Ingestible drug-delivery materials may help patients comply with treatment regimens
Massachusetts Institute of Technology Research News Aug 10, 2017
Hydrogel–based capsules could expand and reside in the GI tract for days, slowly releasing medication.
Researchers at MIT and Brigham and WomenÂs Hospital have developed a new set of drug delivery materials, which can reside in the stomach for up to nine days, slowly releasing their dosage of medication.
The materials, which the researchers describe in a paper published in the journal Nature Communications, are known as triggerable tough hydrogels (TTH), according to Robert Langer, the David H. Koch Institute Professor at MIT and a member of MITÂs Koch Institute for Integrative Cancer Research.
Developing a capsule that does not rapidly pass through the body, but can instead reside in the gastrointestinal (GI) tract for long periods of time, is no easy task, since any material must be able to withstand the considerable compressive forces in the stomach.
Any such device must also be small enough to be swallowed comfortably but large enough to avoid being passed out of the stomach and into the intestines through a region known as the pylorus, says Giovanni Traverso, a research affiliate at the Koch Institute, a gastroenterologist and biomedical engineer at Brigham and WomenÂs Hospital, and the paperÂs co–senior author.
WhatÂs more, it must be possible to trigger the device to self–destruct, in the event of an allergic reaction to, or unwelcome side effects from, the gel or the drug being delivered.
To this end, the researchers began investigating the use of hydrogels, polymer gels that have a high water content, giving them the capacity to swell when hydrated. Capsules made from the hydrogel in a dehydrated state could be swallowed by the patient; they would then swell on entering the stomach, to prevent them passing through the pylorus.
However, hydrogels, which are typically formed from a single network of crosslinked polymer chains, tend to be quite soft, and they do not have the strength to withstand compressive forces.
So the researchers instead used two intertwined polymer networks, to build a stronger, more resilient material. ÂThere are two networks. One is composed of alginate, a material derived from seaweed, and the other is polyacrylamide, a widely–used polymer, Traverso says.
Crosslinked within these intertwined networks are two types of chemical bond, which can be dissolved on demand using biocompatible trigger compounds.
The polyacrylamide network is crosslinked with disulphide bonds, which can be dissolved using the antioxidant glutathione. The alginate network, in contrast, is crosslinked with ionic bonds, which can be dissolved with a chemical known as EDTA (Ethylenediaminetetraacetic acid), which is used as a preservative in some foods and as a treatment for mercury and lead poisoning.
In this way, if the capsule device needs to be removed from the stomach in a hurry, the patient can simply swallow the antidote compounds, triggering the material to break apart and allowing it to safely pass through the body.
When the researchers tested the mechanical strength of the materials, they found they were robust enough to resist fracture, even under pressure from a razor blade.
They then tested devices built from the materials in large animal models, where they found they were able to withstand the forces within the stomach for more than seven days, according to the paperÂs lead author Jinyao Liu, an MIT postdoc.
Finally, they tested the deviceÂs potential as a drug delivery system, by loading it with the antimalarial lumefantrine. They chose this drug as nonadherence to medication is a particular problem in treating cases of malaria in the developing world.
They found the device was able to release the lumefantrine in a controlled manner, over a period of days.
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Researchers at MIT and Brigham and WomenÂs Hospital have developed a new set of drug delivery materials, which can reside in the stomach for up to nine days, slowly releasing their dosage of medication.
The materials, which the researchers describe in a paper published in the journal Nature Communications, are known as triggerable tough hydrogels (TTH), according to Robert Langer, the David H. Koch Institute Professor at MIT and a member of MITÂs Koch Institute for Integrative Cancer Research.
Developing a capsule that does not rapidly pass through the body, but can instead reside in the gastrointestinal (GI) tract for long periods of time, is no easy task, since any material must be able to withstand the considerable compressive forces in the stomach.
Any such device must also be small enough to be swallowed comfortably but large enough to avoid being passed out of the stomach and into the intestines through a region known as the pylorus, says Giovanni Traverso, a research affiliate at the Koch Institute, a gastroenterologist and biomedical engineer at Brigham and WomenÂs Hospital, and the paperÂs co–senior author.
WhatÂs more, it must be possible to trigger the device to self–destruct, in the event of an allergic reaction to, or unwelcome side effects from, the gel or the drug being delivered.
To this end, the researchers began investigating the use of hydrogels, polymer gels that have a high water content, giving them the capacity to swell when hydrated. Capsules made from the hydrogel in a dehydrated state could be swallowed by the patient; they would then swell on entering the stomach, to prevent them passing through the pylorus.
However, hydrogels, which are typically formed from a single network of crosslinked polymer chains, tend to be quite soft, and they do not have the strength to withstand compressive forces.
So the researchers instead used two intertwined polymer networks, to build a stronger, more resilient material. ÂThere are two networks. One is composed of alginate, a material derived from seaweed, and the other is polyacrylamide, a widely–used polymer, Traverso says.
Crosslinked within these intertwined networks are two types of chemical bond, which can be dissolved on demand using biocompatible trigger compounds.
The polyacrylamide network is crosslinked with disulphide bonds, which can be dissolved using the antioxidant glutathione. The alginate network, in contrast, is crosslinked with ionic bonds, which can be dissolved with a chemical known as EDTA (Ethylenediaminetetraacetic acid), which is used as a preservative in some foods and as a treatment for mercury and lead poisoning.
In this way, if the capsule device needs to be removed from the stomach in a hurry, the patient can simply swallow the antidote compounds, triggering the material to break apart and allowing it to safely pass through the body.
When the researchers tested the mechanical strength of the materials, they found they were robust enough to resist fracture, even under pressure from a razor blade.
They then tested devices built from the materials in large animal models, where they found they were able to withstand the forces within the stomach for more than seven days, according to the paperÂs lead author Jinyao Liu, an MIT postdoc.
Finally, they tested the deviceÂs potential as a drug delivery system, by loading it with the antimalarial lumefantrine. They chose this drug as nonadherence to medication is a particular problem in treating cases of malaria in the developing world.
They found the device was able to release the lumefantrine in a controlled manner, over a period of days.
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