生命科学。
3-羟基-7-氧代-5-胆烷酸是有机合成和医药研发的中间体,是利胆药物熊去氧胆酸的合成的中间体。
合成路线 1(1. 合成:4651-67-6)
产率:99%
合成条件:With palladium on activated charcoal; hydrogen In methanol at 70℃; for 12 h;
实验步骤:将式(7)化合物(4g,10.3mmol)溶于甲醇(40mL)钯碳(400mg)H2(4MPa),70℃反应12h。TLC检测反应完成后,硅藻土过滤, 减压浓缩溶剂,加入水(40mL),用二氯甲烷(30mL×3)萃取。合并的有机相,洗涤,饱和盐水,用无水Na 2 SO 4干燥,浓缩,通过硅胶柱色谱法纯化( DCM:CH 3 OH = 10:1)获得式(8)化合物(4g白色固体,99%收率)。
参考文献:
- [1] Patent: CN107383137, 2017, A. Location in patent: Paragraph 0137 [2] Patent: CN106939030, 2017, A. Location in patent: Paragraph 0126; 0127 [3] Patent: CN107033208, 2017, A. Location in patent: Paragraph 0125; 0126
合成路线 2(2. 合成:4651-67-6)
产率:98.6%
合成条件:With dimethyl sulfoxide; triethylamine; trifluoroacetic anhydride In dichloromethane at -30℃; for 1.50 h;
实验步骤:将化合物1(5g,12.7mmol)加入到反应烧瓶中,并加入50mL二氯甲烷,DMSO(1.12g,14.3mmol)和三乙胺(4.2g,41.5mmol)。将反应温度冷却至-30℃。 向其中逐滴加入三氟乙酸酐(3.2g,15.2mmol)。 将反应物温育1.5小时后,加入10mL水。 搅拌混合物并温热至室温。 甲醇萃取两次,每次20ml,合并有机相,用饱和氯化钠溶液洗涤一次,用无水硫酸钠干燥,过滤,将有机相浓缩至干,得到化合物2,产量4.89g,产率98.6%
参考文献:
- [1] Patent: CN104876995, 2016, B. Location in patent: Paragraph 0036-0038; 0042; 0044 [2] Patent: CN106279336, 2017, A. Location in patent: Paragraph 0044; 0045; 0046 [3] Patent: CN107200763, 2017, A. Location in patent: Paragraph 0036; 0037; 0038; 0039 [4] Patent: CN107955056, 2018, A. Location in patent: Paragraph 0019-0022 [5] Patent: CN106986909, 2017, A. Location in patent: Paragraph 0043-0054 [6] Patent: WO2014/20024, 2014, A1. Location in patent: Page/Page column 5; 9; 10 [7] Steroids, 2012, vol. 77, # 13, p. 1335 - 1338 [8] Patent: CN105669815, 2016, A. Location in patent: Paragraph 0019; 0020; 0021 [9] Chemistry Letters, 1999, # 7, p. 693 - 694 [10] Steroids, 2002, vol. 67, # 1, p. 51 - 56 [11] Patent: CN105481925, 2016, A. Location in patent: Paragraph 0037; 0038; 0039 [12] Patent: CN106749466, 2017, A. Location in patent: Paragraph 0051-0053 [13] Organic Process Research and Development, 2002, vol. 6, # 5, p. 665 - 669 [14] Patent: WO2016/173493, 2016, A1. Location in patent: Page/Page column 23 [15] Patent: CN106518946, 2017, A. Location in patent: Paragraph 0138-0141 [16] Patent: US2009/62526, 2009, A1. Location in patent: Page/Page column 3 [17] Bioorganic and Medicinal Chemistry, 2016, vol. 24, # 18, p. 3986 - 3993 [18] Patent: US2017/233431, 2017, A1. Location in patent: Paragraph 0409-0410 [19] Patent: CN105348354, 2016, A. Location in patent: Paragraph 0022 [20] Hoppe-Seyler's Zeitschrift fuer Physiologische Chemie, 1937, vol. 250, p. 31 [21] Journal of Biochemistry (Tokyo, Japan), 1939, vol. 29, p. 51,54 [22] Journal of Organic Chemistry, 1993, vol. 58, # 2, p. 499 - 501 [23] Journal of Medicinal Chemistry, 2012, vol. 55, # 1, p. 84 - 93 [24] Journal of Medicinal Chemistry, 2014, vol. 57, # 3, p. 937 - 954 [25] Patent: US2015/112089, 2015, A1 [26] Process Biochemistry, 2015, vol. 50, # 4, p. 598 - 604 [27] Patent: WO2017/27396, 2017, A1. Location in patent: Page/Page column 72 [28] Patent: CN106892954, 2017, A. Location in patent: Paragraph 0059; 0061; 0064; 0065 [29] Patent: WO2017/208165, 2017, A1. Location in patent: Page/Page column 17; 18 [30] Patent: CN106478756, 2017, A. Location in patent: Paragraph 0025; 0035; 0036 [31] ChemBioChem, 2018, vol. 19, # 4, p. 347 - 353
合成路线 3(3. 合成:4651-67-6)
产率:90%
合成条件:With palladium on activated charcoal; hydrogen In tetrahydrofuran; methanol at 70℃; for 8 h;
实验步骤:式(7)化合物(5.4g,11.28mmol)溶于甲醇(48mL)和四氢呋喃(12mL)的混合溶剂,碳载钯(540mg),氢气压力(4MPa),加热至70° 在高锰酸钾反应完成后,将反应过滤并在硅胶柱中浓缩(DCM:MeOH = 10:1)。式(8)化合物(3.9g白色固体,90%收率) )获得了。
参考文献:
- [1] Patent: CN106995478, 2017, A. Location in patent: Paragraph 0116-0117
