| Literature DB >> 35314953 |
Jung Wuk Lee1,2, Changyu Choi1,2, Jihyung Kim1,2, Sohee Lee1,2, Jina Kim1,2, Yoonji Lee1, Kyung Hoon Min3,4.
Abstract
The gene amplification of human epidermal growth factor receptor 2 (HER2) plays an essential role in the proliferation and progression of several cancers. However, HER2 inhibitors such as lapatinib strongly suppress wild-type EGFR, resulting in severe adverse effects. Therefore, there is an unmet need for highly selective HER2 inhibitors. In this study, we describe the design and synthesis of novel quinazoline derivatives that exhibit enhanced selectivity for HER2 over wild-type EGFR. Structure-activity relationship analysis indicated that the selectivity for HER2 over EGFR depends on the aniline moiety at C-4 and the substituents at C-6 in the quinazoline derivatives. Compound 7c with an IC50 of 8 nM for HER2 exhibited significantly higher selectivity for HER2 over EGFR, with a 240-fold improvement over lapatinib. In addition, the synthesized compounds exhibited anti-proliferative activity in the nanomolar range against SKBR3, a human breast cancer cell line that overexpresses HER2.Entities:
Keywords: Cancer; EGFR; HER2; Kinase inhibitor; Quinazoline; Selectivity
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Year: 2022 PMID: 35314953 DOI: 10.1007/s12272-022-01376-4
Source DB: PubMed Journal: Arch Pharm Res ISSN: 0253-6269 Impact factor: 4.946