Source: http://orgsyn.org/demo.aspx?prep=v94p0034
Timestamp: 2019-04-19 00:30:57+00:00

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A. Pyrazinamide (1). A glass column reactor (Note 1) is packed with Celite (100 mg, Note 2) at the bottom end of the column, amorphous manganese dioxide (3.0 g, Note 3) in the middle section of the column, and Celite (100 mg) at the top end of the column (Note 4). The glass column reactor is mounted vertically in a heating jacket (Note 5) and connected to a pumping system flowing from the bottom to the top of the reactor column (Figure 1a) (Note 6). Polyfluoroalkoxy (PFA) tubing (1/16" OD x 0.040" (1.0mm) ID) is used to connect the feed source to the pump and to connect the pump to the bottom inlet of the reactor column. Wider bore PFA tubing (1/8" OD x 0.062" (1.55 mm) ID) is used to connect the top outlet of the reactor tube to the product collection vessel (Note 7). The reactor column containing the manganese dioxide catalyst is equilibrated by flowing solvent, H2O/ iPrOH (10:1 v/v), through the column at 1.6 mL/min at room temperature until the back pressure reaches a steady value (Note 8). The temperature of the column is then increased to 98 °C while continuing to flow H2O/ iPrOH (10:1 v/v) solvent through the reactor column at 1.6 mL/min. A 0.5 M solution of pyrazinecarbonitrile (2) (50.0 g, 476 mmol, Note 9) in H2O/iPrOH (10:1 v/v, 910 mL) is charged to a feed source bottle (Note 10).
Once the reactor column has equilibrated to a stable pressure (Note 11) and temperature of 98 °C the input to the pump is switched from solvent to the pyrazinecarbonitrile solution, and the pyrazinecarbonitrile solution is fed through the reactor at 1.6 mL/min while maintaining a reactor temperature of 98 °C (Figure 1b). The reactor output is collected in a clean vessel (Note 12) where pyrazinamide (1) precipitates as white solid. Once the entire pyrazinecarbonitrile solution is fed through the reactor (9.5 h), 20 mL of solvent, H2O/ iPrOH (10:1 v/v) is passed through the reactor at 98 °C and 1.6 mL/min. The combined effluent from flowing the pyrazinecarbonitrile solution and the subsequent H2O/ iPrOH (10:1 v/v) solvent wash is allowed to crystallize by standing 14 h at 5 °C (Note 13). The solid precipitate is filtered and dried in vacuo to furnish 56.2 g (97%) of pyrazinamide (1) as a fine white powder (Notes 14, 15 and 16) (Figure 2).
1. Omnifit glass column, 10.0 mm i.d. x 100.0 mm overall length.
2. Celite (AW Standard Super-Cel NF) was obtained from Sigma Aldrich and used as received.
3. Manganese(IV) dioxide (10 μm, reagent grade, ≥90%) was obtained from Sigma Aldrich and used as received.
4. Celite (0.1 g) is transferred into the Omnifit glass column; 3.0 g of Manganese(IV) dioxide are transferred into the reactor column and the material is packed into the column with just a gentle tapping. Another portion of Celite is then added (0.1 g) before closing the column with the frit end.
5. The column jacket allows heating from ambient to +150 °C, with precise temperature control; it accepts standard Omnifit glass columns (3 models for different Omnifit size ranges); two major safety aspects of the glass jacket are: the reaction is visible at all time and any hazard from column rupture is controlled by the shielding effect of the jacket itself.
6. A Vapourtec R2+/R4 flow reactor is used although any other system which could allow pumping an aqueous solution (with pressures up to 13 bar) and heating a column reactor can be used (e.g. Uniqsis, Phoenix ThalesNano, or Syrris flow reactors).
7. Wider bore tubing is used between the column exit and the effluent collection vessel to allow for precipitation of product in this line. The tubing outlet is held against the inner wall of the glass collection vessel to ensure that any precipitate does not build up at this point. The tubing is insulated using cotton wool and aluminum foil. The pressure was carefully monitored over time as the precipitation of the product in the outline (from the column to the receiver) may occur if the line was not well thermally isolated, that will cause fouling and clogging overtime. A back pressure regulator is NOT used after the reactor column.
