Mind & body, Research, Technology & engineering

Drug sponge could minimize side effects of cancer treatment

By Robert Sanders

graphic of human body showing tumor in liver
To treat cancer in organs like the liver, doctors are able to deliver drugs via catheter directly to the tumor, but leftover drug can escape and affect healthy organs elsewhere in the body. A drug sponge developed by UC Berkeley chemical engineers could sop up the residual drug, lessening side effects.
graphic of human body showing tumor in liver

To treat cancer in organs like the liver, doctors are able to deliver drugs via catheter directly to the tumor, but leftover drug can escape and affect healthy organs elsewhere in the body. A drug sponge developed by UC Berkeley chemical engineers could sop up the residual drug, lessening side effects.

With the help of sponges inserted in the bloodstream to absorb excess drugs, doctors are hoping to prevent the dangerous side effects of toxic chemotherapy agents or even deliver higher doses to knock back tumors, like liver cancer, that don’t respond to more benign treatments.

The “drug sponge” is an absorbent polymer coating a cylinder that is 3D printed to fit precisely in a vein that carries the blood flowing out of the target organ – the liver in liver cancer, for example. There, it would sop up any drug not absorbed by the tumor, preventing it from reaching and potentially poisoning other organs.

In early tests in pigs, the polymer-coated drug absorber took up, on average, 64 percent of a liver cancer drug – the chemotherapy agent doxorubicin – injected upstream.

“Surgeons snake a wire into the bloodstream and place the sponge like a stent, and just leave it in for the amount of time you give chemotherapy, perhaps a few hours,” said Nitash Balsara, a professor of chemical and biomolecular engineering at the University of California, Berkeley, and a faculty scientist at Lawrence Berkeley National Laboratory.

“Because it is a temporary device, there is a lower bar in terms of approval by the FDA,” said Steven Hetts, an interventional radiologist at UC San Francisco who first approached Balsara in search of a way to remove drugs from the bloodstream. “I think this type of chemofilter is one of the shortest pathways to patients.”

graphic showing absorber

Proposed approach for drug capture using a 3D-printed absorber for endovascular treatment of liver cancer. The chemotherapy drug is administered intra-arterially via a catheter in the hepatic artery (bottom). Excess drug is captured by the absorber in the vein draining the organ (vena cava, top). (Hee Jeung Oh image)

Most anticancer drugs are poisonous, so doctors walk a delicate line when administering chemotherapy. A dose must be sufficient to kill or stop the growth of cancer cells, but not high enough to irreparably damage the patient’s other organs. Even so, chemotherapy is typically accompanied by major side effects, including nausea, vomiting, diarrhea and suppression of the immune system, not to mention hair loss and ulcers.

“We are developing this around liver cancer because it is a big public health threat – there are tens of thousands of new cases every year – and we already treat liver cancer using intra-arterial chemotherapy,” Hetts said. “But if you think about it, you could use this sort of approach for any tumor or any disease that is confined to an organ, and you want to absorb the drug on the venous side before it can distribute and cause side effects elsewhere in the body. Ultimately we would like to use this technology in other organs to treat kidney tumors and brain tumors.”

Hetts, Balsara and their colleagues at UC Berkeley, UCSF and the University of North Carolina, Chapel Hill, will publish their results online Jan. 9 in the journal ACS Central Science , an open-access publication of the American Chemical Society.

Gentler treatments

Hetts, the chief of interventional neuroradiology at the UCSF Mission Bay Hospitals, treats tumors of the eye and brain by threading catheters through the bloodstream to deliver chemotherapy drugs directly to the site of the tumor. This delivers the maximum dose to the tumor and the least dose to the rest of the body, minimizing side effects. It is a vast improvement over injecting chemotherapy drugs straight into the bloodstream, which allows the drugs to reach and poison every part of the body and gambles on the tumor succumbing before the patient. Nevertheless, typically more than half of the dose injected into the body escapes the target organ.

human body showing improvements in liver cancer treatment

Liver cancer treatment has advanced from intravenous delivery of chemotherapy drugs, which affects not only the tumor and liver but also organs throughout the body (red, left), to intra-arterial chemo (center), which limits the spread of the drug, though up to half can still exit the liver to poison the rest of the body. The proposed absorber would sop up unused drug emerging from the liver, drastically reducing unwanted effects on other organs (right).

Several years ago, he started thinking about a major improvement: filtering the blood coming out of the targeted organ to remove excess chemo so that much less of the drug reaches the body as a whole.

Balsara, a chemical engineer who specializes in ionic polymers for batteries and fuel cells, is one of the people Hetts approached to find a suitable absorber to put in the bloodstream. In 2016, former UC Berkeley and Berkeley Lab postdoctoral fellow Chelea Chen identified an ionic polymer, not unlike polymers used in fuel cells, that efficiently absorbed doxorubicin,

“An absorber is a standard chemical engineering concept,” Balsara said. “Absorbers are used in petroleum refining to remove unwanted chemicals such as sulfur. Literally, we’ve taken the concept out of petroleum refining and applied it to chemotherapy.”

That polymer led Balsara’s team to a commercial version of the absorbent polymer that was easier to obtain in large quantities, and Berkeley postdoc Hee Jeung Oh spent more than a year perfecting a way to adhere the polymer to a 3D-printed cylinder with crisscrossing struts that could be placed inside a person’s vein.

cross section through absorber

Cross section through absorber, showing crosslinks and ionic polymer coating (orange)

“Fitting the cylinder in the vein is important; if the fit is poor, then the blood with the dissolved drug will flow past the cylinder without interacting with the absorbent,” Balsara said. Recognizing the need for customizing the device for individual patients, Balsara solicited the help of a long-time collaborator, Joseph DeSimone, the CEO of Carbon, Inc. , a 3D-printing company in Redwood City.

In the experiments reported in ACS Central Science , Hetts implanted the 3D-printed device into the vein of a pig and measured how much of the doxorubicin injected upstream remained downstream of the absorber. In a healthy pig, about 64 percent of the drug was removed.

They are currently in the midst of experiments to determine how much drug is absorbed when the device is implemented at the exit of a healthy pig liver, though the true test will be in humans, perhaps in a couple of years, Hetts said.

“This is a first level in vivo validation that yes, this device will bind up drug in the bloodstream,” he said. “But extensive animal testing is not the next path; the next path is getting conditional approval from FDA to do first-in-human studies, because it is much more realistic to test these in people who have cancer as opposed to continuing to test in young pigs who have otherwise healthy livers.”

Hetts says that the technique is superior to another liver cancer treatment now undergoing testing, which requires major endovascular surgery to completely block the outputs from the liver with balloons and divert the outflowing blood to an external dialysis machine, where the drug is removed and the blood returned to the body.

“There is a lot of opportunity to develop less-invasive devices that will bind up the drug in a gentler manner,” he said.

Drug sponges could be applied to many types of tumors and chemotherapy drugs, Hetts said, and could potentially be used to sop up other dangerous drugs, such as high-powered antibiotics that are toxic to the kidneys but required to kill a pathogen.

“We think this is a generally applicable concept,” he said.

The work was supported by a grant from the National Institutes of Health. Other coauthors are Mariam Aboian, Mark Wilson, Terilyn Moore and Colin Yee of UCSF; Michael Yi, Jacqueline Maslyn and Whitney Loo of UC Berkeley; Xi Jiang and Dilworth Parkinson of Berkeley Lab; and DeSimone, Gregory Robbins and Florian Barth of Carbon.

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