AUTHOR=Vasdev Roan A. S. , Gaudin Lachlan F. , Preston Dan , Jogy Jackmil P. , Giles Gregory I. , Crowley James D. 

TITLE=Anticancer Activity and Cisplatin Binding Ability of Bis-Quinoline and Bis-Isoquinoline Derived [Pd2L4]4+ Metallosupramolecular Cages

JOURNAL=Frontiers in Chemistry

VOLUME=6

YEAR=2018

URL=https://www.frontiersin.org/journals/chemistry/articles/10.3389/fchem.2018.00563

DOI=10.3389/fchem.2018.00563

ISSN=2296-2646

ABSTRACT=<p>New <italic>bis-</italic>quinoline (<bold>L</bold><sub>q</sub>) and <italic>bis-</italic>isoquinoline-based (<bold>L</bold><sub>iq</sub>) ligands have been synthesized, along with their respective homoleptic [Pd<sub>2</sub>(<bold>L</bold><sub>q</sub> or <bold>L</bold><sub>iq</sub>)<sub>4</sub>]<sup>4+</sup> cages (<bold>C</bold><sub>q</sub> and <bold>C</bold><sub>iq</sub>). The ligands and cages were characterized by <sup>1</sup>H, <sup>13</sup>C and diffusion ordered (DOSY) NMR spectroscopies, high resolution electrospray ionization mass spectrometry (HR-ESIMS) and in the case of the <italic>bis</italic>-quinoline cage, X-ray crystallography. The crystal structure of the <bold>C</bold><sub>q</sub> architecture showed that the [Pd<sub>2</sub>(<bold>L</bold><sub>q</sub>)<sub>4</sub>]<sup>4+</sup> cage formed a twisted <italic>meso</italic> isomer where the [Pd(<bold>quinoline</bold>)<sub>4</sub>]<sup>2+</sup> units at either end of the cage architecture adopt the opposite twists (left and right handed). Conversely, Density Functional Theory (DFT) calculations on the <bold>C</bold><sub>iq</sub> cage architecture indicated that a lantern shaped conformation, similar to what has been observed before for related [Pd<sub>2</sub>(<bold>L</bold><sub>tripy</sub>)<sub>4</sub>]<sup>4+</sup> systems (where <bold>L</bold><sub>tripy</sub> = 2,6-<italic>bis</italic>(pyridin-3-ylethynyl)pyridine), was generated. The different cage conformations manifest different properties for the isomeric cages. The <bold>C</bold><sub>iq</sub> cage is able to bind, weakly in acetonitrile, the anticancer drug cisplatin whereas the <bold>C</bold><sub>q</sub> architecture shows no interaction with the guest under the same conditions. The kinetic robustness of the two cages in the presence of Cl<sup>−</sup> nucleophiles was also different. The <bold>C</bold><sub>iq</sub> cage was completely decomposed into free <bold>L</bold><sub>iq</sub> and [Pd(Cl)<sub>4</sub>]<sup>2−</sup> within 1 h. However, the <bold>C</bold><sub>q</sub> cage was more long lived and was only fully decomposed after 7 h. The new ligands (<bold>L</bold><sub>iq</sub> and <bold>L</bold><sub>q</sub>) and the Pd(II) cage architectures (<bold>C</bold><sub>iq</sub> and <bold>C</bold><sub>q</sub>) were assessed for their cytotoxic properties against two cancerous cell lines (A549 lung cancer and MDA-MB-231 breast cancer) and one non-cancerous cell line (HDFa skin cells). It was found that <bold>L</bold><sub>q</sub> and <bold>C</bold><sub>q</sub> were both reasonably cytotoxic (IC<sub>50S</sub> ≈ 0.5 μM) against A549, while <bold>C</bold><sub>iq</sub> was slightly less active (IC<sub>50</sub> = 7.4 μM). <bold>L</bold><sub>iq</sub> was not soluble enough to allow the IC<sub>50</sub> to be determined against either of the two cancerous cell lines. However, none of the molecules showed any selectivity for the cancer cells, as they were all found to have similar cytotoxicities against HDFa skin cells (IC<sub>50</sub> values ranged from 2.6 to 3.0 μM).</p>