Co-reporter:M. F. Sainz, J. A. Souto, D. Regentova, M. K. G. Johansson, S. T. Timhagen, D. J. Irvine, P. Buijsen, C. E. Koning, R. A. Stockman and S. M. Howdle
Polymer Chemistry 2016 vol. 7(Issue 16) pp:2882-2887
Publication Date(Web):30 Mar 2016
DOI:10.1039/C6PY00357E
We present new acrylic monomers derived directly from abundant naturally available terpenes via a facile, green and catalytic approach. These monomers can be polymerised to create new polymers with a wide range of mechanical properties that positions them ideally for application across the commodity and specialty plastics landscape; from packaging, cosmetic and medical, through to composites and coatings. We demonstrate their utility through formation of novel renewable polymer coatings.
Co-reporter:William M. Dean;Mindaugas &x160;iau&x10d;iulis;Dr. Thomas E. Storr;Dr. William Lewis ; Robert A. Stockman
Angewandte Chemie 2016 Volume 128( Issue 34) pp:10167-10170
Publication Date(Web):
DOI:10.1002/ange.201602264
Abstract
The reaction of chiral (hetero)aryl benzyl sulfoxides with Grignard reagents affords enantiomerically pure diarylalkanes in up to 98 % yield and greater than 99.5 % enantiomeric excess. This ligand coupling reaction is tolerant to multiple substitution patterns and provides access to diverse areas of chemical space in three operationally simple steps from commercially available reagents. This strategy provides orthogonal access to electron-deficient heteroaromatic compounds, which are traditionally synthesized by transition metal catalyzed cross-couplings, and circumvents common issues associated with proto-demetalation and β-hydride elimination.
Co-reporter:Dr. Toni Moragas;Ryan M. Liffey;Dr. Dominika Regentová;Jon-Paul S. Ward;Justine Dutton;Dr. William Lewis; Ian Churcher;Dr. Lesley Walton;Dr. José A. Souto; Robert A. Stockman
Angewandte Chemie 2016 Volume 128( Issue 34) pp:10201-10205
Publication Date(Web):
DOI:10.1002/ange.201604188
Abstract
A novel rearrangement of 2-vinyl aziridine 2-carboxylates to unusual chiral cyclic sulfoximines is described herein. The method allows the synthesis of substituted cyclic sulfoximines in high yields with complete stereocontrol, and tolerates a wide substrate scope. A one-pot process starting directly from sulfinimines provides access to complex chiral sulfoximines in only two steps from commercially available aldehydes. A mechanistic hypothesis and synthetic application in the formal synthesis of trachelanthamidine, by transformation of a cyclic sulfoximine into a pyrroline, is also disclosed.
Co-reporter:William M. Dean;Mindaugas &x160;iau&x10d;iulis;Dr. Thomas E. Storr;Dr. William Lewis ; Robert A. Stockman
Angewandte Chemie International Edition 2016 Volume 55( Issue 34) pp:10013-10016
Publication Date(Web):
DOI:10.1002/anie.201602264
Abstract
The reaction of chiral (hetero)aryl benzyl sulfoxides with Grignard reagents affords enantiomerically pure diarylalkanes in up to 98 % yield and greater than 99.5 % enantiomeric excess. This ligand coupling reaction is tolerant to multiple substitution patterns and provides access to diverse areas of chemical space in three operationally simple steps from commercially available reagents. This strategy provides orthogonal access to electron-deficient heteroaromatic compounds, which are traditionally synthesized by transition metal catalyzed cross-couplings, and circumvents common issues associated with proto-demetalation and β-hydride elimination.
Co-reporter:Dr. Toni Moragas;Ryan M. Liffey;Dr. Dominika Regentová;Jon-Paul S. Ward;Justine Dutton;Dr. William Lewis; Ian Churcher;Dr. Lesley Walton;Dr. José A. Souto; Robert A. Stockman
Angewandte Chemie International Edition 2016 Volume 55( Issue 34) pp:10047-10051
Publication Date(Web):
DOI:10.1002/anie.201604188
Abstract
A novel rearrangement of 2-vinyl aziridine 2-carboxylates to unusual chiral cyclic sulfoximines is described herein. The method allows the synthesis of substituted cyclic sulfoximines in high yields with complete stereocontrol, and tolerates a wide substrate scope. A one-pot process starting directly from sulfinimines provides access to complex chiral sulfoximines in only two steps from commercially available aldehydes. A mechanistic hypothesis and synthetic application in the formal synthesis of trachelanthamidine, by transformation of a cyclic sulfoximine into a pyrroline, is also disclosed.
