Peptide uptake in SCC-25 (a), Detroit 562 (b), and BEAS-2B (c) cells in published conditions. The cells were plated and incubated according to Bao et al. [4]. Tumor cells showed higher peptide interaction than BEAS-2B cells; the binding reaction to “irrelevant” peptide sequence was much lower than that of HN-1 and of its scrambled sequence. The highest binding was found in SCC-25 cells for scr-HN-1 peptide.