Stereocontrolled Total Syntheses of Isodomoic Acids G and H via a Unified Strategy

Denmark, Scott E.; Liu, Jack Hung Chang; Muhuhi, Joseck

doi:10.1021/jo101790z

Cited by 26 publications

(4 citation statements)

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“…The majority of work in this area has focused on hydrosilylation chemistry. − Recently, a number of ruthenium catalyzed protocols have emerged for the synthesis of trisubstituted olefins using an intramolecular hydrosilylation of alkynes. − These complementary routes to trisubstituted vinylsilanes are inherently limited due to the mandatory inclusion of a hydrogen atom into the product alkene. Subsequent studies on silylcarbonylation and silylcyanation of alkynes have been described to circumvent this limitation. − Specifically, Ojima and Denmark have studied the silylformylation of alkynes and found that five- and six-membered rings could be formed readily in this reaction. − Silylformylation and silylcyanation reactions afford the syn -alkene isomers selectively. Intermolecular versions of silylcarbocyclization reactions also afford the syn -isomers. − We have recently reported that vinyl-silicon tethers can be used to control both the regio- and stereochemistry in the silylvinylation of pendent alkynes with acrylates …”

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confidence: 99%

Ethylene Transposition: Ruthenium Hydride Catalyzed Intramolecular trans-Silylvinylation of Internal Alkynes

Zhao

Kaminsky

et al. 2014

Org. Lett.

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confidence: 99%

Ethylene Transposition: Ruthenium Hydride Catalyzed Intramolecular trans-Silylvinylation of Internal Alkynes

Zhao

Kaminsky

et al. 2014

Org. Lett.

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“…Asymmetric reduction of 9 a and 9 b with [Rh(cod)( R , R )‐DiPAMP]]BF 4 (cod=1,5‐cyclooctadiene, DiPAMP=1,2‐bis[(2‐methoxyphenyl)phenylphosphino]ethane) (1 mol %) and one‐pot removal of the Cbz group with 10 % Pd/C under a hydrogen atmosphere afforded amines 11 a and 11 b . The tosylation and subsequent propargylation of the crude sulfonamides under Mitsunobu reaction conditions, as reported by Tsunoda, afforded esters 12 a and 12 b in high yields with a small optical purity loss (93 and 94 % ee , respectively) . Reduction of methyl esters with diisobutylaluminum hydride (DIBAL) at −98 °C yielded aldehydes 7 a and 7 b (Scheme ), which immediately participated in the next “anti‐Wacker”‐type cyclization without further purification.…”

Section: Methodsmentioning

confidence: 99%

Scalable Total Syntheses and Structure–Activity Relationships of Haouamines A, B, and Their Derivatives as Stable Formate Salts

Tsukamoto

Nakamura

Tomida

et al. 2020

Chemistry A European J

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Haouamines A, B, and their derivatives were synthesized via Suzuki-Miyaura coupling and three key cyclization reactions as follows: the newly developed palladium(0)-catalyzed arylativec yclizationo fp henylalaninederivedalkyne-aldehydes with 2-bromoarylboronic acid (an "anti-Wacker"-type cyclization);B F 3 •OEt 2-promoted Friedel-Crafts-type cyclization of symmetrical electron-rich aromatic rings adjacentt oatertiary allylic alcohol leading to the indeno-tetrahydropyridine skeleton;a nd (cyanomethyl)trimethylphosphonium iodide-mediated macrocyclizationo fa mino alcohols to afford aza-paracyclophane precursors. The palladium-catalyzed reductiono fm onoand di-triflate intermediates in the later stages enabled the alteration of both the position and number of hydroxyl groups on the C-ring.T he instability of haouamine B was dramatically improved by salt formation with formic acid. An unambiguous evaluation of the cytotoxicity of the prepared haouamine derivativef ormates with and withouth ydroxyl groups at different positions on the Cring indicated that the catechol structure in haouamine B produced weakcytotoxicity. Scheme1.The strategy used herein for haouamines A(1a)and B(1b)syntheses (pin = pinacolato, TBS = tert-butyldimethylsilyl).

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“…The structure of DA has been known since the 1950s, but the first total synthesis was achieved by Tomita group in 1982 . More recently, general syntheses of domoic acid and its isomers ( 38 , 39 , and 41 – 44 ) were established by the groups of Montgomery, Denmark, and Clayden. − They remain the only means to investigate the effect of DA’s side chain.…”

Section: Structural Considerationsmentioning

confidence: 99%

Kainic Acid-Based Agonists of Glutamate Receptors: SAR Analysis and Guidelines for Analog Design

Tian

Clark

Ménard

2019

ACS Chem. Neurosci.

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A comprehensive survey of kainic acid analogs that have been tested for their biological activity is presented. Specifically, this review (1) gathers and compares over 100 kainoids according to a relative activity scale, (2) exposes structural features required to optimize affinity for kainate receptors, and (3) suggests design rules to create next-generation KA analogs. Literature SAR data are analyzed systematically and combined with the most recent crystallographic studies. In view of the renewed interest in neuroactive molecules, this review aims to help guide the efforts of organic synthesis laboratories, as well as to inform newcomers to KA/GluK research.

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Stereocontrolled Total Syntheses of Isodomoic Acids G and H via a Unified Strategy

Cited by 26 publications

References 136 publications

Ethylene Transposition: Ruthenium Hydride Catalyzed Intramolecular trans-Silylvinylation of Internal Alkynes

Ethylene Transposition: Ruthenium Hydride Catalyzed Intramolecular trans-Silylvinylation of Internal Alkynes

Scalable Total Syntheses and Structure–Activity Relationships of Haouamines A, B, and Their Derivatives as Stable Formate Salts

Kainic Acid-Based Agonists of Glutamate Receptors: SAR Analysis and Guidelines for Analog Design

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