环氧合酶
药理学
前列腺素E2
炎症
微粒体
酶
化学
前列腺素
体外
ATP合酶
前列腺素E
医学
生物化学
免疫学
内科学
作者
Yanyu Zhang,Yun-Da Yao,Jin-Fang Luo,Zhongqiu Liu,Yuming Huang,Feichi Wu,Qin-Hua Sun,Jianxin Liu,Hua Zhou
标识
DOI:10.1016/j.phrs.2021.105977
摘要
Inflammation is closely linked to the abnormal phospholipid metabolism chain of cyclooxygenase-2/microsomal prostaglandin E2 synthase-1/prostaglandin E2 (COX-2/mPGES-1/PGE2). In clinical practice, non-steroidal anti-inflammatory drugs (NSAIDs) as upstream COX-2 enzyme activity inhibitors are widely used to block COX-2 cascade to relieve inflammatory response. However, NSAIDs could also cause cardiovascular and gastrointestinal side effects due to its inhibition on other prostaglandins generation. To avoid this, targeting downstream mPGES-1 instead of upstream COX is preferable to selectively block overexpressed PGE2 in inflammatory diseases. Some mPGES-1 inhibitor candidates including synthetic compounds, natural products and existing anti-inflammatory drugs have been proved to be effective in in vitro experiments. After 20 years of in-depth research on mPGES-1 and its inhibitors, ISC 27864 have completed phase II clinical trial. In this review, we intend to summarize mPGES-1 inhibitors focused on their inhibitory specificity with perspectives for future drug development.
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