textjournal article
Efficient, Enantioselective Assembly of Silanediol Protease Inhibitors
Abstract
A five-step assembly of silicon-protected dipeptide mimics from commercially available reagents is described. This methodology makes silanediol protease inhibitors readily available for the first time. The sequence features asymmetric hydrosilylation, a novel reduction of a silyl ether to a silyllithium reagent, and addition of this dianion to a sulfinimine, to produce the complete inhibitor skeleton with full control of stereochemistry. Oxidation of the primary alcohol to an acid completes the synthesis- Text
- Journal contribution
- Biochemistry
- Genetics
- Pharmacology
- Ecology
- Inorganic Chemistry
- Chemical Sciences not elsewhere classified
- InhibitorsA
- Efficient
- dianion
- dipeptide
- silyl ether
- sequence features
- acid
- hydrosilylation
- methodology
- Silanediol
- synthesis
- assembly
- sulfinimine
- inhibitor skeleton
- novel reduction
- stereochemistry
- Enantioselective Assembly
- Protease
- silanediol protease inhibitors
- silyllithium reagent
- Oxidation
- mimic
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Last time updated on 16/03/2018
This paper was published in The Francis Crick Institute.
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