AI Article Synopsis
- Melanoma is a highly aggressive skin cancer with low treatment effectiveness, prompting research into alternative therapies like tigecycline, a third-generation tetracycline.
- The study found that tigecycline effectively inhibited the growth of both melanotic (COLO 829) and amelanotic (A375) melanoma cells, with more significant effects on the COLO 829 cells, which underwent apoptosis.
- A375 cells showed resistance; instead of apoptosis, they exhibited increased levels of an autophagy marker (LC3A/B) and changes in cell cycle proteins, highlighting the potential for targeted therapy using tigecycline for melanotic melanoma.
Article Abstract
High mortality, aggressiveness, and the relatively low effectiveness of therapy make melanoma the most dangerous of skin cancers. Previously published studies presented the promising therapeutic potential of minocycline, doxycycline, and chlortetracycline on melanoma cells. This study aimed to assess the cytotoxicity of tigecycline, a third-generation tetracycline, on melanotic (COLO 829) and amelanotic (A375) melanoma cell lines. The obtained results showed that tigecycline, proportionally to the concentration and incubation time, efficiently inhibited proliferation of both types of melanoma cells. The effect was accompanied by the dysregulation of the cell cycle, the depolarization of the mitochondrial membrane, and a decrease in the reduced thiols and the levels of MITF and p44/42 MAPK. However, the ability to induce apoptosis was only found in COLO 829 melanoma cells. A375 cells appeared to be more resistant to the treatment with tigecycline. The drug did not induce apoptosis but caused an increase in LC3A/B protein levels-an autophagy marker. The observed differences in drug action on the tested cell lines also involved an increase in p21 and p16 protein levels in melanotic melanoma, which was related to cell cycle arrest in the G1/G0 phase. The greater sensitivity of melanotic melanoma cells to the action of tigecycline suggests the possibility of considering the use of the drug in targeted therapy.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10296940 | PMC |
| http://dx.doi.org/10.3390/cells12121564 | DOI Listing |
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