Australian snakes venom could provide the next generation of human therapeutic drugs.
A blood-clotting protein in taipan venom has been identified by Queensland University of Technology PhD researcher Liam St Pierre to rapidly stop excessive bleeding during vascular surgery and major trauma.
The genetic code for the toxin, Factor X (Factor Ten), was identified by PhD researcher Liam St Pierre from QUTs School of Life Sciences who studied the venom of eight of Australias deadliest land snakes for their therapeutic potential.
His study focussed on the genes in the coastal taipans venom that are responsible for the pro coagulant or blood clotting agent called Factor X which could stem blood flow in a matter of seconds.
A drug lead based on Factor X is being evaluated for clinical trials by bio pharmaceutical development company QRxPharma.
"Australian snakes literally have a two-pronged attack when they bite their prey," Dr St Pierre said.
"Firstly, venom injection causes massive blood clots instantaneously followed by paralysis as a result of neurotoxins which eventually immobilise and kill the victim."
Dr St Pierre said mammals and snakes naturally produced a small amount of Factor X in their livers.
"Snakes produce a more stable and faster acting form of Factor X in their venom which is the only source of Factor X other than mammalian livers," he said.
"They have developed the ability to deliver massive fatal doses of Factor X to specifically target the systems of mammals."
Dr St Pierre studied the venom of the inland and coastal taipan, the common brown, the red bellied black, the mulga, the rough-scaled snake, Stephens banded snake and the tiger snake.
"Only the mulga did not have Factor X as it has developed its own unique mechanism of killing."
Dr St Pierre said snake venom was a huge untapped source of potential drug therapies.
His study is the most detailed ever conducted on the genes responsible for Australian snakes toxins. It is hoped a comprehensive study of all the venom components from Australian snakes may yield further novel components that could be targeted as human drugs.
Niki Widdowson | Source: EurekAlert!
Further information: www.qut.edu.au
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