8. At steady state, a back pressure of approximately 7 bar was observed; in some cases fluctuations between 5-10 bar were noticed. Typically 30 mL of solvent is required for equilibration.
9. Pyrazinecarbonitrile (99 % purity) was purchased from Sigma Aldrich and used as received. The submitters used pyrazinecarbonitrile (98% purity) purchased from Fluorochem Ltd.
10. The feed source bottle is a 1L glass bottle.
11. The pressure of the system ranges between 17-18 bar at operating conditions. The submitters report the pressure of the system ranged between 5-13 bar at operating conditions.
12. The collection bottle is a 1L glass bottle. Typically, to avoid precipitation within the reaction output, the tubing should be fixed to the inner side of the collection bottle allowing for the solution to flow down the bottle's inner wall rather than to drip.
13. Crystallization at room temperature provided isolated yields on the order of 75-78%, and the mother liquor and water wash showed that ~ 20% of pyrazinamide product remained in solution.
14. A second reaction on identical scale provided 55.2 g (95%) of the product as a white solid.
15. The sample for analysis was prepared as a solution in d6-DMSO in a J. Young NMR tube. White solid; mp 191-194 °C; 1H NMR pdf(600 MHz, d6-DMSO; 25 °C) δ: 7.88 (1 H, br s), 8.28 (1 H, br s), 8.72 (1 H, dd, J = 2.5, 1.6 Hz), 8.86 (1 H, d, J = 2.5 Hz), 9.21 (1 H, d, J = 1.6); 13C NMR pdf(100 MHz, d6-DMSO; 25 °C) δ: 143.8 (CH), 144.1 (CH), 145.5 (C), 147.8 (CH), 165.6 (C). FT-IR (neat, ν): 3422, 3132, 1669, 1583, 1525, 1481, 1432, 1373, 1171, 1089, 1046, 1021, 870, 791 cm-1.
16. Isolated product was analyzed by HPLC and weight assay was determined compared to a reference sample from Acros Organic (Lot A0355981). Weight % of products isolated was > 99.9 %. Column: Agilent Eclipse Plus 4.6 mm x 50 mm, observed at 254 nm, with flow rate of 1.4 mL/min. Method : Solvent A : water, Solvent B : Acetonitrile. Time : 0 min, % B : 10; 4 min, % B: 25; 6 min, %B: 45; 9 min, %B: 98; 12 min, %B : 98. Retention time = 1.05 min.
Pyrazinamide is an active pharmaceutical ingredient (API) for the treatment of tuberculosis.3 A number of syntheses have been developed to produce this compound in good purity. However, most of these syntheses require multi-step processes that have significant economic disadvantages. For example, in the patent GB 451304,4 the preparation begins with condensation of o-phenylenediamine and glyoxal to provide quinoxaline. The carbocyclic aromatic ring is then oxidized to yield heterocyclic dicarboxylic acid. Decarboxylation followed by esterification and ammonolysis of the ester provide the desired product over several steps.
The preparation of primary amides5,6 remains a practically problematic transformation, especially on large industrial scale.7 The most environmentally-friendly way to obtain primary amides is via hydration of nitriles. Despite the several methods that have been developed to perform this transformation, there are specific drawbacks associated with the existing protocols. For instance, acid or base catalyzed hydration is affected by over-hydrolysis or byproduct formation.5,8,9 Relatively mild conditions are used for the homogeneous metal catalyzed10 hydration of nitriles to primary amides, although issues associated with purification and cost-effectiveness of the process itself may hinder implementation.
Indeed, MnO2 has been known as a low-cost and useful reagent for its oxidative properties.13 Previous work had identified MnO2 as active catalyst for the hydration of nitriles.14 Nevertheless, the procedures reported require high temperature (>140 oC) and laborious work up procedures, especially on scale.
Innovative Technology Centre, Department of Chemistry, University of Cambridge, Lensfield Road, Cambridge, CB2 1EW, UK. Prof Steven V Ley, email: svl1000@cam.ac.uk. We are grateful to Pfizer Worldwide Research and Development (CB), the Croucher Foundation and Cambridge Trust (SHL) and the EPSRC (SVL, grant n° EP/K009494/1 and EP/M004120/1) for financial support.
Pfizer Worldwide Research and Development, Eastern Point Road, Groton, Connecticut 06340, USA.