Co-reporter:M. J. Rawling, T. E. Storr, W. A. Bawazir, S. J. Cully, W. Lewis, M. S. I. T. Makki, I. R. Strutt, G. Jones, D. Hamza and R. A. Stockman
Chemical Communications 2015 vol. 51(Issue 64) pp:12867-12870
Publication Date(Web):09 Jul 2015
DOI:10.1039/C5CC05070G
A heterocyclic, sp3-rich chemical scaffold was synthesised in just 6 steps via a highly regio- and diastereo-selective tandem nitrone formation/intramolecular nitrone–alkene [3+2] cycloaddition reaction. A library of 543 lead-like compounds based on the scaffold core has been produced.
Co-reporter:Thomas E. Storr, Sarah J. Cully, Michael J. Rawling, William Lewis, Daniel Hamza, Geraint Jones, Robert A. Stockman
Bioorganic & Medicinal Chemistry 2015 Volume 23(Issue 11) pp:2621-2628
Publication Date(Web):1 June 2015
DOI:10.1016/j.bmc.2014.12.050
The application of a tandem condensation/cyclisation/[3+2]-cycloaddition/elimination reaction gives an sp3-rich tricyclic pyrazoline scaffold with two ethyl esters in a single step from a simple linear starting material. The successive hydrolysis and cyclisation (with Boc anhydride) of these 3-dimensional architectures, generates unprecedented 16-membered macrocyclic bisanhydrides (characterised by XRD). Selective amidations could then be achieved by ring opening with a primary amine followed by HATU-promoted amide coupling to yield an sp3-rich natural product-like library.
Co-reporter:José A. Souto, Willian Lewis and Robert A. Stockman
Chemical Communications 2014 vol. 50(Issue 84) pp:12630-12632
Publication Date(Web):01 Sep 2014
DOI:10.1039/C4CC05751A
The thermolysis of S-aryl sulfinimines is shown to generate 1,2-disulfoxides and disulfides via initial Cope elimination, dimerisation of the produced sulfenic acid to a thiosulfinate, and subsequent disproportionation of the thiosulfinate.
Co-reporter:George Procopiou, Pooja Aggarwal, Annabella F. Newton, David Richards, Ian R. Mellor, Gareth Harbottle and Robert A. Stockman
Chemical Communications 2014 vol. 50(Issue 97) pp:15355-15357
Publication Date(Web):15 Oct 2014
DOI:10.1039/C4CC07287A
The first total synthesis of myrmicine ant alkaloid 5-epi-cis-275B′ (4) is presented. A tandem cyclisation established the entire core of the structure in a single transformation as well as the required 2,5-anti stereochemistry. Two-directional synthesis was used to furnish the cyclisation precursor 2, as in each of the subsequent steps towards the natural product. The first electrophysiology studies for 4 (against nicotinic acetylcholine receptors) were also conducted, finding modest inhibition of current.
Co-reporter:Toni Moragas, Ian Churcher, William Lewis, and Robert A. Stockman
Organic Letters 2014 Volume 16(Issue 24) pp:6290-6293
Publication Date(Web):December 5, 2014
DOI:10.1021/ol502967x
The aza-Darzens reaction of substituted 2-bromoesters with chiral tert-butane- and mesitylsulfinimines provides a rapid access to a range of highly substituted aziridines in good yields and excellent levels of stereoselectivity. The synthetic potential of this protocol is further enhanced by the successful removal of the sulfinyl motif, yielding simple access to chiral N–H aziridines in just three steps from commercial aldehyde precursors.
