficient intramolecular enantioselective hydroarylation of aryl hydroxamates. Dihydrofurans that bear methyl‐substituted quaternary stereocenters are thus obtained by C? H functionalization under mild conditions.     

Synthesis of (‐)‐herbertenediol and (aR,aS)‐mastigophorenes A via asymmetric intramolecular heck coupling reaction

Total enantioselective synthesis of the natural (‐)‐Herbertenediol (1) was accomplished in eleven steps with an overall yield of 15% starting from the 2‐methoxy‐4‐methyl‐phenol. The total synthesis features asymmetric intramolecular Heck reaction and Wolff‐Kishner‐Huang reduction. (aR, aS)‐Mastigophorenes A was also synthesized through the oxidative coupling reaction.