It sounds almost too good to be true: a cheap and  simple drug that kills almost all cancers by switching off their  "immortality". The drug, dichloroacetate (DCA), has already been used  for years to treat rare metabolic disorders and so is known to be  relatively safe.
It also has no patent, meaning it could be manufactured for a fraction of the cost of newly developed drugs.
Evangelos Michelakis of the University of  Alberta in Edmonton, Canada, and his colleagues tested DCA on human  cells cultured outside the body and found that it killed lung, breast  and brain cancer cells, but not healthy cells. Tumours in rats  deliberately infected with human cancer also shrank drastically when  they were fed DCA-laced water for several weeks.
DCA attacks a unique feature of cancer  cells: the fact that they make their energy throughout the main body of  the cell, rather than in distinct organelles called mitochondria. This  process, called glycolysis, is inefficient and uses up vast amounts of  sugar.
Until now it had been assumed that cancer  cells used glycolysis because their mitochondria were irreparably  damaged. However, Michelakis's experiments prove this is not the case,  because DCA reawakened the mitochondria in cancer cells. The cells then  withered and died (Cancer Cell, DOI: 10.1016/j.ccr.2006.10.020).
Michelakis suggests that the switch to  glycolysis as an energy source occurs when cells in the middle of an  abnormal but benign lump don't get enough oxygen for their mitochondria  to work properly (see diagram). In order to survive, they switch off their mitochondria and start producing energy through glycolysis.
Crucially, though, mitochondria do another  job in cells: they activate apoptosis, the process by which abnormal  cells self-destruct. When cells switch mitochondria off, they become  "immortal", outliving other cells in the tumour and so becoming  dominant. Once reawakened by DCA, mitochondria reactivate apoptosis and  order the abnormal cells to die.
"The results are intriguing because they  point to a critical role that mitochondria play: they impart a unique  trait to cancer cells that can be exploited for cancer therapy," says  Dario Altieri, director of the University of Massachusetts Cancer Center  in Worcester.
The phenomenon might also explain how  secondary cancers form. Glycolysis generates lactic acid, which can  break down the collagen matrix holding cells together. This means  abnormal cells can be released and float to other parts of the body,  where they seed new tumours.
DCA can cause pain, numbness and gait  disturbances in some patients, but this may be a price worth paying if  it turns out to be effective against all cancers. The next step is to  run clinical trials of DCA in people with cancer. These may have to be  funded by charities, universities and governments: pharmaceutical  companies are unlikely to pay because they can't make money on  unpatented medicines. The pay-off is that if DCA does work, it will be  easy to manufacture and dirt cheap.
Paul Clarke, a cancer cell biologist at  the University of Dundee in the UK, says the findings challenge the  current assumption that mutations, not metabolism, spark off cancers.  "The question is: which comes first?" he says.
 
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