Co-reporter:Alexandre Barthelme, David Richards, Ian R. Mellor and Robert A. Stockman
Chemical Communications 2013 vol. 49(Issue 89) pp:10507-10509
Publication Date(Web):27 Sep 2013
DOI:10.1039/C3CC46800C
Total syntheses of alkaloid cis-223B and xenovenine are reported in 3 and 4 steps respectively using a two-directional synthesis/triple reductive amination strategy, and their neurotoxic properties assessed.
Co-reporter:Elise M. Rochette, William Lewis, Al G. Dossetter and Robert A. Stockman
Chemical Communications 2013 vol. 49(Issue 82) pp:9395-9397
Publication Date(Web):22 Aug 2013
DOI:10.1039/C3CC45452E
Chiral amines are formed by the highly diastereoselective intramolecular addition of alkyl and aryl radicals onto chiral mesityl sulfinimines.
Co-reporter:George Procopiou, William Lewis, Gareth Harbottle, and Robert A. Stockman
Organic Letters 2013 Volume 15(Issue 8) pp:2030-2033
Publication Date(Web):April 4, 2013
DOI:10.1021/ol400720b
The cycloaddition of chiral tert-butanesulfinimines with trimethylenemethane is found to give facile access to methylene-pyrrolidines with good yields and diastereoselectivities. The full scope of the cycloaddition is explored, and a range of transformations of the formed methylenepyrrolidines to give a range of functionalized chiral pyrrolidines is presented.
Co-reporter:Camille Gignoux, Annabella F. Newton, Alexandre Barthelme, William Lewis, Marie-Lyne Alcaraz and Robert A. Stockman
Organic & Biomolecular Chemistry 2012 vol. 10(Issue 1) pp:67-69
Publication Date(Web):01 Sep 2011
DOI:10.1039/C1OB06380D
A short and efficient synthesis of an advanced intermediate (1) in the Clive route to halichlorine has been achieved in 12 steps and 13.2% yield by a combined two-directional synthesis/tandem reaction strategy.
Co-reporter:Diane Robbins, Annabella F. Newton, Camille Gignoux, Jean-Christophe Legeay, Alex Sinclair, Martin Rejzek, Carly A. Laxon, Sai K. Yalamanchili, William Lewis, Maria A. O'Connell and Robert A. Stockman
Chemical Science 2011 vol. 2(Issue 11) pp:2232-2235
Publication Date(Web):24 Aug 2011
DOI:10.1039/C1SC00371B
Tying the knot! The marriage of two-directional synthesis and tandem reactions allows access to twelve skeletally diverse scaffolds in just fifteen reactions. Two-directional synthesis yields a symmetrical linear “rope-like” keto-dienoate which is then subjected to twelve separate tandem reactions to “tie the rope in knots” thus creating twelve diverse natural product-like scaffolds containing useful functionality for further elaboration.
Co-reporter:Toni Moragas Solá, Ian Churcher, William Lewis and Robert A. Stockman
Organic & Biomolecular Chemistry 2011 vol. 9(Issue 14) pp:5034-5035
Publication Date(Web):18 May 2011
DOI:10.1039/C1OB05561E
Stereoselective synthesis of 2,3-di- and 2,2′,3-tri-substituted aziridines in good yields and excellent diastereoselectivities are achieved through aza-Darzens reactions of a range of tert-butanesulfinyl aldimines and ketimines with ethyl bromoacetate.
Co-reporter:Caroline Roe, Heather Hobbs, and Robert A. Stockman
The Journal of Organic Chemistry 2011 Volume 76(Issue 22) pp:9452-9459
Publication Date(Web):October 12, 2011
DOI:10.1021/jo201849j
One-pot five-component reactions of oxathiazolidine-S-oxides with mesitylmagnesium bromide, lithium bis(trimethylsilyl)amide, aldehydes and Grignard reagents afford chiral nonracemic amines or sulfinamides in good yields and high stereoselectivities.
Co-reporter:Dr. Caroline Roe;Dr. Heather Hobbs;Dr. Robert A. Stockman
Chemistry - A European Journal 2011 Volume 17( Issue 9) pp:2704-2708
Publication Date(Web):
DOI:10.1002/chem.201003222
Abstract
Two oxathiozolidine-S-oxide templates have been developed and used in a four-component coupling protocol for the synthesis of a wide range of chiral sulfinimines in high enantiomeric excesses. The templates can be synthesized from cheap commodity chemicals in three steps in high yields. Furthermore the template is easily recovered in high yields for recycling.
