Study of the Cytotoxic and Antitumor Effect of L-lysine-α-oxidase from Trichoderma harzianum Rifai

Background/Aim: Enzymatic anticancer therapies are actively investigated as they can selectively deprive cancer cells of essential nutrients. L‑lysine‑α‑oxidases of different origins have been reported as potential anticancer enzymes with a significant antitumor potency. This study aimed to evaluate the cytotoxic and antitumor activity of L‑lysine‑α‑oxidase obtained from the domestic strain of Trichoderma harzianum Rifai VKPM F‑180. Materials and Methods: The melanoma cell line A875 and normal keratinocytes HaCaT were used for cytotoxicity testing. Murine solid tumors sarcoma 45, carcinosarcoma W‑256, carcinoma PC‑1 and hepatoma 22 were used for experiments with animals. Tumor growth inhibition (TGI) was the primary measure of antitumor efficacy. Results: L‑lysine‑α‑oxidase exhibited selective cytotoxicity toward melanoma cells (IC50=0.09 μg/ml) compared to HaCaT cells (IC50=0.38 μg/ml). In animal models, the enzyme significantly inhibited growth of sarcoma 45, carcinoma PC‑1, and hepatoma 22, with TGI ranging from 25% to 41% at 35 U/kg by the 8th or 9th day post‑treatment. However, carcinosarcoma W‑256, a reactive oxygen species‑producing tumor, demonstrated lower sensitivity, particularly at higher enzyme doses. Conclusion: L‑lysine‑α‑oxidase from Trichoderma harzianum Rifai demonstrates promising selective cytotoxicity and antitumor activity, especially in ROS‑sensitive tumors.

Издательство
International Institute of Anticancer Research
Номер выпуска
7
Язык
English
Страницы
2881-2889
Статус
Published
Том
45
Год
2025
Организации
  • 1 RUDN University
  • 2 Gamaleya National Research Center for Epidemiology and Microbiology of the Russian Ministry of Health
  • 3 Institute of Biomedical Chemistry
Ключевые слова
anticancer enzymes; L‑lysine‑α‑oxidase; trichoderma; cytotoxic activity; antitumor activity
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