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Henry reaction

December 15, 2023

The Henry reaction is a classic carbon–carbon bond formation reaction in organic chemistry. Discovered in 1895 by the Belgian chemist Louis Henry (1834–1913), it is the combination of a nitroalkane and an aldehyde or ketone in the presence of a base to form β-nitro alcohols.[1][2][3] This type of reaction is also referred to as a nitroaldol reaction (nitroalkane, aldehyde, and alcohol). It is nearly analogous to the aldol reaction that had been discovered 23 years prior that couples two carbonyl compounds to form β-hydroxy carbonyl compounds known as "aldols" (aldehyde and alcohol).[2][4] The Henry reaction is a useful technique in the area of organic chemistry due to the synthetic utility of its corresponding products, as they can be easily converted to other useful synthetic intermediates. These conversions include subsequent dehydration to yield nitroalkenes, oxidation of the secondary alcohol to yield α-nitro ketones, or reduction of the nitro group to yield β-amino alcohols.

Henry reaction
Named after Louis Henry
Reaction type Coupling reaction
Identifiers
Organic Chemistry Portal henry-reaction
RSC ontology ID RXNO:0000086
Henry reaction synthetic scheme

Many of these uses have been exemplified in the syntheses of various pharmaceuticals including the β-blocker (S)-propranolol,[5][6] the HIV protease inhibitor Amprenavir (Vertex 478), and construction of the carbohydrate subunit of the anthracycline class of antibiotics, L-Acosamine.[6] The synthetic scheme of the L-Acosamine synthesis can be found in the Examples section of this article.

Mechanism edit

The Henry reaction begins with the deprotonation of the nitroalkane on the α-carbon position forming a nitronate. The pKa of most nitroalkanes is approximately 17.[7][8] Although this structure is nucleophilic both at the deprotonated carbon and at the oxy-anions of the nitro group,[9] the observed result is of the carbon attacking the carbonyl compound. The resulting β-nitro alkoxide is protonated by the conjugate acid of the base that originally deprotonated the nitroalkyl structure, giving the respective β-nitro alcohol as product.

 
Henry reaction mechanism

It is important to note that all steps of the Henry reaction are reversible. This is due to the lack of a committed step in the reaction to form product. It is for this reason that research has been geared towards modifications to drive the reaction to completion.[2][3] More information about this can be found in the modification section of this article.

Stereochemical Course edit

The figure below illustrates one of the commonly accepted models for stereoselection without any modification to the Henry reaction. In this model, stereoselectivity is governed by the size of the R groups in the model (such as a carbon chain), as well as by a transition state that minimizes dipole by orienting the nitro group and carbonyl oxygen anti each other (on opposite sides of the molecule). The R groups play a role in the transition state of the Henry reaction: the larger the R groups on each of the substrates, the more they will tend to orient themselves away from each other (commonly referred to as steric effects). [3][10]

 
Henry stereoselection without modification

Due to the reversibility of the reaction and the tendency for easy epimerization of the nitro-substituted carbon atom (among a number of factors), the Henry reaction will typically produce a mixture of enantiomers or diastereomers. It is for this reason that explanations for stereoselectivity remain scarce without some modification of the reaction.[3] In recent years, research focus has shifted toward modifications of the Henry reaction to overcome this synthetic challenge.

 
Henry reaction synthetic scheme

The first example of an enantioselective nitroaldol reaction was reported in 1992 using Shibasaki catalysts.[11] One of the most frequently employed methods for inducing enantio- or diastereoselectivity in the Henry reaction is the use of chiral metal catalysts, in which the nitro group and carbonyl oxygen coordinate to a metal that is bound to a chiral organic molecule. Some metals that have been used include zinc, cobalt, copper, magnesium, and chromium.[12] A depiction of this coordination is illustrated above.

