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Tytuł pozycji:

Comparative study of the potential cell-penetrating peptide $\Delta M4$ on apoptosis cell signaling in A375 and A431 cancer cell lines

Tytuł:
Comparative study of the potential cell-penetrating peptide $\Delta M4$ on apoptosis cell signaling in A375 and A431 cancer cell lines
Autorzy:
Manrique-Moreno, Marcela
Guevara Lora, Ibeth
Brankiewicz, Aleksandra
Fandino-Devia, Estefanía
Santa-González, Gloria A.
Data publikacji:
2024
Słowa kluczowe:
oxidative stress
cell-penetrating peptides
anticancer peptides
melanoma
apoptosis
epidermoid carcinoma
Język:
angielski
ISBN, ISSN:
19994923
Prawa:
http://creativecommons.org/licenses/by/4.0/legalcode.pl
Udzielam licencji. Uznanie autorstwa 4.0 Międzynarodowa
Dostawca treści:
Repozytorium Uniwersytetu Jagiellońskiego
Artykuł
In recent yearsjajajj, peptide-based therapeutics have attracted increasing interest as a potential approach to cancer treatment. Peptides are characterized by high specificity and low cytotoxicity, but they cannot be considered universal drugs for all types of cancer. Of the numerous anticancer-reported peptides, both natural and synthetic, only a few have reached clinical applications. However, in most cases, the mechanism behind the anticancer activity of the peptide is not fully understood. For this reason, in this work, we investigated the effect of the novel peptide $\Delta M4$, which has documented anticancer activity, on two human skin cancer cell lines. A novel approach to studying the potential induction of apoptosis by anticancer peptides is the use of protein microarrays. The results of the apoptosis protein study demonstrated that both cell types, skin malignant melanoma (A375) and epidermoid carcinoma (A431), exhibited markers associated with apoptosis and cellular response to oxidative stress. Additionally, ∆M4 induced concentration- and time-dependent moderate ROS production, triggering a defensive response from the cells, which showed decreased activation of cytoplasmic superoxide dismutase. However, the studied cells exhibited a differential response in catalase activity, with A375 cells showing greater resistance to the peptide action, possibly mediated by the Nrf2 pathway. Nevertheless, both cell types showed moderate activity of caspases 3/7, suggesting that they may undergo partial apoptosis, although another pathway of programmed death cannot be excluded. Extended analysis of the mechanisms of action of anticancer peptides may help determine their effectiveness in overcoming chemoresistance in cancerous cells.

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