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<dc:creator>Tapia, Lucía</dc:creator>
<dc:creator>Pérez, Yolanda</dc:creator>
<dc:creator>Carreira Barral, Israel</dc:creator>
<dc:creator>Bujons, Jordi</dc:creator>
<dc:creator>Bolte, Michael</dc:creator>
<dc:creator>Bedia, Carmen</dc:creator>
<dc:creator>Solà, Jordi</dc:creator>
<dc:creator>Quesada Pato, Roberto</dc:creator>
<dc:creator>Alfonso, Ignacio</dc:creator>
<dc:date>2024-09</dc:date>
<dc:description>The acidic microenvironment of solid tumors is a potential source of selectivity in the anti-cancer activity of ionophores, which requires delicate control of their biophysical properties. In this context, we have systematically studied fluorine substitutions in the aromatic side chains of HCl-binding pseudopeptidic cages. Interconnected factors like chloride binding, protonation, lipophilicity, and conformation and diffusiveness of the cages can impact their ability to transport HCl through the aqueous-lipid interphase, as demonstrated by robust experimental (X-ray, nuclear magnetic resonance [NMR], fluorescence) and theoretical results. The fine-tuning of these properties allows the modulation of their pH-dependent cytotoxicity against cancer cells, from essentially non-cytotoxic at pH 7.5 (like the extracellular surroundings of healthy tissues) to highly toxic in slightly acidic microenvironments (like those around solid tumors). Thus, a distal fluorine substitution produces a big impact on the physicochemical and biological properties of the cages, improving their selectivity as potential therapeutic ionophores.</dc:description>
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<dc:publisher>Cell Press</dc:publisher>
<dc:title>Tuning pH-dependent cytotoxicity in cancer cells by peripheral fluorine substitution on pseudopeptidic cages</dc:title>
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