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The researchers note that they tested the spider toxins on only one of a dozen suspected human pain channels.
"The likelihood is that within the vast diversity of spider toxins we will find others that are active against other channels important for pain," said Michael Nitabach, associate professor of cellular and molecular physiology and of genetics, and senior author of the paper.
The researchers screened the toxins from a variety of tarantula species to find one that blocked TRPA1, an ion channel on the surface of pain-sensing neurons that is implicated in inflammation and neuropathic pain.
In a process dubbed toxineering by the Yale researchers, the team generated another small library of mutated versions of the tarantula toxin to find one that blocked TRPA1 but had no effect on activity of other channels on the surface of neurons.
"The beauty of the system is we can also screen engineered toxins not found in nature, and identify higher-potency and more specific molecular variants that lack deleterious effects on essential nerve functions," Nitabach said.
His lab plans to ramp up efforts to test tens of thousands of new toxins for similar biological activity against pain-sensing neurons.
Junhong Gui and Boyi Liu of Yale are co-lead authors of the study, which was funded by the National Institutes of Health.
Source: Yale University