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Bischler–Napieralski reaction

November 27, 2023

The Bischler–Napieralski reaction is an intramolecular electrophilic aromatic substitution reaction that allows for the cyclization of β-arylethylamides or β-arylethylcarbamates. It was first discovered in 1893 by August Bischler and Bernard Napieralski [de], in affiliation with Basle Chemical Works and the University of Zurich. The reaction is most notably used in the synthesis of dihydroisoquinolines, which can be subsequently oxidized to isoquinolines.

Bischler-Napieralski reaction
Named after August Bischler
Bernard Napieralski
Reaction type Ring forming reaction
Identifiers
Organic Chemistry Portal bischler-napieralski-reaction
RSC ontology ID RXNO:0000053
A general scheme of the Bischler-Napieralski reaction.

Mechanisms edit

Two types of mechanisms have appeared in the literature for the Bischler–Napieralski reaction. Mechanism I involves a dichlorophosphoryl imine-ester intermediate, while Mechanism II involves a nitrilium ion intermediate (both shown in brackets). This mechanistic variance stems from the ambiguity over the timing for the elimination of the carbonyl oxygen in the starting amide.

 
A mechanism for the Bischler-Napieralski reaction involving an imine-ester intermediate.

In Mechanism I, the elimination occurs with imine formation after cyclization; while in Mechanism II, the elimination yields the nitrilium intermediate prior to cyclization. Currently, it is believed that reaction conditions affect the prevalence of one mechanism over the other (see reaction conditions).

 
A mechanism for the Bischler-Napieralski reaction involving a nitrilium intermediate.

In certain literature, Mechanism II is augmented with the formation of an imidoyl chloride intermediate produced by the substitution of chloride for the Lewis acid group just prior to the nitrilium ion. Because the dihydroisoquinoline nitrogen is basic, neutralization is necessary to obtain the deprotonated product.

General reaction reagents and conditions edit

The Bischler–Napieralski reaction is carried out in refluxing acidic conditions and requires a dehydrating agent. Phosphoryl chloride (POCl3) is widely used and cited for this purpose. Additionally, SnCl4 and BF3 etherate have been used with phenethylamides, while Tf2O and polyphosphoric acid (PPA) have been used with phenethylcarbamates. For reactants lacking electron-donating groups on the benzene ring, phosphorus pentoxide (P2O5) in refluxing POCl3 is most effective. Depending on the dehydrating reagent used, the reaction temperature varies from room temperature to 100 °C.

Related reactions edit

Several reactions that are related to the Bischler–Napieralski reaction are known. In the Morgan–Walls reaction, the linker between the aromatic ring and the amide nitrogen is an ortho-substituted aromatic ring. This N-acyl 2-aminobiphenyl cyclizes to form a phenanthridine. The Pictet–Spengler reaction proceeds from a β-arylamine via condensation with an aldehyde. These two components form an imine, which then cyclizes to form a tetrahydroisoquinoline.

Pictet–Gams reaction edit

The Pictet–Gams reaction proceeds from an β-hydroxy-β-phenethylamide. It involves an additional dehydration under the same conditions as the cyclization, giving an isoquinoline.[1][2] As with the Bischler–Napieralski reaction, the Pictet–Gams reaction requires a strongly dehydrating Lewis acid, such as phosphoryl chloride or phosphorus pentoxide.  

Structural effects and alternate products edit

There are documented variations on the Bischler–Napieralski reaction whose products differ in virtue of either the structure of the initial reactant, the tailoring of reaction conditions, or both. For example, research done by Doi and colleagues suggests that the presence or absence of electron-donating groups on the aryl portion of β-arylethylamides and the ratio of dehydrating reagents influence the patterns of ring closure via electrophilic aromatic substitution, leading to two possible products (see below). Other research on the variations on the Bischler-Napieralski Reaction have investigated the effects of nitro and acetal aryl groups on product formation (see references).

 
An example of mechanistic and product variation in the Bischler-Napieralski reaction. Treatment of N-[2-(4-methoxyphenyl)-ethyl]-4–methoxybenzamide with POCl3 results in the formation of the normal product, 7-methoxy-1-(4-methoxyphenyl)-3,4-dihydroisoquinoline. Treatment exclusively with P2O5 results in a mixture of the normal product and an unexpected product, 6-methoxy-1-(4-methoxyphenyl)-3,4-dihydroisoquinoline. The formation of the abnormal product is attributed to the cyclization via the ipso carbon on the phenyl ring to yield a spiro intermediate.

