Palladium and Gold-Catalyzed transannular [4+3] cycloaddition reactions: Application to the ABCD carbon framework of Cortistatin A. A short synthesis of S-(+)-Siphonodiol. New chiral Au(I) N-heterocyclic carbene complexes and their use in intramolecular c

Craft, Derek T.

26 April 2010

No description available.

Chemistry

transannular

cycloaddition

Cortistatin A

Gold

Development of methodologies employing rhodium catalysis and studies toward the total synthesis of cortistatin A

Smith, Anna Jane, Ph. D.

23 August 2010

[Rh(CO]2Cl]2 has been shown to catalyze sequential, mechanistically- distinct transformations in one pot. Tandem allylic alkylation/cycloisomerization sequences have been developed to access valuable, complex structures from relatively simple substrates. A methodology for the enantioselective conjugate addition of 2-heteroaryl nucleophiles to a variety of Michael acceptors has been developed. This method was used successfully in an ongoing approach to the synthesis of cortistatin A. 10 linear steps have been completed towards the synthesis of cortistatin A, including a highly regioselective propargylation to install a quaternary carbon and a diastereoselective intramolecular Diels-Alder reaction. / text

Cortistatin A

Tandem catalysis

Enantioselective conjugate addition

Studies directed toward the total synthesis of cortistatin A

Littich, Ryan Andrew

07 December 2010

Studies directed toward the total synthesis of the cytotoxic steroidal alkaloid cortistatin A were carried out. In a model system, it was determined that a sequence of reactions involving a lithiocyclopropene addition-intramolecular [4 + 2] cycloaddition cascade and subsequent cyclopropylcarbinyl rearrangement allowed for ready access to the BCD rings of the core steroid. Implementation of this methodology en route to the fully functionalized natural product proved an effective means for the elaboration of the A ring carbocyclic framework. / text

Total synthesis

Cortistatin A

Steroids

Synthetic organic chemistry

Synthesis of Cortistatin Alkaloids and a Versatile Synthesis of Isoquinolines

Si, Chong

10 August 2012

The cortistatins are a recently identified class of marine natural products that were found to exhibit potent and selective inhibition of human umbilical vein endothelial cells (HUVECs), making them promising leads for the development of anti-angiogenic drugs. In our synthesis, we envisioned that natural cortistatins and unnatural analogs could be prepared by late-stage introduction of isoquinolines to 17-keto precursors, and that these differentially substituted precursors could all be derived from a common key intermediate 112. We developed a robust synthetic route to prepare gram quantities of key intermediate 112 starting from readily available benzylzinc reagent 116 and enol triflate 117. Key intermediate 112 was next converted to cortistatin precursors 108, 109, 110, and 111 in three to eight steps, representing each of the four natural cortistatin ABC-ring substitution patterns. Subsequently, a generally applicable method was developed to introduce the isoquinoline moiety. After complexation to N,N,N',N'-tetramethylethylenediamine (TMEDA), 7-lithio-isoquinoline added to 17-keto precursors to provide the corresponding 1,2-addition products; the resulting tertiary alcohols underwent radical deoxygenation via their trifluoroacetates to afford the desired (17S)-products. This organolithium-addition-deoxygenation sequence provided cortistatins A (1, on a 20-mg scale), J (9), K (10), and L (11) in good overall yields. We also synthesized cortistatin primary amines (176 and 186) and used them to prepare several cortistatin based affinity reagents. By employing these reagents in pull-down experiments, we identified a 55-kD membrane kinase as a putative protein target of cortistatins. We wanted to prepare cortistatin analogs with isoquinoline modifications due to the importance of this ring for the biological activity of cortistatins. This led us to develop a novel and versatile synthesis of substituted isoquinolines. In our method, lithiated o-tolualdehyde tert-butylimines were condensed with different nitriles to generate eneamido anion intermediates, which were trapped in situ with various electrophiles at the C4-position, affording a wide range of substituted isoquinolines. Further diversification was achieved by modification of the work-up conditions and by subsequent transformations. / Chemistry and Chemical Biology

angiogenesis

cortistatin

isoquinoline

organolithium addition

radical deoxygenation

organic chemistry

chemistry

Palladium and gold-catalyzed transannular [4+3] cycloaddition reactions application to the ABCD carbon framework of Cortistatin A : a short synthesis of S-(+)-Siphonodiol : new chiral Au(I) N-heterocyclic carbene complexes and their use in intramolecular C /

Craft, Derek T.

January 2010

Title from second page of PDF document. Includes bibliographical references.

An Investigation of Gold(I) Catalyzed Cycloaddition Reactions

Conyers, Ryan C.

19 April 2013

No description available.

Organic Chemistry

Chemistry

Gold

Au

cycloaddition

macrocycle

furan

transannular

intramolecular

intermolecular

cyclopropanation

cascade

cortistatin