AI Article Synopsis

  • Breast Cancer (BC) is a major health issue, affecting 13% of women globally, with current treatments focusing on inhibiting estrogen production and blocking estrogen receptors.
  • Researchers are exploring dual-target drugs that can simultaneously inhibit both the aromatase enzyme and estrogen receptor (ER) α to improve treatment efficacy and reduce side effects.
  • The study identified promising drug candidates with low-nanomolar potency against both targets, highlighting the potential of multitarget strategies as effective treatments for Estrogen Receptor positive BC.

Article Abstract

Breast Cancer (BC) is a leading cause of death in women, currently affecting 13% of female population worldwide. First-line clinical treatments against Estrogen Receptor positive (ER+) BC rely on suppressing estrogen production, by inhibiting the aromatase (AR) enzyme, or on blocking estrogen-dependent pro-oncogenic signaling, by targeting Estrogen Receptor (ER) α with selective Modulators/Degraders (SERMs/SERDs). The development of dual acting molecules targeting AR and ERα represents a tantalizing alternative strategy to fight ER + BC, reducing the incidence of adverse effects and resistance onset that limit the effectiveness of these gold-standard therapies. Here, in silico design, synthesis, biological evaluation and an atomic-level characterization of the binding and inhibition mechanism of twelve structurally related drug-candidates enable the discovery of multiple compounds active on both AR and ERα in the sub-μM range. The best drug-candidate 3a displayed a balanced low-nanomolar IC towards the two targets, SERM activity and moderate selectivity towards a BC cell line. Moreover, most of the studied compounds reduced ERα levels, suggesting a potential SERD activity. This study dissects the key structural traits needed to obtain optimal dual acting drug-candidates, showing that multitarget compounds may be a viable therapeutic option to counteract ER + BC.

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Source
http://dx.doi.org/10.1016/j.ejmech.2021.113733DOI Listing

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