See also edit

References edit

  1. ^ "Pictet-Gams Synthesis". Comprehensive Organic Name Reactions and Reagents. 2010. pp. 2206–2209. doi:10.1002/9780470638859.conrr498. ISBN 9780470638859.
  2. ^ Fitton, Alan O.; Frost, Jonathan R.; Zakaria, Marwan M.; Andrew, Graham (1973). "Observations on the mechanism of the Pictet-Gams reaction". J. Chem. Soc., Chem. Commun. (22): 889–890. doi:10.1039/C39730000889.
  • August Bischler, Bernard Napieralski (1893). "Zur Kenntniss einer neuen Isochinolinsynthese". Berichte der Deutschen Chemischen Gesellschaft. 26 (2): 1903–1908. doi:10.1002/cber.189302602143.
  • Capilla, A. S.; Romero, M.; Pujol, M. D.; Caignard, D. H.; Renard, P. (2001). "Synthesis of isoquinolines and tetrahydroisoquinolines as potential antitumour agents". Tetrahedron. 57 (39): 8297. doi:10.1016/S0040-4020(01)00826-2.
  • Doi, S.; Shirai, N.; Sato, Y. (1997). "Abnormal products in the Bischler–Napieralski isoquinoline synthesis". J. Chem. Soc., Perkin Trans. 1 (15): 2217. doi:10.1039/a701332i.
  • Fodor, G. & Nagubandi, S. (1980). "Correlation of the von Braun, Ritter, Bischler-Napieralski, Beckmann and Schmidt reactions via nitrilium salt intermediates". Tetrahedron. 36 (10): 1279. doi:10.1016/0040-4020(80)85039-3.
  • Ishikawa, T.; Shimooka, K.; Narioka, T.; Noguchi, S.; Saito, T.; Ishikawa, A.; Yamazaki, E.; Harayama, T.; Seki, H.; Yamaguchi, K. J. (2000). "Anomalous Substituent Effects in the Bischler−Napieralski Reaction of 2-Aryl Aromatic Formamides". Org. Chem. 65 (26): 9143–9151. doi:10.1021/jo0012849. PMID 11149862.
  • Wang, X.-j.; Tan, J.; Grozinger, K. (1998). "A significantly improved condition for cyclization of phenethylcarbamates to N-alkylated 3,4-dihydroisoquinolones". Tetrahedron Lett. 39 (37): 6609. doi:10.1016/S0040-4039(98)01395-1.
  • Kitson, S. L. (2007). "Mechanism of the Bischler–Napieralski exocyclic and endocyclic dehydration products in the radiosynthesis of (R)-(−)-[6a-14C]apomorphine". Journal of Labelled Compounds and Radiopharmaceuticals. 50 (5–6): 290. doi:10.1002/jlcr.1270.
  • Lee, Jie J. (2007). Name Reactions: A Collection of Detailed Mechanisms and Synthetic Applications. Berlin, Heidelberg: Springer. doi:10.1007/978-3-642-01053-8. ISBN 978-3-642-01053-8.

