Antiparasitic drug, the next weapon against brain cancer?
ANI Apr 13, 2017
Soon, a common pinworm medication could replace the current treatment used for certain brain cancers.
These findings from the Feinstein Institute for Medical Research's Karches Center for Oncology Research could help to extend the lives of patients suffering from one of the most common types of brain tumours, low-grade glioma. Low-grade glioma is a tumour that originates from cells that support and protect the brain's nervous system. Treatments for these tumours include surgery, radiotherapy and chemotherapy. Brain tumour chemotherapy is challenging as most drugs cannot penetrate the blood-brain barrier, a natural defense mechanism that prevents substances in the bloodstream from getting into the brain. For example, vincristine is a drug that is routinely used as part of different drug cocktails for the treatment of brain tumours, even though it is rather toxic and very poorly crosses the blood-brain barrier.
Marc Symons and colleagues examined mebendazole, a medication that is used to treat parasitic pinworms and that in previous studies had been found to be effective in the treatment of glioma tumours. By studying how mebendazole kills isolated tumour cells in the laboratory, they showed that it works in exactly the same way as vincristine. They also found, however, that while mebendazole effectively slowed down the growth of glioma tumours, vincristine did not work at all.
"We were rather surprised to see that vincristine, which is currently used to treat a range of different brain tumours, was totally ineffective in our in vivo glioma model," said \ Symons. "In contrast, in the same model, mebendazole performed quite well, most likely because mebendazole crosses the blood-brain barrier and reaches the tumour much better than vincristine. The reason that vincristine may be erroneously believed to be effective for the treatment of brain tumours is that it always has been used in combination with other treatments."
Based on the new results and due to the fact that vincristine often has severe side effects in comparison to relatively mild reactions to mebendzole, the team is now strongly motivated to initiate clinical trials to test whether vincristine can be exchanged by mebendazole in the treatment of brain tumours.
The study appears in open-access journal Molecular Medicine.
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