Co-reporter:Jean-Chistophe Legeay, William Lewis and Robert A. Stockman
Chemical Communications 2009 (Issue 16) pp:2207-2209
Publication Date(Web):03 Mar 2009
DOI:10.1039/B900451C
Two new tandem reactions for the synthesis of 3,5-disubstituted pyrrolizidines and the first total synthesis of alkaloidcis-223B (in 7 steps and 43% overall yield), involving a double cross metathesis and double Michael addition as key steps, are presented.
Co-reporter:Stephen J. Roe, Jean-Christophe Legeay, Diane Robbins, Pooja Aggarwal and Robert A. Stockman
Chemical Communications 2009 (Issue 29) pp:4399-4401
Publication Date(Web):10 Jun 2009
DOI:10.1039/B906301C
Two-directional ring-opening cross-metathesis of a range of cyclic alkenes with a variety of electron deficient alkenes has been accomplished; it was found that the process is quite general and gives complete selectivity for the E,E-dienes, making this a very useful and high-yielding protocol for two-directional chain synthesis.
Co-reporter:Annabella F. Newton, Stephen J. Roe, Jean-Christophe Legeay, Pooja Aggarwal, Camille Gignoux, Nicola J. Birch, Robert Nixon, Marie-Lyne Alcaraz and Robert A. Stockman
Organic & Biomolecular Chemistry 2009 vol. 7(Issue 11) pp:2274-2277
Publication Date(Web):28 Apr 2009
DOI:10.1039/B907720K
Two-directional cross-metathesis of a range of α,ω dienes with a variety of electron deficient alkenes has been accomplished. It was found that the process is quite general and gives complete selectivity for the E,E-dienes, making this a very useful and high yielding protocol for two-directional chain elongation.
Co-reporter:Jiangnan Li, Rafid S. Dawood, Shuanglin Qin, Tongtong Liu, Shuangwei Liu, Robert A. Stockman, Shende Jiang, Guang Yang
Tetrahedron Letters (22 March 2017) Volume 58(Issue 12) pp:1146-1150
Publication Date(Web):22 March 2017
DOI:10.1016/j.tetlet.2017.02.008
Co-reporter:Annabella F. Newton, Stephen J. Roe, Jean-Christophe Legeay, Pooja Aggarwal, Camille Gignoux, Nicola J. Birch, Robert Nixon, Marie-Lyne Alcaraz and Robert A. Stockman
Organic & Biomolecular Chemistry 2009 - vol. 7(Issue 11) pp:NaN2277-2277
Publication Date(Web):2009/04/28
DOI:10.1039/B907720K
Two-directional cross-metathesis of a range of α,ω dienes with a variety of electron deficient alkenes has been accomplished. It was found that the process is quite general and gives complete selectivity for the E,E-dienes, making this a very useful and high yielding protocol for two-directional chain elongation.
Co-reporter:Stephen J. Roe, Jean-Christophe Legeay, Diane Robbins, Pooja Aggarwal and Robert A. Stockman
Chemical Communications 2009(Issue 29) pp:NaN4401-4401
Publication Date(Web):2009/06/10
DOI:10.1039/B906301C
Two-directional ring-opening cross-metathesis of a range of cyclic alkenes with a variety of electron deficient alkenes has been accomplished; it was found that the process is quite general and gives complete selectivity for the E,E-dienes, making this a very useful and high-yielding protocol for two-directional chain synthesis.
Co-reporter:Jean-Chistophe Legeay, William Lewis and Robert A. Stockman
Chemical Communications 2009(Issue 16) pp:NaN2209-2209
Publication Date(Web):2009/03/03
DOI:10.1039/B900451C
Two new tandem reactions for the synthesis of 3,5-disubstituted pyrrolizidines and the first total synthesis of alkaloidcis-223B (in 7 steps and 43% overall yield), involving a double cross metathesis and double Michael addition as key steps, are presented.
