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Methods in organosilane assembly

Bo, Yingjian
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Thesis/Dissertation
Date
2012
Advisor
Sieburth, Scott McNeill
Committee member
Andrade, Rodrigo B.
Davis, Franklin A.
Cannon, Kevin C.
Group
Department
Chemistry
Subject
Chemistry
 Chemistry, Organic
 Chymase Inhibitor
 Lithiation of Alkoxysilanes and Hydridosilanes
 Nk3201
 Organosilane
 Silanediol
 Sulfinimine
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http://hdl.handle.net/20.500.12613/821
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BO_temple_0225E_10976.pdf
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DOI
http://dx.doi.org/10.34944/dspace/803
Abstract
Dialkylsilanediols are a novel class of non-hydrolyzable analogues of the tetrahedral intermediate of amide hydrolysis, shown to be good inhibitors of HIV-1 protease, angiotensin converting enzyme (ACE), and thermolysin. An impediment to utilization of these silanediol structures, however, has been the methods for their assembly. This research describes the reductive lithiation of hydridosilanes and alkoxysilanes, and the use of the resulting silyl anions to develop efficient methods to synthesize silanediol precursors. In the first part of research, lithiation of hydridosilanes was studied. As part of this study, a simple 1H NMR method was developed for monitoring and analyzing the progress of lithiation. In addition, this method was converted to a titration for silyllithium reagents using BHT as an internal standard. Silanediols 107 and 177 are analogues of a potent chymase inhibitor, NK-3201 (82). In the second part, diphenylsilanes 108 and 170, precursors to silanediols 107 and 177, were synthesized using addition of silyllithium to sulfinimine 113 as a key step. In the third part, lithiation of alkoxysilanes was studied. (Si,O)-Dianions, generated from lithiation of silane alcohol 175 or 2,2-diphenyl-1-oxa-2-silacyclopentane (225), were reacted with a wide variety of electrophiles to give potentially useful silicon-containing building blocks. Addition of the (Si,O)-dianion 284 to sulfinimines gave silanediol inhibitor precursors with full control of stereochemistry. In the last part, a new method featuring 1,1-diphenyl-2-azaallyllithium chemistry were utilized to synthesize a series of protected α-amino silanes 323, 329 - 331.
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