5 research outputs found

    Acyl protein thioesterase 1 and 2 (APT-1, APT-2) inhibitors palmostatin B, ML348 and ML349 have different effects on NRAS mutant melanoma cells

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    Oncogenic NRAS mutations are frequent in melanoma and lead to increased downstream signaling and uncontrolled cell proliferation. Since the direct inhibition of NRAS is not possible yet, modulators of NRAS posttranslational modifications have become an area of interest. Specifically, interfering with NRAS posttranslational palmitoylation/depalmitoylation cycle could disturb proper NRAS localization, and therefore decrease cell proliferation and downstream signaling. Here, we investigate the expression and function of NRAS depalmitoylating acyl protein thioesterases 1 and 2 (APT-1, APT-2) in a panel of NRAS mutant melanoma cells. First, we show that all melanoma cell lines examined express APT-1 and APT-2. Next, we show that siRNA mediated APT-1 and APT-2 knock down and that the specific APT-1 and -2 inhibitors ML348 and ML349 have no biologically significant effects in NRAS mutant melanoma cells. Finally, we test the dual APT-1 and APT-2 inhibitor palmostatin B and conclude that palmostatin B has effects on NRAS downstream signaling and cell viability in NRAS mutant melanoma cells, offering an interesting starting point for future studies

    Additional file 1 of The therapeutically actionable long non-coding RNA ‘T-RECS’ is essential to cancer cells’ survival in NRAS/MAPK-driven melanoma

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    Supplementary Material 1: Supplementary Table 1: Cell-line information. Supplementary Table 2: Cell Growth Reduction (%) caused by T-RECS-RNA-targeting therapy. Supplementary Table 3: Gene Expression Analysis of downregulated Genes between D04-Cells Treated with Non-targeting ASOs and T-RECS Targeting ASOs. Supplementary Table 4: Gene Expression Analysis of upregulated Genes between D04-Cells Treated with Non-targeting ASOs and T-RECS Targeting ASOs. Supplementary Table 5: DAVID functional clustering analysis. Supplementary Table 6: Tumor size and weight of mice. Supplementary Table 7: Primer sequences (5′-3′

    Immune responses in cardiac repair and regeneration: a comparative point of view

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