General Features edit

One of the many features of the Henry reaction that makes it synthetically attractive is that it utilizes only a catalytic amount of base to drive the reaction. Additionally a variety of bases can be used including ionic bases such as alkali metal hydroxides, alkoxides, carbonates, and sources of fluoride anion (e.g. TBAF) or nonionic organic amine bases including TMG, DBU, DBN, and PAP. It is important to note that the base and solvent used do not have a large influence on the overall outcome of the reaction.[2]

Limitations edit

One of the main drawbacks of the Henry reaction is the potential for side reactions throughout. Aside from the inherent reversibility of the reaction (or "retro–Henry") that can prevent the reaction from proceeding, the β-nitro alcohol also has the potential to undergo dehydration. For sterically hindered substrates, it is also possible for a base-catalyzed self-condensation (Cannizzaro reaction) to occur. A general scheme of the Cannizzaro reaction is depicted below.[2]

 
Cannizzaro Reaction Scheme

Modifications edit

There have been a series of modifications made to the Henry reaction. Of these some of the most important include employing high-pressure and sometimes solvent free conditions to improve chemo- and regioselectivity[2] and chiral metal catalysts to induce enantio-or diastereoselectivity.[12] The aza-Henry reaction is also used to produce nitroamines and can be a reliable synthetic route for the synthesis of vicinal diamines.[13]

Perhaps one of the most synthetically useful modifications to the Henry reaction is the use of an organocatalyst.[2][12][14] The catalytic cycle is shown below.

 
Henry reaction synthetic scheme

Benjamin List described that while this is a broad explanation, his brief review illustrates that this is a plausible mechanistic explanation for almost all reactions that involve an organocatalyst. An example of this type of reaction is illustrated in the Examples section of this article.

In addition to the previously mentioned modifications to the Henry reaction there are a variety of others. This includes the conversion of unreactive alkyl nitro compounds to their corresponding dianions which will react faster with carbonyl substrates, reactions can be accelerated using PAP as base, utilization of the reactivity of aldehydes with α,α-doubly deprotonated nitroalkanes to give nitronate alkoxides that yield mainly syn-nitro alcohols once protonated, and finally generation of nitronate anions in which one oxygenatom on the nitro group is silyl-protected to yield anti-β-nitro alcohols in the presence of a fluoride anion source when reacted with an aldehyde.[2][3]

Examples edit

Industrial Application
In 1999, Menzel and coworkers developed a synthetic route to obtaining L-acosamine, the carbohydrate subunit of the anthracycline class of antibiotics:[6][15]
 
Acosamine scheme
Industrial Application
An enantioselective aldol addition product can be obtained in asymmetric synthesis by reaction of benzaldehyde with nitromethane and the a catalyst system consisting of zinc triflate as a Lewis acid, diisopropylethylamine (DIPEA), and N-methylephedrine (NME) as and as a chiral ligand.[16] A diastereoselective variation of this reaction is depicted below.[17]
 
Henry reaction application
Total Synthesis
In 2005, Barua and coworkers completed the total synthesis of the potent aminopeptidase inhibitor, (–)-bestatin, in an overall yield of 26% overall yield employing Shibasaki's asymmetric Henry reaction as the key step. (illustrated below)[6][18]
 
Bestatin
Organocatalysis
In 2006, Hiemstra and coworkers explored the use of quinine derivatives as asymmetric catalysts for the reaction between aromatic aldehydes and nitromethane. Through the use of particular derivatives, they were able to induce direct enantioselection through the use of the proper catalyst.[19]
 
Chinchura
Biocatalysis
In 2006, Purkarthofer et al. found that (S)-hydroxynitrile lyase from Hevea brasiliensis catalyzes the formation of (S)-β-nitro alcohols.[20] In 2011, Fuhshuku and Asano showed that the (R)-selective hydroxynitrile lyase from Arabidopsis thaliana could catalyze the synthesis of (R)-β-nitro alcohols from nitromethane and aromatic aldehydes.[21]

