4.7 Article

Pharmacological Investigation of CC-LAAO, an L-Amino Acid Oxidase from Cerastes cerastes Snake Venom

Journal

TOXINS
Volume 13, Issue 12, Pages -

Publisher

MDPI
DOI: 10.3390/toxins13120904

Keywords

SV-LAAOs; envenomation; toxicity; apoptosis; glioblastoma cells

Funding

  1. Ministry of Higher Education and Scientific Research of Tunisia [Facility/InsermUMR1231]
  2. [LR20IPT01]

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Snake venom proteins have been developed as potential drugs for treating human diseases despite being responsible for severe injuries. The study evaluated CC-LAAO from Cerastes cerastes snake venom as a potential anti-glioblastoma drug, showing that low concentrations may be safe and have potential in developing anti-glioblastoma agents.
Snake venom proteins, which are responsible for deadly snakebite envenomation, induce severe injuries including neurotoxicity, myotoxicity, cardiotoxicity, hemorrhage, and the disruption of blood homeostasis. Yet, many snake-venom proteins have been developed as potential drugs for treating human diseases due to their pharmacological effects. In this study, we evaluated the use of, an L-amino acid oxidase isolated from Cerastes cerastes snake venom CC-LAAO, as a potential anti-glioblastoma drug, by investigating its in vivo and in vitro pharmacological effects. Our results showed that acute exposure to CC-LAAO at 1 and 2.5 mu g/mL does not induce significant toxicity on vital organs, as indicated by the murine blood parameters including aspartate transaminase (AST), alanine transaminase (ALT), lactate dehydrogenase (LDH) activities, and creatinine levels. The histopathological examination demonstrated that only at high concentrations did CC-LAAO induce inflammation and necrosis in several organs of the test subjects. Interestingly, when tested on human glioblastoma U87 cells, CC-LAAO induced a dose-dependent apoptotic effect through the H2O2 generated during the enzymatic reaction. Taken altogether, our data indicated that low concentration of CC-LAAO may be safe and may have potential in the development of anti-glioblastoma agents.

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