Co-reporter:Toni Moragas Solá, Ian Churcher, William Lewis and Robert A. Stockman
Organic & Biomolecular Chemistry 2011 - vol. 9(Issue 14) pp:NaN5035-5035
Publication Date(Web):2011/05/18
DOI:10.1039/C1OB05561E
Stereoselective synthesis of 2,3-di- and 2,2′,3-tri-substituted aziridines in good yields and excellent diastereoselectivities are achieved through aza-Darzens reactions of a range of tert-butanesulfinyl aldimines and ketimines with ethyl bromoacetate.
Co-reporter:George Procopiou, Pooja Aggarwal, Annabella F. Newton, David Richards, Ian R. Mellor, Gareth Harbottle and Robert A. Stockman
Chemical Communications 2014 - vol. 50(Issue 97) pp:NaN15357-15357
Publication Date(Web):2014/10/15
DOI:10.1039/C4CC07287A
The first total synthesis of myrmicine ant alkaloid 5-epi-cis-275B′ (4) is presented. A tandem cyclisation established the entire core of the structure in a single transformation as well as the required 2,5-anti stereochemistry. Two-directional synthesis was used to furnish the cyclisation precursor 2, as in each of the subsequent steps towards the natural product. The first electrophysiology studies for 4 (against nicotinic acetylcholine receptors) were also conducted, finding modest inhibition of current.
Co-reporter:Camille Gignoux, Annabella F. Newton, Alexandre Barthelme, William Lewis, Marie-Lyne Alcaraz and Robert A. Stockman
Organic & Biomolecular Chemistry 2012 - vol. 10(Issue 1) pp:NaN69-69
Publication Date(Web):2011/09/01
DOI:10.1039/C1OB06380D
A short and efficient synthesis of an advanced intermediate (1) in the Clive route to halichlorine has been achieved in 12 steps and 13.2% yield by a combined two-directional synthesis/tandem reaction strategy.
Co-reporter:Diane Robbins, Annabella F. Newton, Camille Gignoux, Jean-Christophe Legeay, Alex Sinclair, Martin Rejzek, Carly A. Laxon, Sai K. Yalamanchili, William Lewis, Maria A. O'Connell and Robert A. Stockman
Chemical Science (2010-Present) 2011 - vol. 2(Issue 11) pp:NaN2235-2235
Publication Date(Web):2011/08/24
DOI:10.1039/C1SC00371B
Tying the knot! The marriage of two-directional synthesis and tandem reactions allows access to twelve skeletally diverse scaffolds in just fifteen reactions. Two-directional synthesis yields a symmetrical linear “rope-like” keto-dienoate which is then subjected to twelve separate tandem reactions to “tie the rope in knots” thus creating twelve diverse natural product-like scaffolds containing useful functionality for further elaboration.
Co-reporter:Elise M. Rochette, William Lewis, Al G. Dossetter and Robert A. Stockman
Chemical Communications 2013 - vol. 49(Issue 82) pp:NaN9397-9397
Publication Date(Web):2013/08/22
DOI:10.1039/C3CC45452E
Chiral amines are formed by the highly diastereoselective intramolecular addition of alkyl and aryl radicals onto chiral mesityl sulfinimines.
Co-reporter:Alexandre Barthelme, David Richards, Ian R. Mellor and Robert A. Stockman
Chemical Communications 2013 - vol. 49(Issue 89) pp:NaN10509-10509
Publication Date(Web):2013/09/27
DOI:10.1039/C3CC46800C
Total syntheses of alkaloid cis-223B and xenovenine are reported in 3 and 4 steps respectively using a two-directional synthesis/triple reductive amination strategy, and their neurotoxic properties assessed.
Co-reporter:José A. Souto, Willian Lewis and Robert A. Stockman
Chemical Communications 2014 - vol. 50(Issue 84) pp:NaN12632-12632
Publication Date(Web):2014/09/01
DOI:10.1039/C4CC05751A
The thermolysis of S-aryl sulfinimines is shown to generate 1,2-disulfoxides and disulfides via initial Cope elimination, dimerisation of the produced sulfenic acid to a thiosulfinate, and subsequent disproportionation of the thiosulfinate.