References edit

  1. ^ Henry, Louis (1895). "Formation synthétique d'alcools nitrés" [Synthetic formation of nitrated alcohols]. Comptes rendus. 120: 1265–1268.
  2. ^ a b c d e f g h Kurti, L.; Czako, B. (2005). Strategic Applications of Named Reactions in Organic Synthesis. Burlington, MA: Elsevier Academic Press. pp. 202–203. ISBN 978-0-12-369483-6.
  3. ^ a b c d e Noboro, Ono (2001). The Nitro Group in Organic Synthesis. New York, NY: Wiley-VCH. pp. 30–69. ISBN 978-0-471-31611-4.
  4. ^ Wurtz, M.A. (1872). "Sur un aldéhyde-alcool". Bull. Soc. Chim. Fr. 17: 436–442.
  5. ^ Sasai, H., Suzuki, T., Itoh, N., Arai, S., Shibasaki, M. (1993). "Catalytic Asymmetric Nitroaldol Reaction: an efficient synthesis of (s) propranolol using the lanthenum binaphthol complex". Tetrahedron Letters. 34 (52): 855–858. doi:10.1016/0040-4039(93)89031-K.{{cite journal}}: CS1 maint: multiple names: authors list (link)
  6. ^ a b c d Luzzio, F.A. (2001). "The Henry Reaction: recent examples". Tetrahedron. 57 (22): 915–945. doi:10.1002/chin.200122233.
  7. ^ Reich, Hans. "Bordwell pKa table: "Nitroalkanes"". University of Wisconsin Chemistry Department. Retrieved 17 January 2016.
  8. ^ Matthews, Walter; et al. (1975). "Equilibrium acidities of carbon acids. VI. Establishment of an absolute scale of acidities in dimethyl sulfoxide solution". Journal of the American Chemical Society. 97 (24): 7006. doi:10.1021/ja00857a010.
  9. ^ Bersohn, Malcolm (1961). "C versus O Alkylation in the Case of a Stable Cation". J. Am. Chem. Soc. 83 (9): 2136–2138. doi:10.1021/ja01470a022.
  10. ^ Begona, L., Arrieta, A., Morao, I., Cossio, F.P. (1997). "Ab Initio Models for the Nitroaldol (Henry) Reaction". Chem. Eur. J. 3 (1): 20–28. doi:10.1002/chem.19970030105.{{cite journal}}: CS1 maint: multiple names: authors list (link)
  11. ^ Sasai, Hiroaki; Suzuki, Takeyuki; Arai, Shigeru; Arai, Takayoshi; Shibasaki, Masakatsu (1 May 1992). "Basic character of rare earth metal alkoxides. Utilization in catalytic carbon-carbon bond-forming reactions and catalytic asymmetric nitroaldol reactions". Journal of the American Chemical Society. 114 (11): 4418–4420. doi:10.1021/ja00037a068.
  12. ^ a b c List et al. described this process as the organocatalyst functioning as Lewis acid or base or Brønsted acid or base.