(a) World Health Organization (WHO), WHO Report 2010: Global Tuberculosis Control, 2010. (b) Shi, W.; Zhang, X.; Jiang, X.; Yuan, H.; Lee, J. S.; Barry, C. E., III; Wang, H.; Zhang, W. and Zhang Y. Science, 2011, 333, 1630-1632.
Merck, K.; Merck, W.; Merck, L. and Merck, F. Process for the manufacture of new derivatives of pyrazinemoncarboxylic acid, GB Patent 451304-A, Jun 12, 1935.
Dugger, R. W.; Ragan, J. A.; Ripin, D. H. B. Org. Process Res. Dev. 2005, 9, 253-258.
Carey, J. S., Laffan, D.; Thomson, C.; Williams, M. T. Org. Biomol. Chem. 2006, 4, 2337-2347.
Constable, D. J. C.; Dunn, P. J.; Lorenz, K.; Manley, J.; Pearlman, B. A.; Wells, A.; Zals, A.; Zhang, T. Y. Green Chem. 2007, 9, 411-420.
(a) Bailey, P. D.; Mills, T. J.; Pettecrew, R.; Price, R. A. Om Comprehensive Organic Functional Group Transformations II; Katritzky, A. R., Taylor, R. J. K., Eds.; Elsevier: Oxford, 2005; Vol. 5, pp 201-294. (b) Valeur, E.; Bradley, M. Chem. Soc. Rev. 2009, 38, 606-631.
(a) Steynberg, P. J.; Denga, Z.; Stryn, R.; Bezuidenhout, B. C.; Stark, N. L. Production of amides and/or acids from nitriles, World Patent 2000026178 A1, May 11, 2000. (b) Edward, J. T., Meacock, S. C. R. J. Chem. Soc. 1957, 2000-2007.
(a) García-Á lvarez, R.; Crochet, P.; Cadierno, V. Green Chem. 2013, 15, 46-66. (b) Breno, K. L.; Pluth, M. D.; Tyler, D. R. Organometallics 2003, 22, 1203-1211. (c) García-Alvarez, R.; Díez, J.; Crochet, P.; Cadierno, V. Organometallics 2011, 30, 5442-5451. (d) Cadierno, V.; Francos, J.; Gimeno, J. Chem. Eur. J. 2008, 14, 6601-6605. (e) Ahmed, T. J.; Fox, B. R.; Knapp, S. M. M.; Yelle, R. B.; Juliette, J. J.; Tyler, D. R. Inorg. Chem. 2009, 48, 7828-7837. (f) Ramon, R. S.; Marion, N.; Nolan, S. P. Chem.Eur. J. 2009, 15, 8695-8697. (g) Lee, W.-C.; Frost, B. J. Green Chem. 2012, 14, 62-66. (h) Yamada, H.; Nagasawa, T.; Ann. N. Y. Acad. Sci. 1990, 613, 142-154.
(a) Yamaguchi, K.; Matsushita, M.; Mizuno, N. Angew. Chem. 2004, 116, 1602-1606. (b) Mitsudome, T.; Mikami, Y.; Mori, H.; Arita, S.; Mizugaki, T.; Jitsukawa, K.; Kaneda, K. Chem. Commun. 2009, 3258-3260. (c) Liu, Y.- M.; He, L.; Wang, M.-M.; Cao, Y.; He, H.-Y.; Fan, K.-N. ChemSusChem 2012, 5, 1392-1396. (d) Farrar, D.; Flesher, P., Hydration of nitriles, U.S. Patent 4,543,423, Sept 24, 1985. (e) Wilgus, C. P.; Downing, S.; Molitor, E.; Bains, S.; Pagni, R. M.; Kabalka, G. W. Tetrahedron Lett. 1995, 36, 3469-3472. (f) Rao, C. G. Synth. Commun. 1982, 12, 177-181. (g) Sebti, S.; Rhiil, A.; Saber, A.; Hanafi, N. Tetrahedron Lett. 1996, 37, 6555-6556. (h) Tamura, M.; Wakasugi, H.; Shimizu, K.-i.; Satsuma, A. Chem. Eur. J. 2011, 17, 11428-11431. (i) Mori, K.; Yamaguchi, K.; Mizugaki, T.; Ebitani, K.; Kaneda, K. Chem. Commun. 2001, 461-462. (j) Kim, A. Y.; Bae, H. S.; Park, S.; Park, S.; Park, K. H. Catal. Lett. 2011, 141, 685-690. (k) Polshettiwar, V.; Varma, R. S. Chem. Eur. J. 2009, 15, 1582-1586. (l) Subramanian, T.; Pitchumani, K. Catal. Commun. 