Extra virgin olive oil (EVOO), long-known for its heart health benefits, has now been identified for its rapid destruction of cancer cells.
While scientists have proven that the oleocanthal compound found in EVOO causes cell death in cancer cells, they have been unable to provide an explanation for this phenomenon until now.
In a study published in Molecular and Cellular Oncology, researchers discovered that the key to understanding the toxic effect of oleocantha in cancerous cells lies in its reaction with the lysosomes of the cell, where the cells store waste.
The oleocantha ruptures the cancer cell lysosomes causing cell death within 30 minutes to an hour, while leaving un-cancerous cells unharmed. This suggests that the lysosomal membranes of cancerous cells are weaker than those of non-cancerous cells.
Because of oleocantha’s targeted damage to cancer cells, it may prove an option for therapeutic cancer treatment.
Paul Breslin, co-author of the study, said “The mechanism of killing cancer cells and sparing healthy cells, lysosomal membrane permeabilisation, has been hypothesised as a possible mechanism of effectively killing cancer cells and sparing healthy tissues but has never been realised before.”
The study’s focus on the effect of oleocantha on cancerous and non-cancerous cells may lead to larger implications about the health benefits of the Mediterranean diet, which is rich in EVOO.
Breslin stated, “the Mediterranean diet is known to be associated with a reduced risk of many different kinds of cancer. Whereas the entire diet likely has many benefits, this study points directly to the olive oil phenolic, oleocanthal, as playing an especially important role in these observations.
"As more people turn to the Mediterranean diet as a healthy life option, oleocanthal is growing in its significance as a key active component of this diet.”
Reference:
LeGendre et al, (-)-Oleocanthal rapidly and selectively induces cancer cell death via lysosomal membrane permeabilization (LMP), Molecular and Cellular Oncology (2015).
Source: Taylor & Francis
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