Synthesis and PKC Binding of a New Class of A-Ring Diversifiable Bryostatin Analogues Utilizing a Double Asymmetric Hydrogenation and Cross-Coupling Strategy

Paul A. Wender,Joshua C. Horan

Synthesis and PKC Binding of a New Class of A-Ring Diversifiable Bryostatin Analogues Utilizing a Double Asymmetric Hydrogenation and Cross-Coupling Strategy

2006

Paul A. Wender
Joshua C. Horan

The design, asymmetric synthesis, and biological evaluation of a new class of bryostatin analogues based on a pseudosymmetric spacer domain are described. An aryl bromide diversification site is incorporated allowing access to systematically varied analogues. The new analogues all exhibit potent, nanomolar affinity to PKC.

Keywords:

Enantioselective synthesis
Protein kinase C
PKC binding
Aryl
Bromide
Bryostatin
Stereochemistry
Organic chemistry
Chemistry
Asymmetric hydrogenation
Coupling

Correction
Source
Cite
Save
Machine Reading By IdeaReader

References

Citations