Enantioenriched Oxazolidinones as Synthesis Scaffolds and Efforts towards the Total Synthesis of Marineosin A

Lang, Feng (2018) Enantioenriched Oxazolidinones as Synthesis Scaffolds and Efforts towards the Total Synthesis of Marineosin A. Doctoral Dissertation, University of Pittsburgh. (Unpublished)

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Abstract

Enantioenriched Oxazolidinones as Synthesis Scaffolds and
Efforts towards the Total Synthesis of Marineosin
Feng Lang, PhD
University of Pittsburgh, 2018

The utility of enantioenriched oxazolidinones in the preparation of small chiral building blocks has been investigated. Hard nucleophile induced ring opening reactions of oxazolidinones provided a series of enantioenriched α-hydroxy carbonyl compounds. Soft nucleophile induced ring opening reactions of oxazolidinones have been attempted. Aldol reactions and Mannich reactions of oxazolidinones afforded the addition products with good results. Additionally, the aldol addition products were able to be converted to enantioenriched α,β-dihydroxy carbonyl compounds with a quaternary chirality center at the α position. In addition, chiral diol was also obtained through the reductive ring opening reaction of oxazolidinone.

The synthesis of marineosin A, a structurally unique natural product exhibiting acute cytotoxicity, has been under investigation in our laboratory. The previously unreported spiroaminal structure consisting of tetrahydropyrrole ring and dihydropyran ring has been synthesized through a radical cyclization in model study. The 12-membered macrocyclic pyrrole core synthesis has been accomplished by Stetter reaction in model study. It is worth noting that this is the first time that Stetter reaction was used in macrocyclization reaction. Both the diene fragment and the dienophile fragment have been prepared successfully towards the synthesis of the densely functionalized tetrahydropyran ring in marineosin A.

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Details

Item Type:	University of Pittsburgh ETD
Status:	Unpublished
Creators/Authors:	Creators Email Pitt Username ORCID Lang, Feng fel18@pitt.edu fel18 0000-0002-8185-3464
ETD Committee:	Title Member Email Address Pitt Username ORCID Committee Chair Nelson, Scott sgnelson@pitt.edu sgnelson Committee Member Wilcox, Craig daylite@pitt.edu daylite Committee Member Liu, Xinyu xinyuliu@pitt.edu xinyuliu Committee Member Zhang, Lin zhanglx@upmc.edu zhanglx
Date:	28 June 2018
Date Type:	Publication
Defense Date:	29 March 2018
Approval Date:	28 June 2018
Submission Date:	8 April 2018
Access Restriction:	No restriction; Release the ETD for access worldwide immediately.
Number of Pages:	152
Institution:	University of Pittsburgh
Schools and Programs:	Dietrich School of Arts and Sciences > Chemistry
Degree:	PhD - Doctor of Philosophy
Thesis Type:	Doctoral Dissertation
Refereed:	Yes
Uncontrolled Keywords:	Oxazolidinones; Methodology; Asymmetric synthesis; Marineosin A; Total synthesis
Date Deposited:	28 Jun 2018 15:37
Last Modified:	28 Jun 2018 15:37
URI:	http://d-scholarship.pitt.edu/id/eprint/34185

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