Invention Grant
- Patent Title: Aryl, heteroaryl, and heterocyclic compounds for treatment of complement mediated disorders
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Application No.: US16140148Application Date: 2018-09-24
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Publication No.: US10253053B2Publication Date: 2019-04-09
- Inventor: Jason Allan Wiles , Venkat Rao Gadhachanda , Qiuping Wang , Godwin Pais , Akihiro Hashimoto , Dawei Chen , Xiangzhu Wang , Atul Agarwal , Milind Deshpande , Avinash S. Phadke
- Applicant: Achillion Pharmaceuticals, Inc.
- Applicant Address: US CT New Haven
- Assignee: Achillion Pharmaceuticals, Inc.
- Current Assignee: Achillion Pharmaceuticals, Inc.
- Current Assignee Address: US CT New Haven
- Agency: Knowles Intellectual Property Strategies, LLC
- Main IPC: C07D471/04
- IPC: C07D471/04 ; C07D471/08 ; C07D487/04 ; C07D401/14 ; C07D403/04 ; C07D403/14 ; C07D405/12 ; C07D405/14 ; C07D413/06 ; C07D413/12 ; C07D417/06 ; C07D417/12 ; C07F9/572 ; C07D403/12 ; C07D209/42 ; C07D209/30 ; C07D209/44 ; C07D209/88 ; C07D209/12 ; A61K31/519 ; A61K31/501 ; A61K9/00 ; A61K31/4045 ; A61K31/444 ; A61K31/675 ; A61K31/404 ; A61K31/407 ; A61K31/4162 ; A61K31/4178 ; A61K31/4184 ; A61K31/4188 ; A61K31/4192 ; A61K31/437 ; A61K31/4439 ; A61K31/4709 ; A61K31/496 ; A61K31/506 ; A61K31/549 ; A61K31/55 ; A61K31/683 ; C07F9/6558 ; C07F9/6561 ; C07D513/04 ; C07B59/00 ; C07D209/14 ; C07D209/40 ; C07D487/14 ; C07D491/113 ; C07D495/04 ; C07D403/08 ; C07D413/14 ; C07D417/14 ; C07D403/06 ; C07F5/02 ; C07F7/08

Abstract:
Compounds, methods of use, and processes for making inhibitors of complement factor D comprising Formula I, or a pharmaceutically acceptable salt or composition thereof wherein R12 or R13 on the A group is an aryl, heteroaryl or heterocycle (R32) are provided. The inhibitors described herein target factor D and inhibit or regulate the complement cascade at an early and essential point in the alternative complement pathway, and reduce factor D's ability to modulate the classical and lectin complement pathways. The inhibitors of factor D described herein are capable of reducing the excessive activation of complement, which has been linked to certain autoimmune, inflammatory, and neurodegenerative diseases, as well as ischemia-reperfusion injury and cancer.
Public/Granted literature
- US20190023729A1 ARYL, HETEROARYL, AND HETEROCYCLIC COMPOUNDS FOR TREATMENT OF COMPLEMENT MEDIATED DISORDERS Public/Granted day:2019-01-24
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