一二三四区视频,亚洲少妇熟女色,日本久热无码视频网,欧美国产日韩大尺度,亚洲a视频,久久少妇一区二区,日韩999无码视频,刺激久久久久久久,啊啊啊啊不要啊在线

Welcome to chemicalbook!
Chinese English Japanese Germany Korea
010-86108875
Try our best to find the right business for you.
Do not miss inquiry messages Please log in to view all inquiry messages.

Welcome back!

ChemicalBook CAS DataBase List Lenvatinib
417716-92-8

Lenvatinib synthesis

5synthesis methods
Lenvatinib, also known as E7080, is a synthetic, orally available inhibitor of vascular endothelial growth factor receptor 2 (VEGFR2, also known as KDR/FLK-1) tyrosine kinase with potential antineoplastic activity. E7080 blocks VEGFR2 activation by VEGF, resulting in inhibition of the VEGF receptor signal transduction pathway, decreased vascular endothelial cell migration and proliferation, and vascular endothelial cell apoptosis. Synthetic Description Reference: Naito, Toshihiko; Yoshizawa, Kazuhiro. Preparation of urea moiety-containing quinolinecarboxamide derivatives. WO 2005044788. (Assignee Eisai Co., Ltd., Japan) Synthetic Description Reference: Oruganti, Srinivas; Kandagatla, Bhaskar. Improved process for the preparation of lenvatinib using dimethylformamide as a solvent. IN 201641011188. (Assignee Dr. Reddy's Laboratories Limited, India) Synthetic Description Reference: Shah, Dharmesh Mahendrabhai; Wader, Guruprasad Ramchandra; Mehta, Tushar Bharatkumar; Chavda, Rajendra Gokalbhai; Kathrotiya, Harshad Ghanshyambhai; Patel, Arpit Kiritbhai. Improved process for the preparation of lenvatinib. WO 2019016664. (Assignee BDR Lifesciences Private Limited, India) Synthetic Description Reference: Funahashi, Yasuhiro; Tsuruoka, Akihiko; Matsukura, Masayuki; Haneda, Toru; Fukuda, Yoshio; Kamata, Junichi; Takahashi, Keiko; Matsushima, Tomohiro; Miyazaki, Kazuki; Nomoto, Ken-Ichi; Watanabe, Tatsuo; Obaishi, Hiroshi; Yamaguchi, Atsumi; Suzuki, Sachi; Nakamura, Katsuji; Mimura, Fusayo; Yamamoto, Yuji; Matsui, Junji; Matsui, Kenji; Yoshiba, Takako; Suzuki, Yasuyuki; Arimoto, Itaru. Preparation of urea derivatives containing nitrogenous aromatic ring compounds as inhibitors of angiogenesis. US 7253286. (Assignee Eisai Co., Ltd, Japan) Synthetic Description Reference: He, Peng; Wang, Xuechao; Deng, Ta; He, Qian. Method for preparing lenvatinib intermediate. CN 108997214. (Assignee Chengdu Diao Pharmaceutical Group Co., Ltd., Peop. Rep. China) Synthetic Description Reference: Zheng, Shiyang; Zhi, Yonggang. Method for preparation of lenvatinib. CN 108658859. (Assignee Chengdu Organic Chemicals Co., Ltd., Chinese Academy of Sciences, Peop. Rep. China) Synthetic Description Reference: Ge, Wenlei; Gao, Junlong; Liu, Kai; Guo, Dapeng. Process for preparation of lenvatinib impurity 4,4'-(((carbonylbis(azanediyl))bis(3-chloro-4,1-phenylene))bis(oxy))bis(7-methoxyquinoline-6-carboxamide) or its salt. CN 108299294. (Assignee Jiangsu Hengrui Medicine Co., Ltd., Peop. Rep. China) Synthetic Description Reference: Dong, Lichun; Hu, Geng; Li, Qi; Liu, Dianqing; Wang, Haoyuan. Synthesis method of anticancer drug lenvatinib. CN 107629001. (Assignee Chongqing University, Peop. Rep. China) Synthetic Description Reference: Jia, Huijuan; Chen, Yan; Zhang, Fan; He, Xuemin. Synthesis method of lenvatinib mesylate impurities. CN 107266363. (Assignee Hangzhou Huadong Medicine Group New Drug Research Institute Co., Ltd., Peop. Rep. China; Hangzhou Zhuyangxin Pharmaceutical Co., Ltd.; Zhejiang Huayi Pharmaceutical Co., Ltd.) Synthetic Description Reference: Nakamura, Taiju; Abe, Taichi; Miyashita, Yusuke; Kuroda, Hirofumi; Ayata, Yusuke; Akao, Atsushi. Highly pure quinoline derivative and method for the preparation thereof. WO 2016031841. (Assignee Eisai R&D Management Co., Ltd., Japan)
Synthetic Routes
  • ROUTE 1