  13. ^ Westermann, B. (2003). "Asymmetric catalytic aza-Henry reactions leading to 1,2-diamines and 1,2-diaminocarboxylic acids". Angew. Chem. Int. Ed. Engl. 42 (2): 151–153. doi:10.1002/anie.200390071. PMID 12532343.
  14. ^ Seayad, J., List, B. (2005). "Asymmetric organocatalysis". Org. Biomol. Chem. 3 (5): 719–724. doi:10.1039/b415217b. PMID 15731852.{{cite journal}}: CS1 maint: multiple names: authors list (link)
  15. ^ Menzel, A., Ohrlein, R., Griesser, H., Wehner, V., Jager, V. (1999). "A Short Synthesis of L-Acosamine Based on Nitroaldol Addition (Henry Reaction). Analysis of the Key Step Concerning Solvent and Temperature Effects". Synthesis. 9 (45): 1691–1702. doi:10.1002/chin.199945325.{{cite journal}}: CS1 maint: multiple names: authors list (link)
  16. ^ Palomo, Claudio; Oiarbide, Mikel; Laso, Antonio (2005). "Enantioselective Henry Reactions under Dual Lewis Acid/Amine Catalysis Using Chiral Amino Alcohol Ligands". Angewandte Chemie. 44 (25): 3881–3884. doi:10.1002/anie.200463075. PMID 15892142.
  17. ^ Alcaide, Benito; Almendros, Pedro; Luna, Amparo; Paz de Arriba, M.; Rosario Torresc, M. (2007). "Organocatalyzed diastereoselective Henry reaction of enantiopure 4-oxoazetidine-2-carbaldehydes" (PDF). Arkivoc. 2007 (iv): 285–296. doi:10.3998/ark.5550190.0008.425.
  18. ^ Gogoi, N., Boruwa, J., Barua, N.C. (2005). "A total synthesis of (–)-bestatin using Shibasaki's asymmetric Henry reaction". Tetrahedron Letters. 46 (44): 7581–7582. doi:10.1016/j.tetlet.2005.08.153.{{cite journal}}: CS1 maint: multiple names: authors list (link)
  19. ^ Marcelli, T., van der Haas, R., van Maarseveen, J.H., Hiemstra, H. (2006). "Asymmetric Organocatalytic Henry Reaction". Angew. Chem. Int. Ed. 45 (6): 929–931. doi:10.1002/anie.200503724. PMID 16429453.{{cite journal}}: CS1 maint: multiple names: authors list (link)
  20. ^ Purkarthofer, T., Gruber, K., Gruber-Khadjawi, M., Waich, K., Skranc, W., Mink, D. and Griengl, H. (2006). "A Biocatalytic Henry Reaction—The Hydroxynitrile Lyase from Hevea brasiliensis Also Catalyzes Nitroaldol Reactions". Angewandte Chemie. 45 (21): 3454–3456. doi:10.1002/anie.200504230. PMID 16634109.{{cite journal}}: CS1 maint: multiple names: authors list (link)
  21. ^ Fuhshuku K, Asano Y (2011). "Synthesis of (R)-β-nitro alcohols catalyzed by R-selective hydroxynitrile lyase from Arabidopsis thaliana in the aqueous-organic biphasic system". J. Biotechnol. 153 (3–4): 153–159. doi:10.1016/j.jbiotec.2011.03.011. PMID 21439333.

