Asymmetric Total Synthesis of (+)- and <i>ent</i>-(−)-Yatakemycin and Duocarmycin SA:  Evaluation of Yatakemycin Key Partial Structures and Its Unnatural Enantiomer

Tichenor, Mark S.; Trzupek, John D.; Kastrinsky, David B.; Shiga, Futoshi; Hwang, Inkyu; Boger, Dale L.

doi:10.1021/ja064228j

Cited by 72 publications

(51 citation statements)

References 65 publications

(107 reference statements)

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“…Cross-coupling of the ortho -chloro substituent to give phenylated dihydrobenzofuran proceeded in excellent yield 35 . The carboxylic group could be transformed into an NH 2 group ( 8) through Curtis rearrangement 36 . Last but not the least, with methyl substituents, further benzylic C–H activation and lactonization took place to produce a tricyclic compound ( 9 ) in a moderate yield 37 .…”

Section: Resultsmentioning

confidence: 99%

Oxidative coupling of sp 2 and sp 3 carbon–hydrogen bonds to construct dihydrobenzofurans

Shi¹,

Wang²,

Zhang³

et al. 2017

Nat Commun

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Metal-catalyzed cross-couplings provide powerful, concise, and accurate methods to construct carbon–carbon bonds from organohalides and organometallic reagents. Recent developments extended cross-couplings to reactions where one of the two partners connects with an aryl or alkyl carbon–hydrogen bond. From an economic and environmental point of view, oxidative couplings between two carbon–hydrogen bonds would be ideal. Oxidative coupling between phenyl and “inert” alkyl carbon–hydrogen bonds still awaits realization. It is very difficult to develop successful strategies for oxidative coupling of two carbon–hydrogen bonds owning different chemical properties. This article provides a solution to this challenge in a convenient preparation of dihydrobenzofurans from substituted phenyl alkyl ethers. For the phenyl carbon–hydrogen bond activation, our choice falls on the carboxylic acid fragment to form the palladacycle as a key intermediate. Through careful manipulation of an additional ligand, the second “inert” alkyl carbon–hydrogen bond activation takes place to facilitate the formation of structurally diversified dihydrobenzofurans.

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Section: Resultsmentioning

confidence: 99%

Oxidative coupling of sp 2 and sp 3 carbon–hydrogen bonds to construct dihydrobenzofurans

Shi¹,

Wang²,

Zhang³

et al. 2017

Nat Commun

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“…Analogous to observations made in an asymmetric synthesis of CBI itself, 13c formation of the aryl Grignard reagent by metal–halogen exchange (2.0 equiv of EtMgBr, 23 °C) is followed by the rapid intramolecular epoxide ring opening to give near exclusively 8 , the result of intramolecular 6- endo versus 5- exo addition to the epoxide with only detection of trace amounts of the isomeric product (>13:1, <5%). A similar but technically more demanding protocol, entailing metal–halogen exchange ( i -PrMgCl, THF, −40 °C, 20 min) followed by transmetalation with CuI–PBu 3 (−78 °C, 1 h), 15 also provided 8 (−40 °C, 30 min, 68%) in comparable conversions. O-Debenzylation of 8 , accomplished by transfer hydrogenolysis (cat.…”

Section: Results and Discussionmentioning

confidence: 99%

Asymmetric Synthesis of a CBI-Based Cyclic N-Acyl O-Amino Phenol Duocarmycin Prodrug

Uematsu

Boger

2014

J. Org. Chem.

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A short, asymmetric synthesis of a cyclic N-acyl O-amino phenol duocarmycin prodrug subject to reductive activation based on the simplified 1,2,9,9a-tetrahydrocyclopropa[c]benz[e]indol-4-one (CBI) DNA alkylation subunit is described. A key element of the approach entailed treatment of iodo-epoxide 7, prepared by N-alkylation of 6 with (S)-glycidal 3-nosylate, with EtMgBr at room temperature to directly provide the optically pure alcohol 8 in 78% yield (99% ee) derived from an effective metal–halogen exchange and subsequent regioselective intramolecular 6-endo-tet cyclization. Following O-debenzylation, introduction of a protected N-methylhydroxamic acid, direct trannannular spirocyclization, and subsequent stereoelectronically controlled acid-catalyzed cleavage of the resulting cyclopropane (HCl), further improvements in a unique intramolecular cyclization with N–O bond formation originally introduced for formation of the reductively labile prodrug functionality are detailed.

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“…[27] Alkylation reactions using a glycidyl-nosylate [28] had been shown to proceed regioselectively. [29] Thus, reaction of 18 with the nosylate (+)-(S)-29 afforded (+)-(2'R)-30 in 95 % yield, which in the following metal mediated opening of the epoxide delivered the five-membered ring system (+)-(1S)-31 as the main product in 58 % yield in a stereoselective manner without any loss of stereo integrity. Transformation of (+)-(1S)-31 employing an Appel reaction led to the benzyl protected seco-CBI precursor (À)-(1S)-19 (Scheme 4).…”

Section: Synthesis Of the Seco-drugs And The Prodrugsmentioning

confidence: 98%

Asymmetric Synthesis and Biological Evaluation of Glycosidic Prodrugs for a Selective Cancer Therapy

et al. 2008

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A severe limitation in cancer therapy is the often insufficient differentiation between malign and benign tissue using known chemotherapeutics. One approach to decrease side effects is antibody-directed enzyme prodrug therapy (ADEPT). We have developed new glycosidic prodrugs such as (-)-(1S)-26 b based on the antibiotic (+)-duocarmycin SA ((+)-1) with a QIC(50) value of 3500 (QIC(50)=IC(50) of prodrug/IC(50) of prodrug+enzyme) and an IC(50) value for the corresponding drug (prodrug+enzyme) of 16 pM. The asymmetric synthesis of the precursor (-)-(1S)-19 was performed by arylation of the enantiomerically pure epoxide (+)-(S)-29 (> or = 98 % ee).

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Asymmetric Total Synthesis of (+)- and ent-(−)-Yatakemycin and Duocarmycin SA: Evaluation of Yatakemycin Key Partial Structures and Its Unnatural Enantiomer

Cited by 72 publications

References 65 publications

Oxidative coupling of sp 2 and sp 3 carbon–hydrogen bonds to construct dihydrobenzofurans

Oxidative coupling of sp 2 and sp 3 carbon–hydrogen bonds to construct dihydrobenzofurans

Asymmetric Synthesis of a CBI-Based Cyclic N-Acyl O-Amino Phenol Duocarmycin Prodrug

Asymmetric Synthesis and Biological Evaluation of Glycosidic Prodrugs for a Selective Cancer Therapy

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