Journal of Medicinal Chemistry, volume 62, issue 22, pages 10108-10123

Discovery of a Furanopyrimidine-Based Epidermal Growth Factor Receptor Inhibitor (DBPR112) as a Clinical Candidate for the Treatment of Non-Small Cell Lung Cancer

Shu-Yu Lin 1
Yung Chang Hsu 1
Yi Hui Peng 1
Yi-Yu Ke 1
Wen-Hsing Lin 1
Hsu-Yi Sun 1
Hui-Yi Shiao 1
Fu-Ming Kuo 1
Pei-yi Chen 1
Tzu-Wen Lien 1
Chun-Hwa Chen 1
Chang-Ying Chu 1
Sing-Yi Wang 1
Kai Chia Yeh 1
Ching-Ping Chen 1
Tsu-An Hsu 1
Suying Wu 1
Teng-Kuang Yeh 1
Chiung-Yu Chen 1
Show full list: 20 authors
1
 
Institute of Biotechnology and Pharmaceutical Research, National Health Research Institutes, 35 Keyan Road, Zhunan, Miaoli County 35053, Taiwan, ROC
Publication typeJournal Article
Publication date2019-09-27
scimago Q1
wos Q1
SJR1.986
CiteScore12.8
Impact factor6.8
ISSN00222623, 15204804
Drug Discovery
Molecular Medicine
Abstract
Epidermal growth factor receptor (EGFR)-targeted therapy in non-small cell lung cancer represents a breakthrough in the field of precision medicine. Previously, we have identified a lead compound, furanopyrimidine 2, which contains a (S)-2-phenylglycinol structure as a key fragment to inhibit EGFR. However, compound 2 showed high clearance and poor oral bioavailability in its pharmacokinetics studies. In this work, we optimized compound 2 by scaffold hopping and exploiting the potent inhibitory activity of various warhead groups to obtain a clinical candidate, 78 (DBPR112), which not only displayed a potent inhibitory activity against EGFRL858R/T790M double mutations but also exhibited tenfold potency better than the third-generation inhibitor, osimertinib, against EGFR and HER2 exon 20 insertion mutations. Overall, pharmacokinetic improvement through lead-to-candidate optimization yielded fourfold oral AUC better that afatinib along with F = 41.5%, an encouraging safety profile, and significant antitumor efficacy in in vivo xenograft models. DBPR112 is currently undergoing phase 1 clinical trial in Taiwan.
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