Nintedanib-αVβ6 Integrin Ligand Conjugates Reduce TGF β -Induced EMT in Human Non-Small Cell Lung Cancer

Growth factors and cytokines released in the lung cancer microenvironment promote an epithelial-to-mesenchymal transition (EMT) that sustains the progression of neoplastic diseases. TGF is one of the most powerful inducers of this transition, as it induces overexpression of the fibronectin receptor,...

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Veröffentlicht in:International journal of molecular sciences 2023-01, Vol.24 (2), p.1475
Hauptverfasser: Andreucci, Elena, Bugatti, Kelly, Peppicelli, Silvia, Ruzzolini, Jessica, Lulli, Matteo, Calorini, Lido, Battistini, Lucia, Zanardi, Franca, Sartori, Andrea, Bianchini, Francesca
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Sprache:eng
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Zusammenfassung:Growth factors and cytokines released in the lung cancer microenvironment promote an epithelial-to-mesenchymal transition (EMT) that sustains the progression of neoplastic diseases. TGF is one of the most powerful inducers of this transition, as it induces overexpression of the fibronectin receptor, αvβ6 integrin, in cancer cells which, in turn, is strongly associated with EMT. Thus, αvβ6 integrin receptors may be exploited as a target for the selective delivery of anti-tumor agents. We introduce three novel synthesized conjugates, in which a selective αvβ6 receptor ligand is linked to nintedanib, a potent kinase inhibitor used to treat advanced adenocarcinoma lung cancer in clinics. The αvβ6 integrin ligand directs nintedanib activity to the target cells of the tumor microenvironment, avoiding the onset of negative side effects in normal cells. We found that the three conjugates inhibit the adhesion of cancer cells to fibronectin in a concentration-dependent manner and that αvβ6-expressing cells internalized the conjugated compounds, thus permitting nintedanib to inhibit 2D and 3D cancer cell growth and suppress the clonogenic ability of the EMT phenotype as well as intervening in other aspects associated with the EMT transition. These results highlight αvβ6 receptors as privileged access points for dual-targeting molecular conjugates engaged in an efficient and precise strategy against non-small cell lung cancer.
ISSN:1422-0067
1661-6596
1422-0067
DOI:10.3390/ijms24021475