Chemoselective Reactions of 4,6-Dichloro-2-(methylsulfonyl)pyrimidine and Related Electrophiles with Amines

 

 Buy Article Permissions and Reprints All articles of this category

Dedicated to Prof. Scott E. Denmark on the occasion of his 60^th birthday

Abstract

Chemoselective S_NAr reactions of 4,6-dichloro-2-(methylsulfonyl)pyrimidine and several related electrophiles with amines and their derivatives are described. In the presence of weak bases anilines and secondary aliphatic amines selectively displace the chloride group. Deprotonated anilines and their carbonyl derivatives displace the sulfone group. Sterically and electronically unbiased primary aliphatic amines selectively displace the sulfone group in 4,6-dichloro-2-(methylsulfonyl)pyrimidine; however, their reactions with other electrophiles generally are less selective. Steric-driven selectivity explanation was proposed.

• References

• 1a Sanford M. Drugs 2012; 72: 525
  Crossref
• 1b Croxtall JD. Drugs 2012; 72: 847
  Crossref
• 2 Sonpavde G, Hutson TE, Sternberg CN. Drugs Today 2009; 45: 651
  Crossref
• 3a Sabat M, VanRens JC, Laufersweiler MJ, Brugel TA, Maier J, Golebiowski A, De B, Easwaran V, Hsieh LC, Walter RL, Mekel MJ, Evdokimov A, Janusz MJ. Bioorg. Med. Chem. Lett. 2006; 16: 5973
  Crossref
• 3b Gong B, Hong F, Kohm C, Jenkins S, Tulinsky J, Bhatt R, de Vries P, Singer JS, Klein P. Bioorg. Med. Chem. Lett. 2004; 14: 2303
  Crossref
• 3c Yang W, AbdulHameed MD. M, Hamza A, Zhan C.-G. Bioorg. Med. Chem. Lett. 2012; 22: 1629
  Crossref
• 4 Sagi VN, Liu T, Lu X, Bartfai T, Roberts E. Bioorg. Med. Chem. Lett. 2011; 21: 7210
  Crossref
• 5 Deng X, Nagle A, Wu T, Sakata T, Henson K, Chen Z, Kuhen K, Plouffe D, Winzeler E, Adrian F, Tuntland T, Chang J, Simerson S, Howard S, Ek J, Isbell J, Tully DC, Chatterjee AK, Gray NS. Bioorg. Med. Chem. Lett. 2010; 20: 4027
  Crossref
• 6 Rivkin A, Ahearn SP, Chichetti SM, Kim YR, Li C, Rosenau A, Kattar SD, Jung J, Shah S, Hughes BL, Crispino JL, Middleton RE, Szewczak AA, Munoz B, Shearman MS. Bioorg. Med. Chem. Lett. 2010; 20: 1269
  Crossref
• 7 Kumagai T, Okubo T, Kataoka-Okubo H, Chaki S, Okuyama S, Nakazato A. Bioorg. Med. Chem. 2001; 9:  1349
  Crossref
• 8 Gu S, Yang S, He Q, Ma X, Chen F, Dai H, De Clercq E, Balzarini J, Pannecouque C. Bioorg. Med. Chem. 2011; 19: 7093
  Crossref
• 9a Delia TJ, Meltsner BR, Schomaker JM. J. Heterocycl. Chem. 2000; 37: 1457
  Crossref
• 9b Matsuno T, Kato M, Sasahara H, Watanabe T, Inaba M, Takahashi M, Yaguchi S, Yoshioka K, Sakato M, Kawaseima S. Chem. Pharm. Bull. 2000; 48: 1778
  Crossref
• 9c Delia TJ, Meltsner BR, Schomaker JM. J. Heterocyl. Chem. 1999; 36: 1259
  Crossref
• 9d Montebugnoli D, Bravo P, Corradi E, Dettori G, Mioskowski C, Volonterio A, Wagner A, Zanda M. Tetrahedron 2002; 58: 2147
  Crossref
• 9e Zanda M, Talaga P, Wagner A, Mioskowski C. Tetrahedron Lett. 2000; 41: 1757
  Crossref
• 10a D’Atri G, Gomarasca P, Resnati G, Tronconi G, Scolastico C, Sirtori CR. J. Med. Chem. 1984; 27: 1621
  Crossref
• 10b Wernert GT, Winkler DA, Holan G, Nicoletti G. Aust. J. Chem. 2004; 57: 77
  Crossref
• 11 Kopell HC, Springer RH, Cheng CC. J. Org. Chem. 1961; 26: 1884
  Crossref
• 12a Martin RE, Morawitz F, Kuratli C, Alker AM, Alanine AI. Eur. J. Org. Chem. 2012; 47
• 12b Huang T.-H, Tu H.-Y, Aibibu Z, Hou C.-J, Zhang A.-D. ARKIVOC 2011; (ii): 1
• 13 Bebbington D, Binch H, Charrier J.-D, Everitt S, Fraysse D, Golec J, Kay D, Knegtel R, Mak C, Mazzei F, Miller A, Mortimore A, O’Donnell M, Patel S, Pierard F, Pinder J, Pollard J, Ramaya S, Robinson D, Rutherford A, Studley J, Westcott J. Bioorg. Med. Chem. Lett. 2009; 19: 3586
  Crossref
• 14 Xiao X.-Y, Patel DV, Ward JS, Bray MR, Agoston GE, Treston AM. WO 2007041358, 2007
• 15 Medina JR, Becker CJ, Blackledge CW, Duquenne C, Feng Y, Grant SW, Heerding D, Li WH, Miller WH, Romeril SP, Scherzer D, Shu A, Bobko MA, Chadderton AR, Dumble M, Gardiner CM, Gilbert S, Liu Q, Rabindran SK, Sudakin S, Xiang H, Brady PG, Campobasso N, Ward P, Axten JM. J. Med. Chem. 2011; 54: 1871
  Crossref
• 16 Eriksen BL, Hougaard C, Peters D, Christophersen P. WO 2010026087, 2010
• 17 Nagata T, Masuda K, Maeno S, Miura I. Pest Manage. Sci. 2004; 60: 399
  Crossref
• 18 Ji M, Zheng Y, Zheng M. CN 101857589, 2010
• 19 One such byproduct was identified using LC-MS analysis as 2.1 ([M + H]⁺ 430, see Scheme 3). It seems that the N–H in 2a is acidic enough to be deprotonated by stronger bases (such as aliphatic amines or K₂CO₃) and displaces the sulfone in 1, which seems to be the preferred site of displacement by anionic nucleophiles (vide infra).