    • 202112078492478561.jpg

    Reference: Naito, Toshihiko; Yoshizawa, Kazuhiro. Preparation of urea moiety-containing quinolinecarboxamide derivatives. WO 2005044788. (Assignee Eisai Co., Ltd., Japan)

  • ROUTE 2

    • 202112072881288903.jpg

    Reference: Oruganti, Srinivas; Kandagatla, Bhaskar. Improved process for the preparation of lenvatinib using dimethylformamide as a solvent. IN 201641011188. (Assignee Dr. Reddy's Laboratories Limited, India)

  • ROUTE 3

    • 202112075916977677.jpg

    Reference: Shah, Dharmesh Mahendrabhai; Wader, Guruprasad Ramchandra; Mehta, Tushar Bharatkumar; Chavda, Rajendra Gokalbhai; Kathrotiya, Harshad Ghanshyambhai; Patel, Arpit Kiritbhai. Improved process for the preparation of lenvatinib. WO 2019016664. (Assignee BDR Lifesciences Private Limited, India)

  • ROUTE 4

    • 202112079746895160.jpg

    Reference: Funahashi, Yasuhiro; Tsuruoka, Akihiko; Matsukura, Masayuki; Haneda, Toru; Fukuda, Yoshio; Kamata, Junichi; Takahashi, Keiko; Matsushima, Tomohiro; Miyazaki, Kazuki; Nomoto, Ken-Ichi; Watanabe, Tatsuo; Obaishi, Hiroshi; Yamaguchi, Atsumi; Suzuki, Sachi; Nakamura, Katsuji; Mimura, Fusayo; Yamamoto, Yuji; Matsui, Junji; Matsui, Kenji; Yoshiba, Takako; Suzuki, Yasuyuki; Arimoto, Itaru. Preparation of urea derivatives containing nitrogenous aromatic ring compounds as inhibitors of angiogenesis. US 7253286. (Assignee Eisai Co., Ltd, Japan)

  • ROUTE 5

    • 202112076206595874.jpg

    Reference: He, Peng; Wang, Xuechao; Deng, Ta; He, Qian. Method for preparing lenvatinib intermediate. CN 108997214. (Assignee Chengdu Diao Pharmaceutical Group Co., Ltd., Peop. Rep. China)

  • ROUTE 6

    • 202112070113112014.jpg

    Reference: Zheng, Shiyang; Zhi, Yonggang. Method for preparation of lenvatinib. CN 108658859. (Assignee Chengdu Organic Chemicals Co., Ltd., Chinese Academy of Sciences, Peop. Rep. China)

  • ROUTE 7

    • 202112073254700691.jpg

    Reference: Ge, Wenlei; Gao, Junlong; Liu, Kai; Guo, Dapeng. Process for preparation of lenvatinib impurity 4,4'-(((carbonylbis(azanediyl))bis(3-chloro-4,1-phenylene))bis(oxy))bis(7-methoxyquinoline-6-carboxamide) or its salt. CN 108299294. (Assignee Jiangsu Hengrui Medicine Co., Ltd., Peop. Rep. China)

