Direct Ser797 Interacted Pteridine-7(8H)-one Derivatives as Highly Selective and Orally Available EGFRL858R/T790M/C797SInhibitors

Wenzhe Jiang; Yupei He; Yongxiang Wang; Husheng Du; Dou Dou; Yuting Hu; Ruolin Hu; Buyao Hu; Wenjie Sha; Wenyi Mei; Zhenjiang Zhao; Honglin Li; Shengqing Li; Yufang Xu; Zhuo Chen

doi:10.1021/acs.jmedchem.5c01313

Direct Ser797 Interacted Pteridine-7(8H)-one Derivatives as Highly Selective and Orally Available EGFR^{L858R/T790M/C797S}Inhibitors

Wenzhe Jiang
, Yupei He
, Yongxiang Wang
, Husheng Du
, Dou Dou
, Yuting Hu
, Ruolin Hu
, Buyao Hu
, Wenjie Sha
, Wenyi Mei
, Zhenjiang Zhao
, Honglin Li^*
, Shengqing Li^*
, Yufang Xu^*
, Zhuo Chen^*

^*Corresponding author for this work

School of Pharmaceutical Sciences

East China University of Science and Technology
Hebei Agricultural University
Fudan University

Research output: Contribution to journal › Article › peer-review

1 Scopus citations

Abstract

The EGFR^C797Smutation is the main mechanism of acquired resistance to Osimertinib in NSCLC. There is an urgent need for small-molecule inhibitors to overcome Osimertinib-resistance. In this article, we developed a series of pteridin-7(8H)-one-derived inhibitors of EGFR^{L858R/T790M/C797S}(EGFR^LR/TM/CS) integrating direct interactions with the mutated Ser797 residue and the hydrophobic pocket encircled by the gatekeeper Met790 residue. Among them, M49 exhibited potent inhibitory activity against EGFR^LR/TM/CS(IC₅₀= 18.94 nM) and showed great kinase selectivity (S(35) = 0.005). Pharmacokinetic studies revealed that orally dosed M49 at 10 mg/kg resulted in a Cmax of 230.07 ng/mL and oral bioavailability of 12.14%. Moreover, M49 demonstrated effective antitumor efficacy in BaF3-EGFR^{L858R/T790M/C797S}xenograft model in comparison with Brigatinib (TGI = 73.53% vs 56.05%). In all, this study provided a novel EGFR^LR/TM/CSinhibitor discovery strategy and a pteridin-7(8H)-one-based EGFR^LR/TM/CSinhibitor which exhibited great potency and selectivity both in vitro and in vivo.

Original language	English
Pages (from-to)	18463-18490
Number of pages	28
Journal	Journal of Medicinal Chemistry
Volume	68
Issue number	17
DOIs	https://doi.org/10.1021/acs.jmedchem.5c01313
State	Published - 11 Sep 2025

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title = "Direct Ser797 Interacted Pteridine-7(8H)-one Derivatives as Highly Selective and Orally Available EGFRL858R/T790M/C797SInhibitors",

abstract = "The EGFRC797Smutation is the main mechanism of acquired resistance to Osimertinib in NSCLC. There is an urgent need for small-molecule inhibitors to overcome Osimertinib-resistance. In this article, we developed a series of pteridin-7(8H)-one-derived inhibitors of EGFRL858R/T790M/C797S(EGFRLR/TM/CS) integrating direct interactions with the mutated Ser797 residue and the hydrophobic pocket encircled by the gatekeeper Met790 residue. Among them, M49 exhibited potent inhibitory activity against EGFRLR/TM/CS(IC50= 18.94 nM) and showed great kinase selectivity (S(35) = 0.005). Pharmacokinetic studies revealed that orally dosed M49 at 10 mg/kg resulted in a Cmax of 230.07 ng/mL and oral bioavailability of 12.14\%. Moreover, M49 demonstrated effective antitumor efficacy in BaF3-EGFRL858R/T790M/C797Sxenograft model in comparison with Brigatinib (TGI = 73.53\% vs 56.05\%). In all, this study provided a novel EGFRLR/TM/CSinhibitor discovery strategy and a pteridin-7(8H)-one-based EGFRLR/TM/CSinhibitor which exhibited great potency and selectivity both in vitro and in vivo.",

author = "Wenzhe Jiang and Yupei He and Yongxiang Wang and Husheng Du and Dou Dou and Yuting Hu and Ruolin Hu and Buyao Hu and Wenjie Sha and Wenyi Mei and Zhenjiang Zhao and Honglin Li and Shengqing Li and Yufang Xu and Zhuo Chen",

note = "Publisher Copyright: {\textcopyright} 2025 American Chemical Society",

year = "2025",

month = sep,

day = "11",

doi = "10.1021/acs.jmedchem.5c01313",

language = "英语",

volume = "68",

pages = "18463--18490",

journal = "Journal of Medicinal Chemistry",

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publisher = "American Chemical Society",