Co-reporter:M. J. Rawling, T. E. Storr, W. A. Bawazir, S. J. Cully, W. Lewis, M. S. I. T. Makki, I. R. Strutt, G. Jones, D. Hamza and R. A. Stockman
Chemical Communications 2015 - vol. 51(Issue 64) pp:NaN12870-12870
Publication Date(Web):2015/07/09
DOI:10.1039/C5CC05070G
A heterocyclic, sp3-rich chemical scaffold was synthesised in just 6 steps via a highly regio- and diastereo-selective tandem nitrone formation/intramolecular nitrone–alkene [3+2] cycloaddition reaction. A library of 543 lead-like compounds based on the scaffold core has been produced.
![Pyridine, 2-[(phenylmethyl)sulfinyl]-](http://img.cochemist.com/ccimg/87600/87577-90-0.png)
![Pyridine, 2-[(phenylmethyl)sulfinyl]-](http://img.cochemist.com/ccimg/87600/87577-90-0_b.png)
![1H-Isoindole-1,3(2H)-dione, 2-[1-(4-pentenyl)-5-hexenyl]-](http://img.cochemist.com/ccimg/491900/491878-39-8.png)
![1H-Isoindole-1,3(2H)-dione, 2-[1-(4-pentenyl)-5-hexenyl]-](http://img.cochemist.com/ccimg/491900/491878-39-8_b.png)
![Pyridine, 2-[[(4-methoxyphenyl)methyl]sulfinyl]-](http://img.cochemist.com/ccimg/491700/491617-91-5.png)
![Pyridine, 2-[[(4-methoxyphenyl)methyl]sulfinyl]-](http://img.cochemist.com/ccimg/491700/491617-91-5_b.png)
![Carbamic acid, [1-(2-propenyl)-4-pentenyl]-, phenylmethyl ester](http://img.cochemist.com/ccimg/210600/210574-41-7.png)
![Carbamic acid, [1-(2-propenyl)-4-pentenyl]-, phenylmethyl ester](http://img.cochemist.com/ccimg/210600/210574-41-7_b.png)
![Pyridine, 2-[[(3-chlorophenyl)methyl]thio]-](http://img.cochemist.com/ccimg/405100/405063-99-2.png)
![Pyridine, 2-[[(3-chlorophenyl)methyl]thio]-](http://img.cochemist.com/ccimg/405100/405063-99-2_b.png)
![PYRIDINE, 2-[[(4-BROMOPHENYL)METHYL]THIO]-](http://img.cochemist.com/ccimg/83800/83782-57-4.png)
![PYRIDINE, 2-[[(4-BROMOPHENYL)METHYL]THIO]-](http://img.cochemist.com/ccimg/83800/83782-57-4_b.png)
![Pyridine, 2-[[(4-chlorophenyl)methyl]sulfinyl]-](http://img.cochemist.com/ccimg/120000/119929-94-1.png)
![Pyridine, 2-[[(4-chlorophenyl)methyl]sulfinyl]-](http://img.cochemist.com/ccimg/120000/119929-94-1_b.png)
![Pyridine, 2-[[(4-methylphenyl)methyl]sulfinyl]-](http://img.cochemist.com/ccimg/112500/112498-12-1.png)
![Pyridine, 2-[[(4-methylphenyl)methyl]sulfinyl]-](http://img.cochemist.com/ccimg/112500/112498-12-1_b.png)
![Pyridine, 2-[[(3-methylphenyl)methyl]thio]-](http://img.cochemist.com/ccimg/646600/646511-51-5.png)
![Pyridine, 2-[[(3-methylphenyl)methyl]thio]-](http://img.cochemist.com/ccimg/646600/646511-51-5_b.png)
![Pyridine, 2-[(4-methoxyphenyl)methyl]-](http://img.cochemist.com/ccimg/35900/35854-45-6.png)
![Pyridine, 2-[(4-methoxyphenyl)methyl]-](http://img.cochemist.com/ccimg/35900/35854-45-6_b.png)
![Pyridine, 2-[(2-pyridinylmethyl)thio]-](http://img.cochemist.com/ccimg/4300/4262-03-7.png)
![Pyridine, 2-[(2-pyridinylmethyl)thio]-](http://img.cochemist.com/ccimg/4300/4262-03-7_b.png)
