We are investigating the biological and biomedical imaging roles and impacts of fluorescent metallocorrole–TiO 2 nanoconjugates as potential near-infrared optical contrast agents in vitro in cancer and normal cell lines. The TiO 2 nanoconjugate labeled with the small molecule 2,17-bis(chlorosulfonyl)-5,10,15-tris(pentafluorophenyl)corrolato aluminum(III) (1-Al–TiO 2 ) was prepared. The nanoparticle 1-Al–TiO 2 was characterized by transmission electron microscopy (TEM) and integrating-sphere electronic absorption spectroscopy. TEM images of three different samples of TiO 2 nanoparticles (bare, H 2 O 2 etched, and 1-Al functionalized) showed similarity in shapes and sizes with an average diameter of 29nm for 1-Al–TiO 2 . Loading of 1-Al on the TiO 2 surfaces was determined to be ca. 20–40mg 1-Al/g TiO 2 . Confocal fluorescence microscopy (CFM) studies of luciferase-transfected primary human glioblastoma U87-Luc cells treated with the nanoconjugate 1-Al–TiO 2 as the contrast agent in various concentrations were performed. The CFM images revealed that 1-Al–TiO 2 was found inside the cancer cells even at low doses (0.02–2μg/mL) and localized in the cytosol. Bioluminescence studies of the U87-Luc cells exposed to various amounts of 1-Al–TiO 2 showed minimal cytotoxic effects even at higher doses (2–2000μg/mL) after 24h. A similar observation was made using primary mouse hepatocytes (PMH) treated with 1-Al–TiO 2 at low doses (0.0003–3μg/mL). Longer incubation times (after 48 and 72h for U87-Luc) and higher doses (>20μg/mL 1-Al–TiO 2 for U87-Luc and >3μg/mL 1-Al–TiO 2 for PMH) showed decreased cell viability.