A Sperm Model For Powering Nanotech Devices

The biological pathway that powers sperm to swim long distances could be harnessed to nanotech devices, releasing drugs or performing mechanical functions inside the body, according to a presentation at the American Society for Cell Biology’s 47th Annual meeting. The work by researchers at Cornell’s Baker Institute of Animal Health may be the first demonstration of how multistep biological pathways can be assembled and function on a human-made device. Mammalian sperm have to delivery energy to the long, thin, whip-like tails that power their swimming. Sperm meet the challenge, in part, by onsite power generation, modifying the enzymes of glycolysis so that they can attach themselves to a solid structure running the major length of the sperm tail.

The biological pathway that powers sperm to swim long distances could be harnessed to nanotech devices, releasing drugs or performing mechanical functions inside the body, according to a presentation at the American Society for Cell Biology’s 47th Annual meeting.

The work by researchers at Cornell’s Baker Institute of Animal Health may be the first demonstration of how multistep biological pathways can be assembled and function on a human-made device.

Mammalian sperm have to delivery energy to the long, thin, whip-like tails that power their swimming. Sperm meet the challenge, in part, by onsite power generation, modifying the enzymes of glycolysis so that they can attach themselves to a solid structure running the major length of the sperm tail. From that secure perch, glycolytic enzymes convert sugar into ATP, supplying energy all along the sperm’s bending and flexing tail.

Chinatsu Mukai, Alex Travis, and others at Cornell’s College of Veterinary Science looked at the early steps in the glycolysis pathway to see if they could move it from the thin “fibrous sheath” that covers the sperm tail to a solid inorganic substitute—a nickel-NTA (nitrilotriacetic acid) chip.

First, the researchers replaced the sperm-specific targeting domain of hexokinase, the first enzyme of glycolysis, with a tag that binds to a special gold surface. Even when tethered, the enzyme remained functional. Next they tagged the second enzyme in the pathway, glucose-6-phosphate isomerase. This too was active when tethered. With both attached to the same support, the enzymes acted in series with the product of the first reaction serving as substrate for the second.

These are only the first steps in reproducing the full glycolytic pathway on an inorganic support, say Mukai and Travis. Mukai and Travis suggest that their work serves as proof of principle that the organization of the glycolytic pathway in sperm might provide a natural engineering solution of how to produce ATP locally on nano devices.

Paper: "Coupled Metabolic Reaction on a Chip: A Step Toward Energy Production on Implantable Medical Devices"

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