2012, 29, 109-113. (m) Shimizu, K.; Kubo, T.; Satsuma, A.; Kamachi, T.; Yoshizawa, K. ACS Catal. 2012, 2, 2467-2474. (n) Baig, R. B. N.; Varma, R. S. Chem. Commun. 2012, 48, 6220-6222. (o) Bazi, F.; El Badaoui, H.; Tamani, S.; Sokori, S.; Solhy, A.; Macquarrie, D. J.; Sebti, S. Appl. Catal., A 2006, 301, 211-214. (p) Kumar, S.; Das, P. New J. Chem. 2013, 37, 2987-2990. (q) Shimizu, K.; Imaiida, N.; Sawabe, K.; Satsuma, A. Appl. Catal., A 2012, 114, 421-422, 114-120. (r) Hirano, T.; Uehara, K.; Kamata, K.; Mizuno, N. J. Am. Chem. Soc. 2012, 134, 6425-6433.
Battilocchio, C.; Hawkins, J. M.; Ley, S. V. Org. Lett. 2014, 16, 1060-1063.
(a) Fatiadi, A. J. Synthesis 1976, 2, 65-104. (b) Taylor, R. J. K.; Reid, M.; Foot, J.; Raw, S. A. Acc. Chem. Res. 2005, 38, 851-869. (c) Soldatenkov, A. T.; Polyanskii, K. B.; Kolyandina, N. M.; Soldatova, S. A. Chem. Heterocycl. Compd. 2009, 45, 633-657.
(a) Breuilles, P.; Leclerc, R.; Uguen, D. Tetrahedron Lett. 1994, 35, 1401-1404. (b) Liu, K.-T.; Shih, M.-H.; Huang, H.-W.; Hu, C.-J. Synthesis 1988, 715-717. (c) Haefele, L. R.; Young, H. J. Ind. Eng. Chem. Prod. Res. Develop. 1972, 11, 364-365. (d) Roy, S. C.; Dutta, P.; Nandy, L. N.; Roy, S. K.; Samuel, P.; Pillai, S. M.; Kaushik, V. K.; Ravindranathan, M. Appl. Catal., A 2005, 290, 175-180. (e) Shen, C. H.; Lee, C. Y.; Tsai, C. J. Process for producing organic carboxylic acid amides, U.S. Patent 2011/ 0004020 A1, Jan 6, 2011. (f) Yamaguchi, K.; Wang, Y.; Kobayashi, H.; Mizuno, N. Chem. Lett. 2012, 41, 574-576. (g) Yamaguchi, K.; Wang, Y.; Mizuno, N. Chem. Lett. 2012, 41, 633-635.
Alfonsi, K.; Colberg, J.; Dunn, P. J.; Febig, T.; Jennings, S.; Johnson, T. A.; Kleine, H. P., Knight, C.; Nagy, M. A.; Perry, D. A.; Stefaniak, M. Green Chem. 2008, 10, 31-36.
(a) Habermann, J.; Ley, S. V.; Smits, R. J. Chem. Soc., Perkin Trans. 1 1999, 2421-2423. (b) Ley, S. V.; Baxendale, I. R.; Nesi, M.; Piutti, C. Tetrahedron 2002, 58, 6285-6304. (c) Ley, S. V.; Baxendale, I. R.; Lee, A. L. J. Chem. Soc., Perkin Trans. 1 2002, 16, 1850-1857. (d) Nikbin, N.; Ladlow, M.; Ley, S. V. Org. Process Res. Dev. 2007, 11, 458-462. (e) Baumann, M.; Baxendale, I. R.; Ley, S. V.; Nikbin, N.; Smith, C. D. Org. Biomol. Chem. 2008, 6, 1587-1593. (f) Smith, C. J.; Smith, C. D.; Nikbin, N.; Ley, S. V.; Baxendale, I. R. Org. Biomol. Chem. 2011, 9, 1927-1937. (g) Ingham, R. J.; Riva, E.; Nikbin, N.; Baxendale, I. R.; Ley, S. V. Org. Lett. 2012, 14, 3920-3923. (h) Battilocchio, C.; Deadman, B. J.; Nikbin, N.; Kitching, M. O.; Baxendale, I. R.; Ley, S. V. Chem. Eur. J. 2013, 19 , 7917-7930. (i) Battilocchio, C.; Hawkins, J. M.; Ley, S. V. Org. Lett. 2013, 15, 2278-2281. (j) Chorghade, R.; Battilocchio, C.; Hawkins, J. M.; Ley, S. V. Org. Lett. 2013, 15, 5698-5701.
