Scientists in Japan have discovered that a natural compound found in a type of ginger called kencur can throw cancer cells into disarray by disrupting how they generate energy.
According to
Osaka Metropolitan University, the finding opens new doors in the fight against
cancer, showing how natural substances might help target cancer's hidden energy
tricks.
While healthy
cells use oxygen to make energy efficiently, cancer cells often rely on a
backup method. This ginger-derived molecule doesn't attack that method
directly, it shuts down the cells' fat-making machinery instead, which
surprisingly causes the cells to ramp up their backup system even more.
For instance,
human cells oxidise glucose to produce ATP (adenosine triphosphate), an energy
source necessary for life.
Cancer cells
produce ATP through glycolysis, which does not utilise oxygen even under
conditions where oxygen is present, and convert glucose into pyruvic acid and
lactic acid.
This method
of producing ATP, known as the Warburg effect, is considered inefficient, thus
raising questions as to why cancer cells choose this energy pathway to fuel
their proliferation and survival.
In search of
this energy catalyst, Associate Professor Akiko Kojima-Yuasa's team at Osaka
Metropolitan University's Graduate School of Human Life and Ecology analysed
the cinnamic acid ester ethyl p-methoxycinnamate, a main component of kencur
ginger, and its mechanism of action.
In previous
research, the team discovered that ethyl p-methoxycinnamate has inhibitory
effects on cancer cells.
Furthering
their study, the acid ester was administered to Ehrlich ascites tumour cells to
assess which component of the cancer cells' energy pathway was being affected.
Results
revealed that the acid ester inhibits ATP production by disrupting de novo
fatty acid synthesis and lipid metabolism, rather than through glycolysis as
commonly theorised.
Further, the
researchers discovered acid ester-induced inhibition triggered increased
glycolysis, which acted as a possible survival mechanism in the cells.
This adaptability was theorised to be attributed to ethyl p-methoxycinnamate's inability to induce cell death.
"These
findings not only provide new insights that supplement and expand the theory of
the Warburg effect, which can be considered the starting point of cancer
metabolism research, but are also expected to lead to the discovery of new
therapeutic targets and the development of new treatment methods," stated
Professor Kojima-Yuasa. (ANI)
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