External links edit

  •   Media related to Category:Henry reaction at Wikimedia Commons

December 15, 2023
henry, reaction, this, article, technical, most, readers, understand, please, help, improve, make, understandable, experts, without, removing, technical, details, 2019, learn, when, remove, this, template, message, classic, carbon, carbon, bond, formation, rea. This article may be too technical for most readers to understand Please help improve it to make it understandable to non experts without removing the technical details May 2019 Learn how and when to remove this template message The Henry reaction is a classic carbon carbon bond formation reaction in organic chemistry Discovered in 1895 by the Belgian chemist Louis Henry 1834 1913 it is the combination of a nitroalkane and an aldehyde or ketone in the presence of a base to form b nitro alcohols 1 2 3 This type of reaction is also referred to as a nitroaldol reaction nitroalkane aldehyde and alcohol It is nearly analogous to the aldol reaction that had been discovered 23 years prior that couples two carbonyl compounds to form b hydroxy carbonyl compounds known as aldols aldehyde and alcohol 2 4 The Henry reaction is a useful technique in the area of organic chemistry due to the synthetic utility of its corresponding products as they can be easily converted to other useful synthetic intermediates These conversions include subsequent dehydration to yield nitroalkenes oxidation of the secondary alcohol to yield a nitro ketones or reduction of the nitro group to yield b amino alcohols Henry reactionNamed after Louis HenryReaction type Coupling reactionIdentifiersOrganic Chemistry Portal henry reactionRSC ontology ID RXNO 0000086 Henry reaction synthetic schemeMany of these uses have been exemplified in the syntheses of various pharmaceuticals including the b blocker S propranolol 5 6 the HIV protease inhibitor Amprenavir Vertex 478 and construction of the carbohydrate subunit of the anthracycline class of antibiotics L Acosamine 6 The synthetic scheme of the L Acosamine synthesis can be found in the Examples section of this article Contents 1 Mechanism 2 Stereochemical Course 3 General Features 4 Limitations 5 Modifications 6 Examples 7 References 8 External linksMechanism editThe Henry reaction begins with the deprotonation of the nitroalkane on the a carbon position forming a nitronate The pKa of most nitroalkanes is approximately 17 7 8 Although this structure is nucleophilic both at the deprotonated carbon and at the oxy anions of the nitro group 9 the observed result is of the carbon attacking the carbonyl compound The resulting b nitro alkoxide is protonated by the conjugate acid of the base that originally deprotonated the nitroalkyl structure giving the respective b nitro alcohol as product nbsp Henry reaction mechanismIt is important to note that all steps of the Henry reaction are reversible This is due to the lack of a committed step in the reaction to form product It is for this reason that research has been geared towards modifications to drive the reaction to completion 2 3 More information about this can be found in the modification section of this article Stereochemical Course editThe figure below illustrates one of the commonly accepted models for stereoselection without any modification to the Henry reaction In this model stereoselectivity is governed by the size of the R groups in the model such as a carbon chain as well as by a transition state that minimizes dipole by orienting the nitro group and carbonyl oxygen anti each other on opposite sides of the molecule The R groups play a role in the transition state of the Henry reaction the larger the R groups on each of the substrates the more they will tend to orient themselves away from each other commonly referred to as steric effects 3 10 nbsp Henry stereoselection without modificationDue to the reversibility of the reaction and the tendency for easy epimerization of the nitro substituted carbon atom among a number of factors the Henry reaction will typically produce a mixture of enantiomers or diastereomers It is for this reason that explanations for stereoselectivity remain scarce without some modification of the reaction 3 In recent years research focus has shifted toward modifications of the Henry reaction to overcome this synthetic challenge nbsp Henry reaction synthetic schemeThe first example of an enantioselective nitroaldol reaction was reported in 1992 using Shibasaki catalysts 11 One of the most frequently employed methods for inducing enantio or diastereoselectivity in the Henry reaction is the use of chiral metal catalysts in which the