Enantioselective Deaminative Alkylation of Amino Acid Derivatives with Unactivated Olefins

Sun, Shang‐Zheng; Cai, Yueming; Zhang, Deliang; Jia-bao, Wang; Yao, Hongqing; Rui, Xiyan; Martı́n, Rubén; Shang, Maoyu

doi:10.1021/jacs.1c12350

Cited by 72 publications

(32 citation statements)

References 73 publications

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“…The use of 2,6-di- tert -butylpyridine led to a huge loss of reaction efficiency, demonstrating that a sterically more hindered pyridine derivative lowers the reactivity (entry 7) 50 . 2,4,6-Triphenylpyridine, which may form an acyl analog of the Katritzky salt 51 , 52 , generated the targeted product in a moderate yield (entry 8). When 2,6-lutidine was replaced with common inorganic bases such as cesium carbonate, sodium bicarbonate, or potassium phosphate, the reaction efficiency decreased significantly (entries 9–11).…”

Section: Resultsmentioning

confidence: 99%

Stereoretentive cross-coupling of chiral amino acid chlorides and hydrocarbons through mechanistically controlled Ni/Ir photoredox catalysis

2022

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The direct modification of naturally occurring chiral amino acids to their amino ketone analogs is a significant synthetic challenge. Here, an efficient and robust cross-coupling reaction between chiral amino acid chlorides and unactivated C(sp3)–H hydrocarbons is achieved by a mechanistically designed Ni/Ir photoredox catalysis. This reaction, which proceeds under mild conditions, enables modular access to a wide variety of chiral amino ketones that retain the stereochemistry of the starting amino acids. In-depth mechanistic analysis reveals that the strategic generation of an N-acyllutidinium intermediate is critical for the success of this reaction. The barrierless reduction of the N-acyllutidinium intermediate facilitates the delivery of chiral amino ketones with retention of stereochemistry. This pathway avoids the formation of a detrimental nickel intermediate, which could be responsible for undesirable decarbonylation and transmetalation reactions that limit the utility of previously reported methods.

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Section: Resultsmentioning

confidence: 99%

Stereoretentive cross-coupling of chiral amino acid chlorides and hydrocarbons through mechanistically controlled Ni/Ir photoredox catalysis

2022

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“…Our scope studies were expanded to include Katritzky salts derived from primary aliphatic amines (29, 31, 36-40, 42, 43), as well as electron-poor or heterocyclic benzylic amines (30,41,44), although these substrates required heating to 110 °C. The method is quite general, tolerating basic amines (39)(40)42), amides (32), esters (35)(36)(37)(38), Michael acceptors (41), acetals (36,38), protecting groups including Boc and tosyl (29,(36)(37)(38), and oxime ethers (43) as well as polyfunctionalities seen in drug molecules such as levofloxacin (33), Boclysine methyl ester (37) enoxolone (41), and fluvoxamine (43). 39 and 40 are matched molecular pairs of moclobemide and metoclopramide, respectively, wherein the nitrogen atom has been replaced by an oxygen.…”

Section: Resultsmentioning

confidence: 99%

Repurposing amine and carboxylic acid building blocks with an automatable esterification reaction

McGrath¹,

Zhang²,

Shafiq³

et al. 2022

Preprint

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New methodologies to unite amines and carboxylic acids that complement the popular amide coupling can significantly expand accessible chemical space because they yield products distinct from the classic R–NHC(O)–R’ amide arrangement. Here we have developed an amine–acid esterification reaction based on pyridinium salt activation of amine C–N bonds to create products of type R–OC(O)–R’ upon reaction with alkyl and aryl carboxylic acids. The protocol is robust and facile, as demonstrated by automation on open-source robotics.

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“…12,13,14,15,16 More recently, pyridinium salts have been utilized in deaminative transformations through activation by photoredox catalysis 17 or the formation of CT complexes with electron rich molecules. 18 Despite the widespread application of pyridinium salts as radical precursors, the use of these substrates in catalytic enantioselective transformations is rare, 19 and enantioselective reactions with prochiral enolate equivalents is unprecedented. We initiated our studies by coupling hydrocinnamaldehyde 9 with Katritzky salt 10a derived from the ethyl ester of glycine (Table 1).…”

Section: Scheme 1 Strategy For Catalytic Enantioselective α-Alkylatio...mentioning

confidence: 99%

Catalytic Photochemical Enantioselective α-Alkylation with Pyridinium Salts

Yetra

Schmitt

Tambar

2022

Preprint

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We have developed a chiral amine catalyzed enantioselective α-alkylation of aldehydes with amino acid derived pyridinium salts as alkylating reagents. The reaction proceeds in the presence of visible light (390 nm) and in the absence of a photocatalyst via a light activated charge-transfer complex. We apply this photochemical stereoconvergent process to the total synthesis of the lignan natural products (–)-enterolactone and (–)-enterodiol. Mechanistic studies support the ground-state complex-ation of the reactive components followed by divergent charge-transfer processes involving catalyst-controlled radical chain and in-cage radical recombination steps.

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Enantioselective Deaminative Alkylation of Amino Acid Derivatives with Unactivated Olefins

Cited by 72 publications

References 73 publications

Stereoretentive cross-coupling of chiral amino acid chlorides and hydrocarbons through mechanistically controlled Ni/Ir photoredox catalysis

Stereoretentive cross-coupling of chiral amino acid chlorides and hydrocarbons through mechanistically controlled Ni/Ir photoredox catalysis

Repurposing amine and carboxylic acid building blocks with an automatable esterification reaction

Catalytic Photochemical Enantioselective α-Alkylation with Pyridinium Salts

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