- 概述
6-氯-2,3-二氨基吡啶是一种有机中间体,可由2-氨基-3-硝基-6-氯吡啶通过一步还原制备得到。
- 6-氯-2,3-二氨基吡啶是有机合成中间体和医药中间体,可用于实验室研发过程和化工医药合成过程中。
- 制备
将2-氨基-3-硝基-6-氯吡啶(500g,2.89mol),氯化铵(300g,5.75mol)溶解于5000ml乙酸乙酯和 3000ml的水中,室温下向此混合溶液中加入铁粉(482.5g,8.65mol),室温反应4小时,TLC检 测反应完全,将反应液过滤,滤液分层后,水相用乙酸乙酯1500ml萃取2次,合并有有机相,并用饱和食盐水干燥,浓缩得化合物6-氯-2,3-二氨基吡啶(370g,2.58mol),收率89.2%。
有机合成中间体; 医药中间体
合成路线 1(1. 合成:40851-95-4)
产率:95.6%
合成条件:With hydrogen In methanol at 20℃; for 24 h;
实验步骤:将6-氯-2-硝基吡啶-3-胺(E-23)(8.8g,51mmol,1.0当量)和阮内镍(0.88g)在甲醇(100mL)中的混合物在氢气下在室温下搅拌24小时。 然后过滤,将滤液真空浓缩,得到所需产物6-氯吡啶-2,3-二胺(E-24)(7g,95.6%收率),为苍白色固体。 ESI-MS m / z:144.05 [M + H] +。
参考文献:
- [1] Patent: WO2011/149937, 2011, A1. Location in patent: Page/Page column 40; 41; 84 [2] Patent: WO2013/78441, 2013, A1. Location in patent: Paragraph 00143; 00326 [3] Patent: WO2014/151147, 2014, A1. Location in patent: Paragraph 00641 [4] Patent: US2015/30588, 2015, A1. Location in patent: Page/Page column 66 [5] Patent: US9295673, 2016, B2. Location in patent: Page/Page column 341; 342
合成路线 2(2. 合成:40851-95-4)
产率:91%
合成条件:With iron; ammonium chloride In water; isopropyl alcohol at 90℃; for 1 h;
实验步骤:a)6-氯吡啶-2,3-二胺(A45)将铁粉(9.65g,173mmol)加入到6-氯-3-硝基吡啶-2-胺A44(10.0g,57.6mmol)和NH 4 Cl的悬浮液中 (6.16g,115mmol)在异丙醇(180mL)和水(90mL)中的溶液。 将所得混合物在90℃下加热1小时。 此后,将悬浮液冷却至室温,然后用EtOAc(100mL)稀释,通过硅藻土过滤,并将残余物用另外的EtOAc(2×150mL)洗涤。 将滤液用水(3×100mL),盐水(100mL)洗涤,经Na 2 SO 4干燥,并在减压下除去挥发物,得到标题化合物(7.50g,91%),为深棕色固体。 1 H NMR(400MHz,cfe-DMSO)δ6.68(d,J = 7.8Hz,1H),6.35(d,J = 7.8Hz,1H),5.78(s,2H),4.76(s,2H)。
参考文献:
- [1] Patent: WO2014/128465, 2014, A1. Location in patent: Page/Page column 73; 74 [2] Catalysis Communications, 2015, vol. 67, p. 64 - 67 [3] Patent: CN104860943, 2017, B. Location in patent: Paragraph 0038-0042 [4] Patent: WO2009/27732, 2009, A1. Location in patent: Page/Page column 68 [5] Patent: WO2012/80449, 2012, A1. Location in patent: Page/Page column 25-26 [6] Patent: WO2013/186335, 2013, A1. Location in patent: Page/Page column 85 [7] Patent: WO2014/114776, 2014, A1. Location in patent: Page/Page column 34 [8] Organic and Biomolecular Chemistry, 2017, vol. 15, # 6, p. 1313 - 1316 [9] Journal of Organic Chemistry, 2014, vol. 79, # 3, p. 852 - 866 [10] European Journal of Organic Chemistry, 2016, vol. 2016, # 14, p. 2421 - 2434 [11] Journal of Medicinal Chemistry, 2000, vol. 43, # 16, p. 3052 - 3066 [12] Helvetica Chimica Acta, 2007, vol. 90, # 6, p. 1043 - 1068 [13] Patent: WO2006/24666, 2006, A1. Location in patent: Page/Page column 48 [14] Collection of Czechoslovak Chemical Communications, 1991, vol. 56, # 11.1, p. 2420 - 2429 [15] Journal of Medicinal Chemistry, 1996, vol. 39, # 6, p. 1331 - 1338 [16] Bioorganic and Medicinal Chemistry Letters, 1996, vol. 6, # 22, p. 2749 - 2754 [17] Collection of Czechoslovak Chemical Communications, 1991, vol. 56, # 11.1, p. 2420 - 2429 [18] Patent: US2003/36652, 2003, A1 [19] Bioorganic and Medicinal Chemistry Letters, 2008, vol. 18, # 14, p. 4191 - 4194 [20] Patent: WO2009/155156, 2009, A1. Location in patent: Page/Page column 67 [21] Organic Letters, 2016, vol. 18, # 18, p. 4714 - 4717 [22] Patent: US6348474, 2002, B1. Location in patent: Page column 44
合成路线 3(3. 合成:40851-95-4)
产率:45%
合成条件:With palladium 10% on activated carbon; hydrogen; sodium hydrogencarbonate In methanol at 20℃; for 2 h; Sealed tube
实验步骤:通用方法:向2-氯吡啶衍生物(1当量)的MeOH(10mL)溶液中加入10%Pd / C(1mol%)和NaHCO 3(每氯化吡啶1当量)。密封反应容器。 用氢气冲洗三次。 将黑色悬浮液在室温下在氢气氛(1个大气压)下搅拌2小时。 将混合物通过硅藻土过滤,用甲醇洗涤并真空浓缩。 根据需要通过柱色谱法纯化,得到加氢脱氯的吡啶产物。
参考文献:
- [1] Tetrahedron Letters, 2014, vol. 55, # 39, p. 5386 - 5389
