Dokumentdetails
ID

oai:pubmedcentral.nih.gov:1069...

Thema
Original Article
Autor
Wang, Yubo Min, Jian Deng, Xiangping Feng, Tian Hu, Hebing Guo, Xinyi Cheng, Yan Xie, Baohua Yang, Yu Chen, Chun-Chi Guo, Rey-Ting Dong, Chune Zhou, Hai-Bing
Langue
en
Editor

Elsevier

Kategorie

Acta Pharmaceutica Sinica. B

Jahr

2023

Auflistungsdatum

04.12.2023

Schlüsselwörter
erα estrogen degraders receptor cancer breast 29c novel
Metrisch

Zusammenfassung

Endocrine-resistance remains a major challenge in estrogen receptor α positive (ERα(+)) breast cancer (BC) treatment and constitutively active somatic mutations in ERα are a common mechanism.

There is an urgent need to develop novel drugs with new mode of mechanism to fight endocrine-resistance.

Given aberrant ERα activity, we herein report the identification of novel covalent selective estrogen receptor degraders (cSERDs) possessing the advantages of both covalent and degradation strategies.

A highly potent cSERD 29c was identified with superior anti-proliferative activity than fulvestrant against a panel of ERα(+) breast cancer cell lines including mutant ERα.

Crystal structure of ERα‒29c complex alongside intact mass spectrometry revealed that 29c disrupted ERα protein homeostasis through covalent targeting C530 and strong hydrophobic interaction collied on H11, thus enforcing a unique antagonist conformation and driving the ERα degradation.

These significant effects of the cSERD on ERα homeostasis, unlike typical ERα degraders that occur directly via long side chains perturbing the morphology of H12, demonstrating a distinct mechanism of action (MoA).

In vivo, 29c showed potent antitumor activity in MCF-7 tumor xenograft models and low toxicity.

This proof-of-principle study verifies that novel cSERDs offering new opportunities for the development of innovative therapies for endocrine-resistant BC.

Wang, Yubo,Min, Jian,Deng, Xiangping,Feng, Tian,Hu, Hebing,Guo, Xinyi,Cheng, Yan,Xie, Baohua,Yang, Yu,Chen, Chun-Chi,Guo, Rey-Ting,Dong, Chune,Zhou, Hai-Bing, 2023, Discovery of novel covalent selective estrogen receptor degraders against endocrine-resistant breast cancer, Elsevier

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