  • ROUTE 8

    • 202112077286801575.jpg

    Reference: Dong, Lichun; Hu, Geng; Li, Qi; Liu, Dianqing; Wang, Haoyuan. Synthesis method of anticancer drug lenvatinib. CN 107629001. (Assignee Chongqing University, Peop. Rep. China)

  • ROUTE 9

    • 202112078516073397.jpg

    Reference: Jia, Huijuan; Chen, Yan; Zhang, Fan; He, Xuemin. Synthesis method of lenvatinib mesylate impurities. CN 107266363. (Assignee Hangzhou Huadong Medicine Group New Drug Research Institute Co., Ltd., Peop. Rep. China; Hangzhou Zhuyangxin Pharmaceutical Co., Ltd.; Zhejiang Huayi Pharmaceutical Co., Ltd.)

  • ROUTE 10

    • 202112076425423325.jpg

    Reference: Nakamura, Taiju; Abe, Taichi; Miyashita, Yusuke; Kuroda, Hirofumi; Ayata, Yusuke; Akao, Atsushi. Highly pure quinoline derivative and method for the preparation thereof. WO 2016031841. (Assignee Eisai R&D Management Co., Ltd., Japan)

202112078492478561.jpg

Reference: Naito, Toshihiko; Yoshizawa, Kazuhiro. Preparation of urea moiety-containing quinolinecarboxamide derivatives. WO 2005044788. (Assignee Eisai Co., Ltd., Japan)

-

Yield:417716-92-8 90%

Reaction Conditions:

Stage #1: 4?(4?amino?3?chlorophenoxy)?7?methoxyquinoline?6?carboxamide;phenyl chloroformatewith pyridine in water;N,N-dimethyl-formamide at -20; for 3 h;Inert atmosphere;
Stage #2: Cyclopropylamine in water;N,N-dimethyl-formamide at 8; for 15 h;Inert atmosphere;Time;

Steps:

2 Example 2 4-[3-Chloro-4-(cyclopropylaminocarbonyl)aminophenoxy]-7-methoxy-6-quinoline-carboxamide

Example 2 4-[3-Chloro-4-(cyclopropylaminocarbonyl)aminophenoxy]-7-methoxy-6-quinoline-carboxamide (0148) (0149) To a mixture of 26.0 kg of 4-(4-amino-3-chlorophenoxy)-7-methoxy-quinoline-6-carboxamide, 13.2 kg of pyridine, 1.36 kg of water and 196.0 L of N,N-dimethylformamide there was added 26.6 kg of phenyl chloroformate at -20° C. under a nitrogen atmosphere, and the mixture was stirred for 3 hours. Next, 19.4 kg of cyclopropylamine was further added at 8° C. and the mixture was stirred for 15 hours. After adding 13.0 L of water and 261.0 L of acetone to the reaction mixture, the deposited precipitate was filtered. The precipitate was rinsed with acetone, and the obtained solid was dried under reduced pressure to obtain 28.7 kg of a crude product of the title compound (89% yield). This was crystallized from 359.6 L of 1,3-dimethyl-2-imidazolidinone and 575.0 L of 2-propanol, to obtain 25.7 kg of compound (IV) (90% yield).

References:

US2017/233344,2017,A1 Location in patent:Paragraph 0148; 0149

Lenvatinib Related Search:

旅游| 伊春市| 钟山县| 探索| 永仁县| 苏尼特右旗| 武城县| 孟连| 喜德县| 齐齐哈尔市| 诸暨市| 昌宁县| 潢川县| 河东区| 探索| 潼南县| 高平市| 三门县| 丹巴县| 滦平县| 三门峡市| 苍南县| 榆林市| 黄浦区| 云梦县| 北京市| 隆林| 兴国县| 景洪市| 张家川| 武平县| 屏山县| 浦江县| 双辽市| 呼玛县| 晋江市| 富锦市| 南澳县| 南澳县| 双辽市| 阿巴嘎旗|