nitro group and carbonyl oxygen coordinate to a metal that is bound to a chiral organic molecule Some metals that have been used include zinc cobalt copper magnesium and chromium 12 A depiction of this coordination is illustrated above General Features editOne of the many features of the Henry reaction that makes it synthetically attractive is that it utilizes only a catalytic amount of base to drive the reaction Additionally a variety of bases can be used including ionic bases such as alkali metal hydroxides alkoxides carbonates and sources of fluoride anion e g TBAF or nonionic organic amine bases including TMG DBU DBN and PAP It is important to note that the base and solvent used do not have a large influence on the overall outcome of the reaction 2 Limitations editOne of the main drawbacks of the Henry reaction is the potential for side reactions throughout Aside from the inherent reversibility of the reaction or retro Henry that can prevent the reaction from proceeding the b nitro alcohol also has the potential to undergo dehydration For sterically hindered substrates it is also possible for a base catalyzed self condensation Cannizzaro reaction to occur A general scheme of the Cannizzaro reaction is depicted below 2 nbsp Cannizzaro Reaction SchemeModifications editThere have been a series of modifications made to the Henry reaction Of these some of the most important include employing high pressure and sometimes solvent free conditions to improve chemo and regioselectivity 2 and chiral metal catalysts to induce enantio or diastereoselectivity 12 The aza Henry reaction is also used to produce nitroamines and can be a reliable synthetic route for the synthesis of vicinal diamines 13 Perhaps one of the most synthetically useful modifications to the Henry reaction is the use of an organocatalyst 2 12 14 The catalytic cycle is shown below nbsp Henry reaction synthetic schemeBenjamin List described that while this is a broad explanation his brief review illustrates that this is a plausible mechanistic explanation for almost all reactions that involve an organocatalyst An example of this type of reaction is illustrated in the Examples section of this article In addition to the previously mentioned modifications to the Henry reaction there are a variety of others This includes the conversion of unreactive alkyl nitro compounds to their corresponding dianions which will react faster with carbonyl substrates reactions can be accelerated using PAP as base utilization of the reactivity of aldehydes with a a doubly deprotonated nitroalkanes to give nitronate alkoxides that yield mainly syn nitro alcohols once protonated and finally generation of nitronate anions in which one oxygenatom on the nitro group is silyl protected to yield anti b nitro alcohols in the presence of a fluoride anion source when reacted with an aldehyde 2 3 Examples editIndustrial Application In 1999 Menzel and coworkers developed a synthetic route to obtaining L acosamine the carbohydrate subunit of the anthracycline class of antibiotics 6 15 nbsp Acosamine scheme dd Industrial Application An enantioselective aldol addition product can be obtained in asymmetric synthesis by reaction of benzaldehyde with nitromethane and the a catalyst system consisting of zinc triflate as a Lewis acid diisopropylethylamine DIPEA and N methylephedrine NME as and as a chiral ligand 16 A diastereoselective variation of this reaction is depicted below 17 nbsp Henry reaction application dd Total Synthesis In 2005 Barua and coworkers completed the total synthesis of the potent aminopeptidase inhibitor bestatin in an overall yield of 26 overall yield employing Shibasaki s asymmetric Henry reaction as the key step illustrated below 6 18 nbsp Bestatin dd Organocatalysis In 2006 Hiemstra and coworkers explored the use of quinine derivatives as asymmetric catalysts for the reaction between aromatic aldehydes and nitromethane Through the use of particular derivatives they were able to induce direct enantioselection through the use of the proper catalyst 19 nbsp Chinchura dd Biocatalysis In 2006 Purkarthofer et al found that S hydroxynitrile lyase from Hevea brasiliensis catalyzes the formation of S b nitro alcohols 20 In 2011 Fuhshuku and Asano showed that the R selective hydroxynitrile lyase from Arabidopsis thaliana could catalyze the synthesis of R b nitro alcohols from nitromethane and aromatic aldehydes 21 References edit Henry Louis 1895 Formation synthetique d alcools nitres Synthetic formation of nitrated alcohols Comptes rendus 120 1265 1268 a b c d e f g h Kurti L Czako B 2005 Strategic Applications of Named Reactions in Organic