Discovery of Novel Prostacyclin Mimetics with Highly Potent and Selective IP Receptor Agonists
-
- Hattori Kouji
- Astellas Pharma Inc. Chemistry Research Laboratories
Bibliographic Information
- Other Title
-
- 非プロスタノイド骨格を有する新規プロスタサイクリン類縁体の創製と立体選択的合成研究
- ヒプロスタノイド コッカク オ ユウスル シンキ プロスタサイクリン ルイエンタイ ノ ソウセイ ト リッタイ センタクテキ ゴウセイ ケンキュウ
Search this article
Abstract
Prostacyclin (PGI2) is primarily secreted from vascular endothelium and plays an extremely important inhibitory role in platelet aggregation and as a vasodilator in maintaining homeostatic circulation. Despite fascinating pharmacological properties, the inherent instability and side effect of prostacyclin limit its therapeutic applicability. In this paper, we described that discovery of three classes of prostacyclin mimetics without PG skeleton, which are cycloalkene skeleton type (FR 181560, FR 181157), tetrahydronaphthalene skeleton type (FK 788), and amino acid type (FR 193264, FR 193262). Several designed prostacyclin mimetics exhibited potent PGI2 agonistic activity with good selectivity for IP receptor and bioavailability. The specific compounds were prepared by asymmetric synthesis with high selectivity. Furthermore, we also described metabolism study using rat and human liver microsomes to lead new drug design (FR 223346, FR 232149).
Journal
-
- Journal of Synthetic Organic Chemistry, Japan
-
Journal of Synthetic Organic Chemistry, Japan 64 (9), 923-933, 2006
The Society of Synthetic Organic Chemistry, Japan
- Tweet
Keywords
Details 詳細情報について
-
- CRID
- 1390282680289601536
-
- NII Article ID
- 10018052326
-
- NII Book ID
- AN0024521X
-
- ISSN
- 18836526
- 00379980
-
- NDL BIB ID
- 8091388
-
- Text Lang
- ja
-
- Data Source
-
- JaLC
- NDL
- Crossref
- CiNii Articles
-
- Abstract License Flag
- Disallowed