• 20 A ¹H NMR experiment (data not shown) demonstrated that pyridine reacts with 1 within minutes at r.t. in DMSO-d ₆ to provide a complex mixture of products.
• 21 The reaction is less general with these amines. Many heteroaromatic and all heterocyclic amines that we tested reacted unselectively, with substitution occurring at both C2 and C4, as well as forming multiple other byproducts. Unselective examples include 2-, 3-, or 4-aminopyridine, 2-aminothiazole, etc. Imidazole and benzimidazole preferentially react at C2.
• 22 See Supporting Information for details.
• 23 When indole was combined with 1 in DMSO in the presence of 2,6-lutidine (1.2 equiv), after 3 d at r.t. side products started forming according to LC-MS analysis of the reaction mixture. At that point LC-MS analysis failed to demonstrate formation of either the C4–Cl or the C2–SO₂Me displacement products.
• 24 Preliminary data suggests that the higher acidity of heterocyclic aromatic amines may be a reason for some of these reactions being unselective. Both neutral and deprotonated species may coexist and react with 1 via different pathways.
• 25a With aziridine: see ref. 11.
• 25b With methylamine: see ref. 15.
• 25c With alkoxide: see ref. 12a.
• 25d With thiolate: see ref. 13.
• 25e With RMgX: see ref. 14
• 25f With deprotonated formamide: see ref. 17
• 25g With deprotonated heterocyclic amine: see ref. 16.
• 26 Slightly lower yields were generally obtained when PhLi/Et₂O or i-PrMgCl·LiCl/THF were used instead of NaHMDS.
• 27 One such side product was isolated and identified as V (see Scheme 4). Its formation may be explained by the mechanism shown in the scheme that starts with the deprotonation of 1. Product V was the major product (38%) isolated when cyclohexylamine was combined with NaHMDS and 1. Analytical data for V: white solid, LC-MS (ESI) [M + H]⁺ 311 (4 Cl atoms pattern); ¹H NMR (500 MHz, DMSO-d ₆): δ = 8.00 (s, 2 H), 4.57 (s, 2 H); ¹³C NMR (126 MHz, DMSO-d ₆): δ = 167.5, 161.3, 120.0, 47.3.
• 28 Similar reaction has been reported in ref. 8f.
• 29 Reaction with Boc-protected pyridin-3-ylmethanamine did not provide the clean product even though the reaction was moderately clean according to the LC-MS analysis of the reaction mixture. The product seems to be unstable.
• 30 The byproduct (Figure 1) was identified as the product of bis-arylation of the amine with 1 based on LC-MS analysis. This reaction was not optimized.
• 31 Unfortunately, reactions with deprotonated N-alkylanilines, such as N-methylaniline or indoline (NaHMDS, TMPMgCl·LiCl, n-BuLi; various modes of addition) were not clean. These reactions produced mixtures of products, with displacements at C2, C4 and double C2 and C4 displacement, as well as other unidentified byproducts.
• 32 The alternate products 4a–c or 5e,f could be detected by LC-MS or ¹H NMR analysis of the reaction mixtures. However, these minor products could be isolated only in impure form and negligible amounts.
• 33 Henne AL, Stewart JJ. J. Am. Chem. Soc. 1955; 77: 1901
  Crossref
• 34 Kanzian T, Nigst TA, Maier A, Pilch S, Mayr H. Eur. J. Org. Chem. 2009; 6379
• 35 Various modes of addition and stoichiometries were tried unsuccessfully.
• 36a With 3-chloro-6-(methylsulfonyl)-1,2-diazine and 4-chloro-6-(methylsulfonyl)pyrimidine: Nyberg WH, Cheng CC. J. Heterocyl. Chem. 1964; 1: 1
  Crossref
• 36b With 4-chloro-2-(ethylsulfonyl)-6-phenylpyrimidine and 4-chloro-2-(ethylsulfonyl)pyrimidine: Sawayama T, Yamamoto R, Kinugasa H, Nishimura H. Heterocycles 1977; 8: 299
  Crossref
• 37 See experimental section for details.
• 38 Some limited information is also available on reactions with 4-chloro-6-(ethylsulfonyl)pyrimidine (see ref. 19b) and 4-chloro-6-(propylsulfonyl)pyrimidine, see: Porter JR, Archibald SC, Brown JA, Childs K, Critchley D, Head JC, Hutchinson B, Parton TA. H, Robinson MK, Shock A, Warrellow GJ, Zomaya A. Bioorg. Med. Chem. Lett. 2002; 12: 1595
  Crossref
• 39 Calculations were conducted using Spartan software, B3LYP 6-31G* in DMSO.
• 40 In anilines the NH₂-group is planarized. This may lead to anilines being effectively bulkier compared to, for example, CyNH₂.
• 41 This conclusion is similar to the one made earlier; see ref. 19b.
• 42 Assigned based on the LC-MS data.

• Supplementary Material