Synthesis Burlington MA Elsevier Academic Press pp 202 203 ISBN 978 0 12 369483 6 a b c d e Noboro Ono 2001 The Nitro Group in Organic Synthesis New York NY Wiley VCH pp 30 69 ISBN 978 0 471 31611 4 Wurtz M A 1872 Sur un aldehyde alcool Bull Soc Chim Fr 17 436 442 Sasai H Suzuki T Itoh N Arai S Shibasaki M 1993 Catalytic Asymmetric Nitroaldol Reaction an efficient synthesis of s propranolol using the lanthenum binaphthol complex Tetrahedron Letters 34 52 855 858 doi 10 1016 0040 4039 93 89031 K a href Template Cite journal html title Template Cite journal cite journal a CS1 maint multiple names authors list link a b c d Luzzio F A 2001 The Henry Reaction recent examples Tetrahedron 57 22 915 945 doi 10 1002 chin 200122233 Reich Hans Bordwell pKa table Nitroalkanes University of Wisconsin Chemistry Department Retrieved 17 January 2016 Matthews Walter et al 1975 Equilibrium acidities of carbon acids VI Establishment of an absolute scale of acidities in dimethyl sulfoxide solution Journal of the American Chemical Society 97 24 7006 doi 10 1021 ja00857a010 Bersohn Malcolm 1961 C versus O Alkylation in the Case of a Stable Cation J Am Chem Soc 83 9 2136 2138 doi 10 1021 ja01470a022 Begona L Arrieta A Morao I Cossio F P 1997 Ab Initio Models for the Nitroaldol Henry Reaction Chem Eur J 3 1 20 28 doi 10 1002 chem 19970030105 a href Template Cite journal html title Template Cite journal cite journal a CS1 maint multiple names authors list link Sasai Hiroaki Suzuki Takeyuki Arai Shigeru Arai Takayoshi Shibasaki Masakatsu 1 May 1992 Basic character of rare earth metal alkoxides Utilization in catalytic carbon carbon bond forming reactions and catalytic asymmetric nitroaldol reactions Journal of the American Chemical Society 114 11 4418 4420 doi 10 1021 ja00037a068 a b c List et al described this process as the organocatalyst functioning as Lewis acid or base or Bronsted acid or base Westermann B 2003 Asymmetric catalytic aza Henry reactions leading to 1 2 diamines and 1 2 diaminocarboxylic acids Angew Chem Int Ed Engl 42 2 151 153 doi 10 1002 anie 200390071 PMID 12532343 Seayad J List B 2005 Asymmetric organocatalysis Org Biomol Chem 3 5 719 724 doi 10 1039 b415217b PMID 15731852 a href Template Cite journal html title Template Cite journal cite journal a CS1 maint multiple names authors list link Menzel A Ohrlein R Griesser H Wehner V Jager V 1999 A Short Synthesis of L Acosamine Based on Nitroaldol Addition Henry Reaction Analysis of the Key Step Concerning Solvent and Temperature Effects Synthesis 9 45 1691 1702 doi 10 1002 chin 199945325 a href Template Cite journal html title Template Cite journal cite journal a CS1 maint multiple names authors list link Palomo Claudio Oiarbide Mikel Laso Antonio 2005 Enantioselective Henry Reactions under Dual Lewis Acid Amine Catalysis Using Chiral Amino Alcohol Ligands Angewandte Chemie 44 25 3881 3884 doi 10 1002 anie 200463075 PMID 15892142 Alcaide Benito Almendros Pedro Luna Amparo Paz de Arriba M Rosario Torresc M 2007 Organocatalyzed diastereoselective Henry reaction of enantiopure 4 oxoazetidine 2 carbaldehydes PDF Arkivoc 2007 iv 285 296 doi 10 3998 ark 5550190 0008 425 Gogoi N Boruwa J Barua N C 2005 A total synthesis of bestatin using Shibasaki s asymmetric Henry reaction Tetrahedron Letters 46 44 7581 7582 doi 10 1016 j tetlet 2005 08 153 a href Template Cite journal html title Template Cite journal cite journal a CS1 maint multiple names authors list link Marcelli T van der Haas R van Maarseveen J H Hiemstra H 2006 Asymmetric Organocatalytic Henry Reaction Angew Chem Int Ed 45 6 929 931 doi 10 1002 anie 200503724 PMID 16429453 a href Template Cite journal html title Template Cite journal cite journal a CS1 maint multiple names authors list link Purkarthofer T Gruber K Gruber Khadjawi M Waich K Skranc W Mink D and Griengl H 2006 A Biocatalytic Henry Reaction The Hydroxynitrile Lyase from Hevea brasiliensis Also Catalyzes Nitroaldol Reactions Angewandte Chemie 45 21 3454 3456 doi 10 1002 anie 200504230 PMID 16634109 a href Template Cite journal html title Template Cite journal cite journal a CS1 maint multiple names authors list link Fuhshuku K Asano Y 2011 Synthesis of R b nitro alcohols catalyzed by R selective hydroxynitrile lyase from Arabidopsis thaliana in the aqueous organic biphasic system J Biotechnol 153 3 4 153 159 doi 10 1016 j jbiotec 2011 03 011 PMID 21439333 External links edit nbsp Media related to Category Henry reaction at Wikimedia Commons Retrieved from https en wikipedia org w index php title Henry reaction amp oldid 1161138363, wikipedia, wiki, book, books, library,

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