(a) Wegner, J.; Ceylan, S.; Kirschning, A. Adv. Synth. Catal. 2012, 354, 17-57. (b) Hartman, R. L.; McMullen, J. P.; Jensen, K. F. Angew. Chem., Int. Ed. 2011, 50, 7502-7519. (c) Hessel, V. Chem. Eng. Technol. 2009, 32, 1655-1681.
Claudio Battilocchio received his bachelor degree from La Sapienza in 2008 and started his Ph.D. studies with Prof Mariangela Biava in 2009, researching the development of novel molecular hybrids. In 2011, he was a visiting Ph.D. student in the Innovative Technology Centre at the University of Cambridge working with enabling technologies. After a 3-year research position at the University of Cambridge working on the Open Innovation Programme with Pfizer Worldwide R&D, Claudio is now a research associate at Homerton College, working in the Ley group on a Collaborative Programme with Syngenta to explore new synthetic enabling tools.
Shing-Hing Lau obtained his M.Sc. Chemistry with a year in industry (AkzoNobel N.V.) from Imperial College London in 2013, working on natural product synthesis for his master's project. In the same year he was awarded a Croucher Cambridge International Scholarship to pursue Ph.D. studies at the University of Cambridge under the supervision of Professor Steven Ley. His research focused on the development of sustainable processes using flow chemistry.
Joel Hawkins received his Ph.D. at MIT in 1986 with Professor Barry Sharpless. He went on to become an NIH Postdoctoral Fellow at Caltech with Professor Robert Grubbs. As an Assistant Professor at the University of California at Berkeley from 1987 to 1993, he studied asymmetric Diels-Alder catalysts and fullerene chemistry. In 1993, he moved to Pfizer where he is a Senior Research Fellow in Chemical Research and Development and is particularly interested in the development and application of new technologies for pharmaceutical process research and development.
Steven Ley is currently Professor of Chemistry and Director of Research at the University of Cambridge. He is also a Fellow of Trinity College and was BP 1702 Professor of Chemistry for 21 years. He was appointed as a lecturer at Imperial College in 1975, promoted to Professor in 1983, and became Head of Department there in 1989. In 1990 he was elected to the Royal Society (London) and was President of The Royal Society of Chemistry from 2000-2002. Steve's research interests span many disciplines including new synthetic methodologies, the total synthesis of natural products and the development of enabling technologies. He has published over 800 papers and has been honored with 50 major awards.
Dr. Andrew Brusoe was born and raised in Toledo, Ohio. He received his Bachelor's degree at Albion College before earning his Ph.D. in organic chemistry in 2013 from the University of North Carolina at Chapel Hill working under Erik Alexanian. After completion of his degree Andrew was a postdoctoral researcher for John Hartwig at UC Berkeley. Andrew joined the process research flow chemistry group at Boehringer Ingelheim in October in 2015. Outside of work Andrew enjoys running, hiking, and roasting and brewing specialty coffee.
Dr. Frederic Buono has 12 years of experience in Pharmaceutical Industry and he is currently working in Boehringer Ingelheim. He is originally from France, where he got his Ph.D. in organic chemistry and chemical engineer degree from "Ecole Centrale de Marseille". He moved to England to do his postdoctoral with Prof. Donna Blackmond, where he worked in the area of physical organic chemistry and developed several kinetic models of organic reactions mechanisms. Prior to Boehringer, he started his career with Bristol Myers Squibb, in the Process Group. In his current position, he is developing and implementing continuous flow technology for several projects on multi-kilogram scale process, by using in-situ monitoring techniques and kinetic studies.

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