November 27, 2023
bischler, napieralski, reaction, intramolecular, electrophilic, aromatic, substitution, reaction, that, allows, cyclization, arylethylamides, arylethylcarbamates, first, discovered, 1893, august, bischler, bernard, napieralski, affiliation, with, basle, chemic. The Bischler Napieralski reaction is an intramolecular electrophilic aromatic substitution reaction that allows for the cyclization of b arylethylamides or b arylethylcarbamates It was first discovered in 1893 by August Bischler and Bernard Napieralski de in affiliation with Basle Chemical Works and the University of Zurich The reaction is most notably used in the synthesis of dihydroisoquinolines which can be subsequently oxidized to isoquinolines Bischler Napieralski reactionNamed after August Bischler Bernard NapieralskiReaction type Ring forming reactionIdentifiersOrganic Chemistry Portal bischler napieralski reactionRSC ontology ID RXNO 0000053 A general scheme of the Bischler Napieralski reaction Contents 1 Mechanisms 2 General reaction reagents and conditions 3 Related reactions 3 1 Pictet Gams reaction 4 Structural effects and alternate products 5 See also 6 ReferencesMechanisms editTwo types of mechanisms have appeared in the literature for the Bischler Napieralski reaction Mechanism I involves a dichlorophosphoryl imine ester intermediate while Mechanism II involves a nitrilium ion intermediate both shown in brackets This mechanistic variance stems from the ambiguity over the timing for the elimination of the carbonyl oxygen in the starting amide nbsp A mechanism for the Bischler Napieralski reaction involving an imine ester intermediate In Mechanism I the elimination occurs with imine formation after cyclization while in Mechanism II the elimination yields the nitrilium intermediate prior to cyclization Currently it is believed that reaction conditions affect the prevalence of one mechanism over the other see reaction conditions nbsp A mechanism for the Bischler Napieralski reaction involving a nitrilium intermediate In certain literature Mechanism II is augmented with the formation of an imidoyl chloride intermediate produced by the substitution of chloride for the Lewis acid group just prior to the nitrilium ion Because the dihydroisoquinoline nitrogen is basic neutralization is necessary to obtain the deprotonated product General reaction reagents and conditions editThe Bischler Napieralski reaction is carried out in refluxing acidic conditions and requires a dehydrating agent Phosphoryl chloride POCl3 is widely used and cited for this purpose Additionally SnCl4 and BF3 etherate have been used with phenethylamides while Tf2O and polyphosphoric acid PPA have been used with phenethylcarbamates For reactants lacking electron donating groups on the benzene ring phosphorus pentoxide P2O5 in refluxing POCl3 is most effective Depending on the dehydrating reagent used the reaction temperature varies from room temperature to 100 C Related reactions editSeveral reactions that are related to the Bischler Napieralski reaction are known In the Morgan Walls reaction the linker between the aromatic ring and the amide nitrogen is an ortho substituted aromatic ring This N acyl 2 aminobiphenyl cyclizes to form a phenanthridine The Pictet Spengler reaction proceeds from a b arylamine via condensation with an aldehyde These two components form an imine which then cyclizes to form a tetrahydroisoquinoline Pictet Gams reaction edit The Pictet Gams reaction proceeds from an b hydroxy b phenethylamide It involves an additional dehydration under the same conditions as the cyclization giving an isoquinoline 1 2 As with the Bischler Napieralski reaction the Pictet Gams reaction requires a strongly dehydrating Lewis acid such as phosphoryl chloride or phosphorus pentoxide nbsp Structural effects and alternate products editThere are documented variations on the Bischler Napieralski reaction whose products differ in virtue of either the structure of the initial reactant the tailoring of reaction conditions or both For example research done by Doi and colleagues suggests that the presence or absence of electron donating groups on the aryl portion of b arylethylamides and the ratio of dehydrating reagents influence the patterns of ring closure via electrophilic aromatic substitution leading to two possible products see below Other research on the variations on the Bischler Napieralski Reaction have investigated the effects of nitro and acetal aryl groups on product formation see references nbsp An example of mechanistic and product variation in the Bischler Napieralski reaction Treatment of N 2 4 methoxyphenyl ethyl 4 methoxybenzamide with POCl3 results in the formation of the normal product 7 methoxy 1 4 methoxyphenyl 3 4 dihydroisoquinoline Treatment exclusively with P2O5 results in a mixture of the normal product and an unexpected product 6 methoxy 1 4 methoxyphenyl 3 4 dihydroisoquinoline The formation of the abnormal product is attributed to the cyclization via the ipso carbon on the phenyl ring to yield a spiro intermediate See also editPomeranz Fritsch reactionReferences edit Pictet Gams Synthesis Comprehensive Organic Name Reactions and Reagents 2010 pp 2206 2209 doi 10 1002 9780470638859 conrr498 ISBN 9780470638859 Fitton Alan O Frost Jonathan R Zakaria Marwan M Andrew Graham 1973 Observations on the mechanism of the Pictet Gams reaction J Chem Soc Chem Commun 22 889 890 doi 10 1039 C39730000889 August Bischler Bernard Napieralski 1893 Zur Kenntniss einer neuen Isochinolinsynthese Berichte der Deutschen Chemischen Gesellschaft 26 2 1903 1908 doi 10 1002 cber 189302602143 Capilla A S Romero M Pujol M D Caignard D H Renard P 2001 Synthesis of isoquinolines and tetrahydroisoquinolines as potential antitumour agents Tetrahedron 57 39 8297 doi 10 1016 S0040 4020 01 00826 2 Doi S Shirai N Sato Y 1997 Abnormal products in the Bischler Napieralski isoquinoline synthesis J Chem Soc Perkin Trans 1 15 2217 doi 10 1039 a701332i Fodor G amp Nagubandi S 1980 Correlation of the von Braun Ritter Bischler Napieralski Beckmann and Schmidt reactions via nitrilium salt intermediates Tetrahedron 36 10 1279 doi 10 1016 0040 4020 80 85039 3 Ishikawa T Shimooka K Narioka T Noguchi S Saito T Ishikawa A Yamazaki E Harayama T Seki H Yamaguchi K J 2000 Anomalous Substituent Effects in the Bischler Napieralski Reaction of 2 Aryl Aromatic Formamides Org Chem 65 26 9143 9151 doi 10 1021 jo0012849 PMID 11149862 Wang X j Tan J Grozinger K 1998 A significantly improved condition for cyclization of phenethylcarbamates to N alkylated 3 4 dihydroisoquinolones Tetrahedron Lett 39 37 6609 doi 10 1016 S0040 4039 98 01395 1 Kitson S L 2007 Mechanism of the Bischler Napieralski exocyclic and endocyclic dehydration products in the radiosynthesis of R 6a 14C apomorphine Journal of Labelled Compounds and Radiopharmaceuticals 50 5 6 290 doi 10 1002 jlcr 1270 Lee Jie J 2007 Name Reactions A Collection of Detailed Mechanisms and Synthetic Applications Berlin Heidelberg Springer doi 10 1007 978 3 642 01053 8 ISBN 978 3 642 01053 8 Retrieved from https en wikipedia org w index php title Bischler Napieralski reaction amp oldid 1097156368, wikipedia, wiki, book, books, library,

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