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TY - JOUR

T1 - Direct Ser797 Interacted Pteridine-7(8H)-one Derivatives as Highly Selective and Orally Available EGFRL858R/T790M/C797SInhibitors

AU - Jiang, Wenzhe

AU - He, Yupei

AU - Wang, Yongxiang

AU - Du, Husheng

AU - Dou, Dou

AU - Hu, Yuting

AU - Hu, Ruolin

AU - Hu, Buyao

AU - Sha, Wenjie

AU - Mei, Wenyi

AU - Zhao, Zhenjiang

AU - Li, Honglin

AU - Li, Shengqing

AU - Xu, Yufang

AU - Chen, Zhuo

PY - 2025/9/11

Y1 - 2025/9/11

N2 - The EGFRC797Smutation is the main mechanism of acquired resistance to Osimertinib in NSCLC. There is an urgent need for small-molecule inhibitors to overcome Osimertinib-resistance. In this article, we developed a series of pteridin-7(8H)-one-derived inhibitors of EGFRL858R/T790M/C797S(EGFRLR/TM/CS) integrating direct interactions with the mutated Ser797 residue and the hydrophobic pocket encircled by the gatekeeper Met790 residue. Among them, M49 exhibited potent inhibitory activity against EGFRLR/TM/CS(IC50= 18.94 nM) and showed great kinase selectivity (S(35) = 0.005). Pharmacokinetic studies revealed that orally dosed M49 at 10 mg/kg resulted in a Cmax of 230.07 ng/mL and oral bioavailability of 12.14%. Moreover, M49 demonstrated effective antitumor efficacy in BaF3-EGFRL858R/T790M/C797Sxenograft model in comparison with Brigatinib (TGI = 73.53% vs 56.05%). In all, this study provided a novel EGFRLR/TM/CSinhibitor discovery strategy and a pteridin-7(8H)-one-based EGFRLR/TM/CSinhibitor which exhibited great potency and selectivity both in vitro and in vivo.

AB - The EGFRC797Smutation is the main mechanism of acquired resistance to Osimertinib in NSCLC. There is an urgent need for small-molecule inhibitors to overcome Osimertinib-resistance. In this article, we developed a series of pteridin-7(8H)-one-derived inhibitors of EGFRL858R/T790M/C797S(EGFRLR/TM/CS) integrating direct interactions with the mutated Ser797 residue and the hydrophobic pocket encircled by the gatekeeper Met790 residue. Among them, M49 exhibited potent inhibitory activity against EGFRLR/TM/CS(IC50= 18.94 nM) and showed great kinase selectivity (S(35) = 0.005). Pharmacokinetic studies revealed that orally dosed M49 at 10 mg/kg resulted in a Cmax of 230.07 ng/mL and oral bioavailability of 12.14%. Moreover, M49 demonstrated effective antitumor efficacy in BaF3-EGFRL858R/T790M/C797Sxenograft model in comparison with Brigatinib (TGI = 73.53% vs 56.05%). In all, this study provided a novel EGFRLR/TM/CSinhibitor discovery strategy and a pteridin-7(8H)-one-based EGFRLR/TM/CSinhibitor which exhibited great potency and selectivity both in vitro and in vivo.

UR - https://www.scopus.com/pages/publications/105015629010

U2 - 10.1021/acs.jmedchem.5c01313

DO - 10.1021/acs.jmedchem.5c01313

M3 - 文章

C2 - 40874809

AN - SCOPUS:105015629010

SN - 0022-2623

VL - 68

SP - 18463

EP - 18490

JO - Journal of Medicinal Chemistry

JF - Journal of Medicinal Chemistry

IS - 17

ER -

Direct Ser797 Interacted Pteridine-7(8H)-one Derivatives as Highly Selective and Orally Available EGFR^{L858R/T790M/C797S}Inhibitors

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