Figueiredo CR , Matsuo AL , Pereira FV , Rabaça AN , Farias CF , Girola N , Massaoka MH , Azevedo RA , Scutti JA , Arruda DC , Silva LP , Rodrigues EG , Lago JH , Travassos LR , Silva RM .

	Figure 1. Cytotoxicity of HE in B16F10-Nex2 murine melanoma and nontumorigenic HUVEC, HF and 3T3 cells. Dose dependent activity of HE over 104 tumor cells in 18 h
	Figure 2. Morphological evidence and DNA degradation in HE-treated apoptotic melanoma cells. (a) B16F10-Nex2 cell morphology after treatment with 50 μg/ml HE for 18 h. Apoptotic bodies’ formation is indicated by white arrows; (b) Evaluation of chromatin condensation in HE treated cells. B16F10-Nex2 cells (104) were treated with 50μg/ml of HE for 18 h, labeled with Hoechst dye, and analyzed by fluorescence microscopy. Arrows indicate pronounced chromatin condensation in treated cells (Magnification 60x) Scale bar: 20μm; (c) Agarose gel electrophoresis of DNA fragmentation in B16F10-Nex2 cells induced by 50 μg/ml HE treatment for 24 h; (d) Fluorescence microscopy for DNA fragmentation. Melanoma cells (5 × 104) were treated with 50 μg/ml of HE and 150 μM of combretastatin A4 as positive apoptotic control for 24 h, and DNA fragmentation was detected using a TUNEL assay (green fluorescence). DAPI (blue) were used for total cell nuclei (Scale bar: 20 μm)
	Figure 3. Phosphatidyl serine surface expression and caspase activation. (a) Annexin V and propidium iodide labeling of B16F10- Nex2 (3 × 105) cells grown for 24 h in 12-well plate and incubated with 12 and 25 μg/ml of HE or RPMI medium for 18 h at 37 °C. Positive annexin V (AV) and propidium iodide cells were detected with an inverted fluorescence microscope at 10X magnification; (b) Activation of caspase-2, 3, 8 and 9 in HE treated melanoma cells. B16F10-Nex2 cells (107) were treated with 50 μg/ml of HE for 24 h, and the HE induced enzymatic activity of caspase-2, 3, 8 and 9 was evaluated by colorimetric assay
	Figure 4. Mitochondrial effects of HE treatment. (a) Representative images of superoxide anions’ negative and positive cells treated with 12.5 and 25 μg/ml of HE for 18 h, and 5 mm of hydrogen peroxide (positive control) for 30 min. B16F10-Nex2 cells were stained with 5 μM of DHE (dihydroethidium). Scale bar: 20 μm; (b) Representative images of mitochondrial ÄѰm following HE treatment. B16F10-Nex2 cells were treated with negative control and with 12 and 25 μg/ml of HE for 18 h (original magnification, 20×). Positive apoptotic cells were stained with annexin V (original magnification, 10X). (c) Percentage of TMRE (tetramethylrhodamine ethyl ester) and DHE positive cells; (d) Protective effect of N-acetyl cysteine (NAC) on HE-treated cells. B16F10-Nex2 cells (104) were pretreated for 2 h with 10 mM NAC, washed and incubated with 50 μg/ml of HE at 37°C for 18 h
	Figure 5. Effect of HE on the melanoma cell cycle. (a) Cell cycle analysis of B16F10-Nex2 tumor cells treated with 25 μg/ml HE and 75 μM of CA4 for 24 h. (b) Representative images of tumor cell morphology following HE treatment
	Figure 8. (a) 1H NMR spectrum of fraction HEF2 (~ CDCl3, 200 MHz)-the signal at ~ 7.24 ppm corresponding to hydrogens of residual CHCl3 in deuterated solvent; (b) GC-MS of HEF2 components with 4 main alkane species with the retention times of (1) tetracosane (C24H50), (2) hexacosane (C26H54), (3) octacosane (C28H58), (4) triacontane (C30H62), and 3 other minor species as listed in Table 3; (c) Mass spectrum of octacosane (GC component 3) and (d) triacontane (GC component 4), further identified by co-injection with standard n-octacosane, Rt 37.7 min, MM 620 Da, and triacontane, Rt 39.57 min, MM 422 Da
	Figure 9. Cytotoxicity of HE individual alkanes. (a) Cytotoxicity of octacosane and triacontane in B16F10-Nex2 cells after 18 h. (b) Tumor cell morphology after incubation with different concentrations of octacosane and triacontane

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