Молимо вас користите овај идентификатор за цитирање или овај линк до ове ставке: https://scidar.kg.ac.rs/handle/123456789/19096
Назив: Human estrogen receptor α antagonists, part 2: Synthesis driven by rational design, in vitro antiproliferative, and in vivo anticancer evaluation of innovative coumarin-related antiestrogens as breast cancer suppressants
Аутори: Kurtanović N.
Tomašević, Nevena
Matić, Sanja
Mitrović, Marina
Kostić, Danijela A
Sabatino, Manuela
Antonini, Lorenzo
Ragno, Rino
Mladenović, Milan
Датум издавања: 2022
Сажетак: New twelve in silico designed coumarin-based ERα antagonists, namely 3DQ-1a to 3DQ-1е, were synthesized and confirmed as selective ERα antagonists, showing potencies ranging from single-digit nanomolar to picomolar. The hits were confirmed as selective estrogen receptor modulators and validated as antiproliferative agents using MCF-7 breast cancer cell lines exerting from picomolar to low nanomolar potency, at the same time showing no agonistic activity within endometrial cell lines. Their mechanism of action was inspected and revealed to be through the inhibition of the Raf-1/MAPK/ERK signal transduction pathway, preventing hormone-mediated gene expression on either genomic direct or genomic indirect level, and stopping the MCF-7 cells proliferation at G0/G1 phase. In vivo experiments, by means of the per os administration to female Wistar rats with pre-induced breast cancer, distinguished six derivatives, 3DQ-4a, 3DQ-2a, 3DQ-1a, 3DQ-1b, 3DQ-2b, and 3DQ-3b, showing remarkable potency as tumor suppressors endowed with optimal pharmacokinetic profiles and no significant histopathological profiles. The presented data indicate the new compounds as potential candidates to be submitted in clinical trials for breast cancer therapy.
URI: https://scidar.kg.ac.rs/handle/123456789/19096
Тип: article
DOI: 10.1016/j.ejmech.2021.113869
Налази се у колекцијама:Institute for Information Technologies, Kragujevac

Број прегледа

357

Број преузимања

1

Датотеке у овој ставци:
Не постоје датотеке повезане са овом ставком.


Ова ставка је заштићена лиценцом Креативне заједнице Creative Commons