![Benzenesulfinamide, N-[(4-methoxyphenyl)methylene]-4-methyl-, (E)-](http://img.cochemist.com/ccimg/158200/158109-77-4.png)
![Benzenesulfinamide, N-[(4-methoxyphenyl)methylene]-4-methyl-, (E)-](http://img.cochemist.com/ccimg/158200/158109-77-4_b.png)
![(2R,3aS,6aR,9aR)-2-methyldodecahydropyrido-[2,1,6-de]quinolizine](http://img.cochemist.com/ccimg/138900/138812-41-6.png)
![(2R,3aS,6aR,9aR)-2-methyldodecahydropyrido-[2,1,6-de]quinolizine](http://img.cochemist.com/ccimg/138900/138812-41-6_b.png)
![Pyridine, 2-[[(2-methylphenyl)methyl]thio]-](http://img.cochemist.com/ccimg/646600/646511-49-1.png)
![Pyridine, 2-[[(2-methylphenyl)methyl]thio]-](http://img.cochemist.com/ccimg/646600/646511-49-1_b.png)
![Pyridine, 2-[[(4-methoxyphenyl)methyl]thio]-](http://img.cochemist.com/ccimg/155300/155222-26-7.png)
![Pyridine, 2-[[(4-methoxyphenyl)methyl]thio]-](http://img.cochemist.com/ccimg/155300/155222-26-7_b.png)
![Hexanal, 6-[[(1,1-dimethylethyl)dimethylsilyl]oxy]-](http://img.cochemist.com/ccimg/118800/118794-69-7.png)
![Hexanal, 6-[[(1,1-dimethylethyl)dimethylsilyl]oxy]-](http://img.cochemist.com/ccimg/118800/118794-69-7_b.png)
![Carbamic acid, [[2-(trimethylsilyl)ethyl]sulfonyl]-, 1,1-dimethylethyl ester](http://img.cochemist.com/ccimg/145400/145387-82-2.png)
![Carbamic acid, [[2-(trimethylsilyl)ethyl]sulfonyl]-, 1,1-dimethylethyl ester](http://img.cochemist.com/ccimg/145400/145387-82-2_b.png)
![Pyridine, 2-[[(4-chlorophenyl)methyl]thio]-](http://img.cochemist.com/ccimg/105900/105837-32-9.png)
![Pyridine, 2-[[(4-chlorophenyl)methyl]thio]-](http://img.cochemist.com/ccimg/105900/105837-32-9_b.png)
![Butanal, 4-[[(1,1-dimethylethyl)dimethylsilyl]oxy]-](http://img.cochemist.com/ccimg/87200/87184-81-4.png)
![Butanal, 4-[[(1,1-dimethylethyl)dimethylsilyl]oxy]-](http://img.cochemist.com/ccimg/87200/87184-81-4_b.png)
![Pyridine, 2-[[3-(trifluoromethyl)phenyl]methyl]-](http://img.cochemist.com/ccimg/782600/782504-60-3.png)
![Pyridine, 2-[[3-(trifluoromethyl)phenyl]methyl]-](http://img.cochemist.com/ccimg/782600/782504-60-3_b.png)
![Benzamide, N-[(1S)-1-(4-methoxyphenyl)-2-methylpropyl]-](http://img.cochemist.com/ccimg/875000/874960-73-3.png)
![Benzamide, N-[(1S)-1-(4-methoxyphenyl)-2-methylpropyl]-](http://img.cochemist.com/ccimg/875000/874960-73-3_b.png)
![Pyridine, 2-[(4-methylphenyl)methyl]-](http://img.cochemist.com/ccimg/29400/29335-87-3.png)
![Pyridine, 2-[(4-methylphenyl)methyl]-](http://img.cochemist.com/ccimg/29400/29335-87-3_b.png)
![6-OXABICYCLO[3.1.0]HEX-2-ENE](http://img.cochemist.com/ccimg/7200/7129-41-1.png)
![6-OXABICYCLO[3.1.0]HEX-2-ENE](http://img.cochemist.com/ccimg/7200/7129-41-1_b.png)
![2-[(2-CHLOROPHENYL)METHYL]PYRIDINE](http://img.cochemist.com/ccimg/37000/36995-37-6.png)
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