Artikel

Identification of a New Interesting BAG3 Modulator Able to Disrupt Cancer‐Related Pathways

12.08.2025

Von Wiley-VCH zur Verfügung gestellt

Compound 2, identified through in-house screening and derived from SP18, exhibits high affinity for BAG3, as demonstrated by Surface Plasmon Resonance and docking studies. It induces a dose-dependent proapoptotic response in HeLa cells, evidenced by increased Annexin V/PI staining, underscoring the triazole scaffold as a promising platform for BAG3-targeted anticancer drug development.


Continuing the research aimed at discovering new BAG3 modulators as attractive anticancer drug candidates, a screening campaign on an in-house library is performed, including compounds featuring a large variety of scaffolds. The obtained results prompted a focus on the triazole moiety and, following a stepwise structural refinement of this scaffold guided by biophysical assays and computational studies, a very attractive compound (2) is identified showing a tight interaction with BAG3 and displaying a significant cytotoxic activity. The discovery of compound 2, whose effects on apoptosis and proteostasis confirm the disruption of BAG3-related pathways, is particularly relevant given the limited number of BAG3 modulators reported so far. Moreover, the computational data highlight the potential to further explore the triazole scaffold for the development of more potent anticancer agents.

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Identification of a New Interesting BAG3 Modulator Able to Disrupt Cancer‐Related Pathways
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Identification of a New Interesting BAG3 Modulator Able to Disrupt Cancer‐Related Pathways
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Identification of a New Interesting BAG3 Modulator Able to Disrupt Cancer‐Related Pathways
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Identification of a New Interesting BAG3 Modulator Able to Disrupt Cancer‐Related Pathways
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Identification of a New Interesting BAG3 Modulator Able to Disrupt Cancer‐Related Pathways
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