Ann M. Tickner-Eldridge scite author profile

An asymmetric synthesis of the novel nonracemic endothelin receptor antagonists, SB 209670 (1a) and SB 217242 (1b) is described which utilizes an unprecedented asymmetric Nazarovtype ring closure of the alkylidene-1,3-carbonyl compounds. Excellent 1,5-induction is observed which establishes the required S configuration at the C-3 carbon of an indane skeleton.Successful development of a multikilogram scale synthesis of the novel endothelin receptor antagonists, SB 209670 (1a) and SB 217242 (1b) containing three contiguous stereogenic centers, demanded parallel exploratory development of several potentially scaleable routes. 1 Descriptions of several of those routes have already been, and/or, shortly will be disclosed elsewhere. [2][3][4][5][6] In this communication, we summarize the description of an unprecedented asymmetric Nazarov-type ring closure of the alkylidene-1,3-carbonyl compound 3 where excellent 1,5-induction establishes the required S configuration at the C-3' carbon (eq 1). In our most efficient example, an Evan's oxazolidinone chiral auxiliary of S configuration was employed. 7 Equation 1The Nazarov cyclization is an example of a 4p-electrocyclic closure of a pentadienyl cation. As with all pericyclic reactions, the mechanism and stereochemistry on cyclization are inherently related. For 4p-electrolytic cyclization, in addition to the prerequisite stereochemical imperative of conrotatory or disrotatory ring closure, there exists a secondary stereochemical feature that arises because of the duality of allowed electrocyclization pathways. This feature is called torquoselectivity 8-10 and manifests itself when a remote chiral substituent is present, thus, leading to possibilities of diastereoisomers (eq 2 ). Equation 2Shortly after this work was begun, a report by Tietze 11 appeared describing a cyclization to form enantiomerically pure trans-1,2-disubstituted cyclopentanes with three stereogenic centers using chiral malonic acid derivatives. In that report, asymmetric induction was transferred across five carbons, i.e. 1,5-induction. In our results, reported herein, we employ similar conditions on the chiral derivatives 3a-c to form selectively the indanone 4a-c with similar 1,5-asymmetric induction. Scheme 1

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ChemInform Abstract: A Catalytic Enantioselective Synthesis of the Endothelin Receptor Antagonists SB‐209670 and SB‐217242. A Base‐Catalyzed Stereospecific Formal 1,3‐Hydrogen Transfer of a Chiral 3‐Arylindenol.

Clark

Tickner-Eldridge

Huang

et al. 1998

ChemInform

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A Catalytic Enantioselective Synthesis of the Endothelin Receptor Antagonists SB-209670 and SB-217242. A Base-Catalyzed Stereospecific Formal 1,3-Hydrogen Transfer of a Chiral 3-Arylindenol.-The title antagonists (X) and (XII), containing three contiguous stereocenters, are prepared via a palladium-catalyzed 5-endo-trig cyclization yielding ketone (III). Its enantioselective reduction with the boron catalyst affords alcohol (IV), and as key step a highly stereoselective hydrogen rearrangement of (IV) under optimized conditions gives indanone (V). Further elaboration leads to the desired products. -(CLARK, W. M.; TICKNER-ELDRIDGE, A. M.; HUANG, G. K.; PRIDGEN, L. N.; OLSEN, M. A.; MILLS, R. J.; LANTOS, I.; BAINE, N. H.; J.

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Ann M. Tickner-Eldridge

A Catalytic Enantioselective Synthesis of the Endothelin Receptor Antagonists SB-209670 and SB-217242. A Base-Catalyzed Stereospecific Formal 1,3-Hydrogen Transfer of a Chiral 3-Arylindenol

An Unprecedented Asymmetric Nazarov Cyclization for the Synthesis of Nonracemic Indanes as Endothelin Receptor Antagonists

ChemInform Abstract: A Catalytic Enantioselective Synthesis of the Endothelin Receptor Antagonists SB‐209670 and SB‐217242. A Base‐Catalyzed Stereospecific Formal 1,3‐Hydrogen Transfer of a Chiral 3‐Arylindenol.

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